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SECURITIES AND EXCHANGE COMMISSION
WASHINGTON, DC 20549
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FORM 20-F-A
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[ ] REGISTRATION STATEMENT PURSUANT TO SECTION 12 (b) or (g) OF THE SECURITIES
EXCHANGE ACT OF 1934
OR
[X] ANNUAL REPORT PURSUANT TO SECTION 13 OR 15(D) OF THE SECURITIES EXCHANGE ACT
OF 1934
For the year ended December 31, 1997
OR
[ ] TRANSITION REPORT PURSUANT TO SECTION 13 OR 15(D) OF THE SECURITIES EXCHANGE
ACT OF 1934
For the transition period from to
COMMISSION FILE NUMBER 0-19539
BIOCHEM PHARMA INC.
(EXACT NAME OF REGISTRANT AS SPECIFIED IN ITS CHARTER)
NOT APPLICABLE
(TRANSLATION OF REGISTRANT'S NAME INTO ENGLISH)
CANADA
(JURISDICTION OF INCORPORATION OR ORGANIZATION)
275 Armand-Frappier Blvd.
Laval, Quebec, Canada H7V 4A7
(ADDRESS OF PRINCIPAL EXECUTIVE OFFICES)
Securities registered or to be registered pursuant to Section 12(b) of the Act:
None
Securities registered or to be registered pursuant to Section 12(g) of the Act:
COMMON SHARES, WITHOUT PAR VALUE
(TITLE OF CLASS)
Securities for which there is a reporting obligation pursuant to Section 15(d)
of the Act: None
Indicate the number of outstanding shares of each of the issuer's classes of
capital or common stock as of the close of the period covered by the annual
report:
108,255,640 common shares, without par value (December 31, 1997)
Indicate by check mark whether the registrant (1) has filed all reports required
to be filed by Section 13 or 15(d) of the Securities Exchange Act of 1934 during
the preceding 12 months (or for such shorter period that the registrant was
required to file such reports), and (2) has been subject to such filing
requirements for the past 90 days.
Yes [X] No [ ]
Indicate by check mark which financial statements item the registrant has
elected to follow.
Item 17 [X] Item 18 [ ]
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TABLE OF CONTENTS
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PAGE
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<S> <C> <C>
PART I
Item 1 Description of Business
The Company................................................. 4
Therapeutics................................................ 5
Vaccines.................................................... 11
Diagnostics................................................. 12
Investments................................................. 13
Significant Agreements...................................... 13
Reliance on Collaborative Relationships..................... 20
Marketing................................................... 21
Manufacturing............................................... 21
Patents and Proprietary Information......................... 22
Competition................................................. 24
Government Regulation....................................... 26
Pharmaceutical Pricing and Reimbursement.................... 27
Technology.................................................. 27
Product Liability........................................... 28
International Operations.................................... 28
Employees................................................... 28
Item 2 Description of Properties................................... 28
Item 3 Legal Proceedings........................................... 29
Item 4 Control of Registrant....................................... 30
Item 5 Nature of Trading Market.................................... 30
Item 6 Exchange Controls and Other Limitations Affecting Holders of
Common Shares............................................... 31
Item 7 Taxation.................................................... 32
Item 8 Selected Financial Data..................................... 32
Item 9 Management's Discussion and Analysis of Financial Condition
and Results of Operations................................... 35
Item 10 Directors and Officers of the Company....................... 43
Item 11 Compensation of Directors and Officers...................... 47
Item 12 Options to Purchase Securities from the Company or
Subsidiaries................................................ 49
Item 13 Interest of Management in Certain Transactions.............. 50
PART II
Item 14 Description of Securities (1)............................... 50
PART III
Item 15 Defaults Upon Senior Securities............................. 50
Item 16 Changes in Securities and Changes in Security for Registered
Securities.................................................. 50
PART IV
Item 17 Financial Statements........................................ 51
Item 18 Financial Statements (2).................................... 51
Item 19 Financial Statements and Exhibits........................... 51
Signatures.................................................. 55
Financial Statements........................................ 56
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(1) Pursuant to General Instruction G(b) of Form 20-F, this annual report
includes the information specified in Parts I, III and IV.
(2) Pursuant to General Instruction G(c) of Form 20-F, the registrant has
elected to provide the financial statements and related information
specified in Item 17.
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IMPORTANT NOTES
1. EXCHANGE RATE DATA
ALL CURRENCY AMOUNTS IN THIS REPORT ON FORM 20-F ARE STATED IN CANADIAN
DOLLARS, UNLESS OTHERWISE INDICATED.
The high and low exchange rates, the average exchange rate (i.e., the
average of the exchange rates on the last day of each month during the period)
and the period-end exchange rate of the Canadian dollar in exchange for United
States dollars for each of the fiscal years in the four-year and eleven-month
period ended December 31, 1997 based on the noon buying rate in New York City
for cable transfers in foreign currencies as certified for customs purposes by
the Federal Reserve Bank of New York, were as follows:
<TABLE>
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YEARS ENDED
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1994-01-31 1994-12-31 1995-12-31 1996-12-31 1997-12-31
---------- ---------- ---------- ---------- ----------
(12 MONTHS) (11 MONTHS) (12 MONTHS) (12 MONTHS) (12 MONTHS)
<S> <C> <C> <C> <C> <C>
High................................... US$.8046 US$.7532 US$.7527 US$.7513 US$.7487
Low.................................... .7468 .7103 .7023 .7235 .6945
Average................................ .7701 .7279 .7305 .7332 .7197
Period-End............................. .7536 .7128 .7323 .7301 .6999
</TABLE>
2. STOCK SPLIT
A two-for-one stock split of the common stock took effect as of the close
of business on April 7, 1997. The share information contained in this Report on
Form 20-F reflects the stock split.
3. TRADEMARKS
BioChem Pharma and its logo, BioChem Vaccines, BioChem ImmunoSystems,
BioChem Therapeutic, CliniChem Development and its logo, Labotech, Personal Lab,
Fluviral, Fluviral S/F, PACIS, Allertech, SR1, System 9100+ Series, Detect-HIV,
Detect-HCV, Detect-TB, Detect-HTLV, Spirit Lite, Spirit Ax, Spirit Ep and Spirit
are all trademarks of BioChem Pharma Inc. or its subsidiaries.
BioChem's discovery to treat HIV/AIDS, sold in certain countries under the
brand name 3TC and in others under the brand name Epivir, or in a tablet also
containing AZT and sold in the United States under the brand name Combivir, has
the generic name lamivudine. Lamivudine is also being developed to treat chronic
hepatitis B infection, and is expected to have the brand name Zeffix in a number
of markets and Heptodin in China. To avoid confusion herein, 3TC will be used to
describe the product for HIV/AIDS and lamivudine and Zeffix will be generally
used to describe the product in development for chronic hepatitis B. 3TC,
Epivir, Combivir, Zeffix and Heptodin are trademarks of Glaxo Wellcome plc
which, with its subsidiaries, is the worldwide licensee of 3TC and lamivudine,
subject to special arrangements for Canada, where a Glaxo Wellcome-BioChem
partnership is commercializing 3TC and will commercialize lamivudine.
Intron A is a trademark of Schering-Plough Corporation; Zadaxin is a
trademark of SciClone Pharmaceuticals Inc.; Theradigm is a trademark of Cytel
Corporation ; and Retrovir is a trademark of Glaxo Wellcome plc.
4. SAFE HARBOUR
THIS REPORT ON FORM 20-F CONTAINS PROJECTIONS AND FORWARD LOOKING
STATEMENTS REGARDING FUTURE EVENTS AND THE FUTURE FINANCIAL PERFORMANCE OF THE
COMPANY. WE WISH TO CAUTION YOU THAT THESE STATEMENTS ARE ONLY OUR PREDICTIONS
AND OBJECTIVES. ACTUAL EVENTS OR RESULTS MAY DIFFER MATERIALLY. PLEASE NOTE IN
PARTICULAR THROUGHOUT THIS DOCUMENT WHERE WE HAVE HIGHLIGHTED SPECIFIC RISKS
ASSOCIATED WITH THE COMPANY AND ITS ACTIVITIES. WE ALSO REFER YOU TO THE
DOCUMENTS THE COMPANY FILES FROM TIME TO TIME WITH THE UNITED STATES SECURITIES
AND EXCHANGE COMMISSION AND THE CANADIAN SECURITIES ADMINISTRATORS, SUCH AS ITS
MATERIAL CHANGE REPORTS, ITS ANNUAL REPORT AND ITS MANAGEMENT PROXY CIRCULAR.
THESE DOCUMENTS, AS WELL AS THIS REPORT ON FORM 20-F CONTAIN IMPORTANT FACTORS
THAT COULD CAUSE OUR ACTUAL RESULTS TO DIFFER FROM OUR CURRENT EXPECTATIONS AND
THE FORWARD-LOOKING STATEMENTS CONTAINED IN THIS REPORT ON FORM 20-F. THE
COMPANY WILL NOT UPDATE THE INFORMATION CONTAINED IN THIS REPORT ON FORM 20-F
EXCEPT IN THE NORMAL COURSE OF ITS PUBLIC DISCLOSURE PRACTICES.
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PART I
ITEM 1. DESCRIPTION OF BUSINESS
THE COMPANY
BioChem Pharma Inc. ("BioChem" or the "Company") is an international
biopharmaceutical company involved in the research, development, manufacturing
and marketing of innovative products for the prevention, detection and treatment
of human diseases.
BioChem conducts its business through BioChem Therapeutic Inc.
("Therapeutic"), BioChem Vaccines Inc. ("Vaccines"), BioChem ImmunoSystems
Inc.("ImmunoSystems") and the Company's foreign subsidiaries. Therapeutic, a
wholly-owned subsidiary, is responsible for efforts in the area of therapeutics.
Vaccines, a wholly-owned subsidiary, is responsible for BioChem's vaccine
operations. The Company's diagnostics business is conducted through its
91.0%-owned subsidiary, ImmunoSystems.
The Company supports its therapeutic, vaccine and diagnostic products with
extensive research and development. There are a number of programs currently
being conducted. These programs are discussed under the captions "Therapeutics",
"Vaccines" and "Significant Agreements -- The CliniChem Programs".
The Company's most significant therapeutic product is 3TC, a nucleoside
analog with a novel heterocyclic surrogate sugar ring which has been developed
with the Company's worldwide licensee, Glaxo Wellcome plc and its subsidiaries
(collectively "Glaxo Wellcome"), for the treatment of patients with HIV
infection, including AIDS. On November 17, 1995, the United States Food and Drug
Administration (the "FDA"), in accordance with its procedures for accelerated
approval of new drugs, approved 3TC for marketing and sale in the United States
for use in combination with Retrovir (a Glaxo Wellcome product also known as AZT
or zidovudine) for the treatment of HIV infection and AIDS as a first-line
therapy. On December 8, 1995, the Canadian Health Protection Branch (the "HPB")
approved 3TC for marketing and sale in Canada under its priority review process
for use in combination with AZT for the treatment of HIV infection and AIDS. In
Europe, the European Union Committee on Proprietary Medicinal Products (the
"EUCPMP") and the European Medicines Evaluation Agency (the "EMEA") on August 8,
1996 gave full approval under exceptional circumstances for the 15 Member
States. On April 14, 1997, the FDA released 3TC under its traditional approval
regulations for use in combination with Retrovir. On September 29, 1997, the FDA
authorized the marketing of Combivir, the first product to combine two
antiretroviral drugs in a single tablet formulation. Each tablet of Combivir
contains 3TC and AZT and can be taken twice daily, offering the advantage of
reducing significantly the number of tablets a person on an Epivir/Retrovir
based treatment regimen needs to take. This reduction is simplifying the complex
multi-drug treatment regimens and is assisting patient adherence to therapy
schedules. The European Commission gave approval to market Combivir in the 15
Member States of the European Union on March 18, 1998. 3TC is being marketed in
more than 80 countries worldwide. Worldwide sales of 3TC were $973.3 million for
the fiscal year ended December 31, 1997.
A different dosage regimen of 3TC, referred to as lamivudine, is being
developed by the Company's worldwide licensee, Glaxo Wellcome, as a treatment
for chronic hepatitis B infection, including in the pre-and post-liver
transplant setting to prevent graft re-infection by HBV. Phase II and Phase III
clinical trials have shown that 100 mg lamivudine taken once daily reduced human
hepatitis B virus DNA to levels undetectable by the most widely used diagnostic
test, the Abbott Genostics assay, in the majority of patients while on therapy.
Nine Phase III clinical trials to evaluate lamivudine as a treatment of chronic
hepatitis B infection began during 1994, 1995 and 1996. The majority of these
trials are now completed, overall confirming that lamivudine has an excellent
safety and efficacy profile. The first regulatory filing submission seeking
marketing approval of lamivudine was made in China by BioChem's licensee, Glaxo
Wellcome on August 25, 1997 followed by filings in other Asian countries and in
many other countries including the countries of the European Union and Canada in
March 1998.
The Company has also developed, and is manufacturing and marketing, a line
of vaccines including whole virus and split virus influenza vaccines, a combined
diphtheria tetanus vaccine and a BCG vaccine against tuberculosis. These
vaccines are marketed to physicians and other healthcare providers in Canada by
the Company's direct sales force. The Company has also developed and is
manufacturing an immunotherapeutic
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product PACIS used in the treatment of certain superficial bladder cancers sold
by Faulding. Canadian sales of the Company's vaccines were $5.9 million for the
fiscal year ended December 31, 1997.
The Company's diagnostics operations, which had worldwide sales of $114.5
million for the year ended December 31, 1997, is engaged in the development,
manufacturing and marketing of a wide range of diagnostic products and automated
laboratory analyzers for the detection of a variety of infectious diseases, and
for use in immunology, endocrinology and hematology. In 1996, the Company
launched Personal Lab, a smaller version of Labotech, the Company's microtiter
plate analyzer and in 1997, Spirit, a new hematology analyzer.
THERAPEUTICS
BioChem's therapeutic activities currently are directed at discovering
innovative medicines principally in the antivirals and anticancer areas, and as
well in pain control. These activities are either done internally, through
agreements with CliniChem Development Inc., or through other strategic alliances
(see "Significant Agreements").
The Company's strategy in therapeutics is to commercialize its antiviral,
anticancer and related products in selected territories where there is a
relatively focused target physician audience and address broader markets with
co-marketing, licensing and other agreements. The Company's partnership with
Glaxo Wellcome represented the first step in this strategy, with the Company
sharing commercialization rights for 3TC and lamivudine in Canada but granting
exclusive commercialization rights in the rest of the world. In the future, as
the Company develops additional products in these therapeutic areas, it intends
to retain a larger share of marketing and other rights in additional
territories. The Company's efforts to successfully develop its own products will
be supplemented by seeking access to other products through collaboration,
licensing, acquisition and other arrangements.
In other therapeutic areas, including pain control, where markets are
broader and therefore the resources needed for the development and
commercialization are greater, the Company intends to continue to forge
alliances with established pharmaceutical companies. To that end, it already has
established partnerships with Astra AB in the pain control area.
The Company's most advanced therapeutic internal research and development
programs are:
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POTENTIAL
PRODUCT/COMPOUND APPLICATION/INDICATIONS DEVELOPMENT STATUS(1) COMMERCIAL RIGHTS
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ANTIVIRAL:
3TC HIV and AIDS Approved BioChem/Glaxo Wellcome
Lamivudine Chronic hepatitis B In registration BioChem/Glaxo Wellcome
Lamivudine Prevention of liver graft Phase II/III BioChem/Glaxo Wellcome
re-infection by hepatitis B
virus
Other antivirals Hepatitis B virus, hepati- Research BioChem or Biochem/OSI
tis C virus and HIV
PAIN CONTROL:
BCH-3963 Pain control Phase I BioChem/Astra
Oral peripheral (LOGO)-agonist Pain control Research BioChem/Astra
ANTI-CANCER:
Apoptosis Cancer Research BioChem
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(1) Indicates product development status. "Research" includes discovery,
research, development of screening assays, product design, synthesis and
subsequent identification of a candidate compound for clinical studies.
"Preclinical" (not used here) denotes efficacy, pharmacological and
toxicity studies in animal models necessary to support an application to
initiate human clinical testing. Human clinical trials for the Company's
drugs and biological products are conducted in three phases. "Phase I"
clinical trials are generally conducted in healthy volunteers to determine
pharmacokinetics and safety. "Phase II" clinical trials are conducted to
gain preliminary information regarding efficacy and dosing regimen and
additional safety information. The final stage is "Phase III", in which
studies are conducted to provide sufficient statistical data regarding
safety and efficacy to support an application for marketing approval of a
new drug or license of a biological product. In the case of AIDS and
certain other life-threatening diseases for which there is an urgent need
for treatment, the FDA may grant approval under its accelerated approval
regulations, based on analysis of
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surrogate endpoints even when definitive information on efficacy and
long-term safety is not yet available. Manufacturers of accelerated
approval drugs are then required to conduct more definitive clinical
endpoint studies to confirm the drug's effect on the clinical endpoints of
the disease. "In registration" means a license application to market the
product has been filed in one or more countries but has not yet been
approved. See "Government Regulation".
The Company believes that future success will from now on largely be based
on the ability to discover truly innovative therapies responding to unmet
medical needs and to rapidly move several compounds into clinical development.
To achieve its mission in this evolving industry, BioChem's strategy is to focus
intensively in the antiviral and anticancer areas, to enhance internal research
capability and to broaden a diverse external research network, involving
primarily university collaborations and partnerships with companies, as well as
to build a commercial organization and a portfolio of antiviral and anticancer
products for the North American market.
AIDS/HIV INFECTION
Market
The World Health Organization (the "WHO") estimates that, as of the end of
1997, more than 30 million people worldwide had been infected with HIV, the
virus that leads to the development of AIDS. The WHO estimates that, as of the
end of 1997, approximately 860,000 people were infected with HIV in the United
States and predicts that, by the year 2000, approximately 40 million people
worldwide will have been infected with HIV and the number of AIDS cases will
more than double. The WHO predicts that the largest increase in the incidence of
HIV infection will be in the Asia-Pacific region, Eastern Europe and the Middle
East.
3TC
The therapeutic product 3TC is for the treatment of HIV infection and AIDS.
3TC is one of a novel class of nucleoside analogs with a novel heterocyclic
surrogate sugar ring discovered and synthesized by BioChem scientists which
targets the HIV reverse transcriptase enzyme. By targeting the HIV reverse
transcriptase enzyme, 3TC appears to interfere with the transcription of viral
RNA to viral DNA, a process necessary for HIV replication. On November 17, 1995,
3TC, marketed as Epivir in the United States, was approved by the FDA under its
accelerated approval regulations for marketing and sale in the United States for
use in combination with AZT for the treatment of HIV infection and AIDS as a
first-line therapy. On April 11, 1997, the FDA released 3TC under its
traditional product approval regulations, for use in combination with Retrovir.
On December 8, 1995, the HPB approved 3TC for marketing and sale in Canada under
its priority review process for use in combination with AZT for the treatment of
HIV infection and AIDS. The EUCPMP and the EMEA on August 8, 1996 gave full
approval under exceptional circumstances for the 15 Member States. On September
29, 1997, the FDA authorized the marketing of Combivir, the first product to
combine two antiretroviral drugs in a single tablet formulation. Each tablet of
Combivir contains 3TC and AZT and can be taken twice daily, offering the
advantage of reducing significantly the number of tablets a person on an
Epivir/Retrovir based treatment regimen needs to take. This reduction is
simplifying the complex multi-drug treatment regimens and is assisting patient
adherence to therapy schedules. The EUCPMP recommended the approval of Combivir
in the week of November 18, 1997. The European Commission gave approval to
market Combivir in the 15 Member States of the European Union on March 18, 1998.
The results from four pivotal trials and from the clinical endpoint study of 3TC
have served not only to demonstrate 3TC's safety and efficacy, but also to
successfully establish 3TC as the cornerstone of combination therapy in HIV
infection. In fact, those positive results together with 3TC's ease of
administration (one tablet twice a day, independently of food intake) helped
identify the way to combine antiretrovirals for maximum clinical benefit and
compliance. They also led to 3TC being used in many triple and quadruple
combination therapies including protease inhibitors and non-nucleoside reverse
transcriptase inhibitors.
Combination therapy using two nucleoside analogs and a protease inhibitor
has become the standard of care for HIV infection. This therapeutic approach has
been validated through the results of a clinical endpoint study designed to
assess the safety and efficacy of the most widely used triple-combination
regimen. 3TC is available for sale and marketing in more than 80 countries and
is the most widely prescribed medication for HIV and AIDS in the world.
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Pursuant to agreements entered into with Glaxo Wellcome, BioChem has
licensed to Glaxo Wellcome the worldwide rights, with the exception of Canada,
to develop, manufacture and sell 3TC. In Canada, 3TC is being sold by BioChem in
partnership with Glaxo Wellcome.
Although 3TC has rapidly penetrated the market, there are certain factors
that can influence its continued success including, the willingness and ability
of HIV-infected patients to remain compliant on these complex multi-drug
combination therapies. It has been demonstrated that lack of compliance can lead
to treatment failure due to the capacity of HIV to become resistant to
antiretrovirals. The potential number of combinations that are now available has
significantly increased since 3TC was first approved for marketing and there is
no assurance that 3TC will remain or be part of all these combination therapies.
On May 6, 1998, BioChem announced the beginning of a Phase I clinical trial
in the United States on BCH-10652, a nucleoside analogue (discovered by BioChem
and which development will be pursued by BioChem through agreements with
CliniChem Development Inc.) to fight HIV infection and AIDS. The purpose of this
Phase I study in healthy volunteers is to evaluate the compound's safety and the
appropriate dosing for further studies in people living with HIV.
HEPATITIS B
Market
HBV is the infectious causative agent of both the acute and chronic forms
of hepatitis B, a liver disease which is a major cause of morbidity and
mortality throughout the world. Data from the WHO indicate that over 2 billion
people worldwide have been infected with hepatitis B, 75% of whom are found in
the Asia-Pacific region. Of these 2 billion, there are over 350 million people
chronically infected (WHO 1996), who are at high risk of developing chronic
active hepatitis which kill more than 1 million persons per year. The WHO
estimated that as many as 25-35% of individuals who become chronic carriers will
eventually die prematurely as a result of their hepatitis B of either cirrhosis
or hepatocellular carcinoma (liver cancer). Vaccines to prevent hepatitis B are
currently available; however, they have not been shown to be effective in those
already infected with the virus. Despite the availability of these vaccines for
more than a decade, the incidence of HBV infection in the United States has
increased.
Hepatitis B virus is estimated to be approximately 100 times more
infectious than the HIV virus. The main routes of transmission in North America
are: parenterally (through the use of needles) and via sexual contact. The main
routes of transmission in the rest of the world (including the Asia-Pacific
region) are from person to person and perinatally (from mother to baby during
the perinatal period).
Alpha interferon is approved for the treatment of patients with chronic
active hepatitis B. It is administered by injection, is only successful in
controlling the virus in a minority of patients and is associated with
undesirable side-effects such as flu-like symptoms. Alpha interferon has poor
efficacy in the majority of chronic hepatitis B patients who are located in the
Asia-Pacific region and who could be presumed to have acquired the disease
perinatally or at a young age. This usually leads to an immune tolerance state
of infection where an immunostimulant such as alpha interferon works poorly. The
Company believes a significant market opportunity exists for an effective and
safe oral antiviral therapy against chronic hepatitis B, especially for a
product with efficacy in immune tolerant chronic hepatitis B patients, such as
the vast majority in the Asia-Pacific region.
Lamivudine
A different dosage regimen of 3TC (referred to as lamivudine) is being
developed with Glaxo Wellcome as an oral treatment for chronic hepatitis B
infection and for the prevention of liver graft reinfection. Like 3TC with AIDS,
lamivudine targets the reverse transcriptase enzyme of HBV and appears to
interfere with the transcription of viral RNA to viral DNA, a process necessary
for HBV replication.
Clinical Trials
Pursuant to the agreements entered into between BioChem and Glaxo Wellcome,
Glaxo Wellcome is currently completing the Phase III clinical trial program of
lamivudine as a treatment for chronic hepatitis B infection and has already
completed regulatory submissions in several countries and is in the process of
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completing regulatory submissions in several other countries. To date, a total
of nine Phase III clinical trials have been initiated and almost all of them are
completed. Clinical trial sites include countries in the Asia/Pacific region and
in Europe, Australia, South Africa, Canada and the United States. Most of these
trials investigated 100 mg of lamivudine given once daily. The majority of Phase
III clinical trials were for a duration of one year of treatment with follow-up
periods ranging from three months to six months. A longer follow-up trial for up
to four years of lamivudine treatment is also ongoing.
Most of these clinical trials were designed to compare the efficacy of
lamivudine versus placebo in patients with chronic hepatitis B infection who
were alpha interferon therapy-naive. Results were measured by improvements in
liver histology and reduction of both HBeAg and HBV DNA levels as well as the
normalization of liver enzyme (ALT) and the rate of antigen HBeAg
seroconversion. Other objectives of these trials are to assess the safety of
lamivudine treatment. In certain trials, lamivudine alone were compared against
lamivudine in combination with alpha interferon. Lamivudine was also studied in
patients who were previously unresponsive to alpha interferon.
At the 32nd annual meeting of the European Association for the Study of the
Liver ("EASL") held April 9-12, 1997 in London, U.K., the results of a pivotal
Phase III lamivudine trial involving 358 Asian chronic hepatitis B patients were
presented. This was a placebo-controlled, double-blind, multicenter study where
patients were randomized to receive either placebo or lamivudine 25 mg once per
day or 100 mg once per day. Patients were assessed at 12 months. The primary
end-point of the study was the demonstration of an improvement in liver
histology with lamivudine versus placebo. The data showed a significant
improvement in liver histology in patients treated with lamivudine (100 mg once
per day). Of these patients, 67% experienced a statistically significant
improvement in liver histology versus 30% with placebo (p<0.001). Secondary
end-points of the study were lamivudine-induced normalization of liver enzymes
(ALT), suppression of HBV DNA, and increased HBeAg seroconversion. The results
demonstrated a sustained and statistically significant (p<0.001) ALT
normalization in 72% of patients with elevated ALT levels at entry versus 24%
with placebo. There was a statistically significant (p<0.001) reduction in HBV
DNA greater than 95% in patients versus placebo. HBeAg seroconversion with
undetectable HBV DNA was demonstrated in 16% of patients (p=0.022) at the 100 mg
once per day dose versus 4% in placebo. Lamivudine was well tolerated and safe
in this study, with patient withdrawal rates and adverse events not different
than placebo. Genotypic analyses have shown that 14% of patients on 25 mg and
100 mg lamivudine daily have developed genotypic changes after one year of
lamivudine treatment. However, these instances of genotypic changes were
reported to be subclinical and patients have continued to receive lamivudine
monotherapy. This data is very significant as it represents the first
demonstration of a histologic improvement regardless of serological response in
a randomized controlled study of any therapy for chronic hepatitis B patients.
It is even more significant in that these results were obtained in a group of
patients (Asian) who typically do not respond well to presently available
conventional therapy (alpha interferon).
At the American Association for the Study of Liver Disease ("AASLD") held
November 7-11, 1997 in Chicago, Illinois, U.S.A., the results of a Phase III
lamivudine trial involving 137 Japanese chronic hepatitis B patients were
presented. Patients were randomized to receive lamivudine 100 mg daily or
placebo for 16 weeks. Following the initial 16-week treatment, all patients
received lamivudine 100 mg for a further 16 weeks and were then followed off
treatment for an additional eight weeks. The study showed that in comparison to
placebo, lamivudine reduced HBV DNA significantly. Reproliferation of HBV DNA
was observed in the majority of cases after the end of treatment but its
disappearance was sustained in some patients. Lamivudine also showed a
significant reduction of HBe antigen in comparison to placebo. The seronegative
and seroconversion rates tended to increase as the treatment period prolonged.
ALT was also improved significantly by lamivudine in comparison to the placebo
group. Adverse events were similar between the lamivudine group and the placebo
group. Abnormal laboratory values were more prevalent in the placebo group
compared to the lamivudine group.
At the Alimentary Disease Week held December 12-17, 1997 in Hong Kong, the
result of a Phase III lamivudine trial involving 429 Chinese chronic hepatitis B
patients were presented. This was a randomized multicenter double-blind placebo
controlled 12-week study. All patients were offered a further nine months of
open label lamivudine treatment. 24-week data were presented and showed that
lamivudine treatment 100 mg
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daily is very effective in the inhibition of HBV replication indicated by the
rapid loss of serum HBV DNA and often accompanied by a decrease of serum ALT
levels. Lamivudine was well tolerated and the overall incidence of adverse
events was similar to placebo.
According to results presented on April 16, 1998 at the EASL in Lisbon,
Portugal, on two major clinical studies, lamivudine is consistently effective
across different hepatitis B patient groups, thus a major advance over current
therapy. One study showed lamivudine monotherapy to be effective in a specific
group of patients with a form of the disease known as "pre-core mutant hepatitis
B" which is particularly prevalent in Southern Europe, the Middle East and some
Asian countries and which responds poorly to current treatment with interferon.
This study, involving 124 patients with chronic pre-core mutant hepatitis B, was
carried out in 17 centers in Greece, Italy, Canada, Spain and the United
Kingdom. After 24 weeks of treatment, 63% of treated patients had lost
detectable virus in the blood and showed ALT normalization. This compared with
only 6% of patients taking placebo. After 52 weeks of treatment, 65% of treated
patients had lost detectable virus in the blood using Chiron bDNA tests and
showed ALT normalization. This compared with only 9% of patients taking placebo.
Also lamivudine induced a 2 point reduction in Knodell necro-inflammatory score
in 60% of patients and resulted in an improvement or no change in fibrosis in
98% of patients. Lamivudine was found to be safe and well tolerated; the
incidence of adverse events and laboratory toxicity were similar in
lamivudine-treated patients compared to placebo. A second major study compared
lamivudine therapy to a standard course of interferon (Intron A) and a course of
lamivudine and interferon combined. The study showed that patients treated with
a once daily tablet of lamivudine for 52 weeks had a similar seroconversion rate
to that achieved with injections of interferon. Patients on the combination
treatment showed a slight improvement in HBeAg seroconversion rate. However,
this improvement was not statistically significant. Lamivudine caused effective
HBV DNA suppression during treatment but HBV DNA returned off treatment in
patients who had not seroconverted. Additionally, a greater number of patients
treated with lamivudine showed improvement in liver disease regardless of
whether or not seroconversion occurred. Patients taking lamivudine also suffered
from fewer side effects than either of the other two groups treated with
interferon.
Resistance is expected with all anti-infective therapies. Selection of
genotypic mutations is a natural consequence of hepatitis B virus replication
and antiviral treatment. Resistance has been thoroughly investigated in
lamivudine clinical trials and in collaboration with academic experts.
Resistance to lamivudine results primarily from the selection of YMDD mutations
in HBV Pol gene. Data from several Phase III trials showed that the YMDD
mutations occur in a minority of patients after one year of treatment (14-32% in
individual studies, 23% overall average). Data have shown that most patients
derive significant clinical benefit from one year or more of lamivudine therapy
whether or not genotypic changes (YMDD mutations) occur. Pre-clinical and
clinical data suggest that the YMDD mutant HBV does not replicate as effectively
as the wild type and that the YMDD mutants may be less virulent than wild type
HBV.
Overall, studies confirm that lamivudine has an excellent safety and
efficacy profile across diverse hepatitis B patient groups from Europe, Asia and
North America.
In addition to these Phase III clinical trials for the treatment of chronic
hepatitis B infection, Glaxo Wellcome has initiated several Phase II clinical
trials to evaluate the safety and efficacy of lamivudine in chronic hepatitis B
patients who are in end-stage liver failure and are about to undergo liver
transplantation or who underwent liver transplantation. The objective is to
evaluate the effect of lamivudine on serologic and histological markers of HBV
re-infection post-transplantation. Preliminary results of some of these Phase II
clinical trials have been presented at a number of different scientific meetings
and indicate that lamivudine appears to be well tolerated and may prevent
re-infection following orthotopic liver transplantation.
Among the many HBV transplant patients who were on multi-drug
immunosuppressive regimens, a limited number of cases of recurrence of hepatitis
B has been reported. These recurrences have occurred post-transplant after four
to eleven months of therapy and are probably due to genotypic changes following
treatment with lamivudine. The development of HBV mutations leading to a
diminished sensitivity to lamivudine occurs at a greater rate in this patient
population compared to immunocompetent patients.
Pursuant to agreements entered into with Glaxo Wellcome, BioChem has
licensed to Glaxo Wellcome the worldwide rights, with the exception of Canada,
to develop, manufacture and sell lamivudine. In Canada, lamivudine would be sold
by BioChem in partnership with Glaxo Wellcome.
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Glaxo Wellcome will be required to demonstrate the safety and efficacy of
lamivudine through the successful completion of Phase III clinical trials in the
United States prior to applying for FDA approval for treatment of chronic
hepatitis B. There can be no assurance that the regulatory approval will be
obtained in all countries it plans to commercialize and that, if obtained, it
will be on a timely basis. Failure to obtain regulatory marketing approval on a
timely basis in each country it plans to commercialize could have a material
adverse effect on the Company's future business, financial condition and results
of operations.
The filing of submissions seeking marketing approval of lamivudine were
first made in China by BioChem's licensee, Glaxo Wellcome, on August 25, 1997
then in other Asian countries, and in March 1998 in the European Union and
Canada; to date some 30 country submissions have been made.
PAIN CONTROL
BioChem is currently developing a new class of analgesics for the control
of acute and chronic pain. The analgesics in use today for the control of severe
pain, such as morphine, an opium derivative, are widely used in spite of the
development of tolerance and the undesirable side effects suffered due to their
action on the central nervous system. The most serious side effects are physical
dependence and respiratory depression.
In August 1992, BioChem entered into a series of agreements with Astra AB
of Sweden ("Astra") providing for the research, development and
commercialization of a new class of analgesic compounds. Pursuant to these
agreements, BioChem transferred and assigned its rights to the relevant
proprietary technology to Astra and retained a right to re-acquire the Canadian
rights in exchange for the payment of royalties to Astra. In collaboration with
Astra, the Company is developing a peripherally-acting analgesic, BCH-3963, a
peripheral u-agonist which binds predominantly to u-opioid receptors located
outside the central nervous system. In animal models, BCH-3963 has exhibited
potency similar to morphine, without the associated serious side effects. The
Company believes that because this new lead compound does not appear to cross
into the central nervous system, as narcotics such as morphine do, peripheral
pain control can be achieved without the serious side effects associated with
morphine. An Investigational New Drug application ("IND") was filed in Sweden by
Astra on March 16, 1998 and was approved in April 1998. A Phase I clinical trial
is starting on May 18, 1998 in Sweden by Astra. The Company believes that this
compound could potentially be developed for the treatment of subacute or chronic
painful conditions associated with inflammation, such as post-operative pain and
pain due to cancer and arthritis.
In collaboration with Astra, BioChem is also carrying out research to
discover a second generation of peripheral u-agonists with oral bioavailability
which, like BCH-3963, would act predominantly through peripheral u-opioid
receptors.
OTHER RESEARCH AND DEVELOPMENT
BioChem also has research and development programs in the anticancer and
antiviral areas.
In the area of anticancer, a collaboration was entered into on August 1,
1997 between ImmunoGen Inc.'s subsidiary Apoptosis Technology, Inc ("ATI"), and
BioChem for the discovery and development of novel anticancer therapeutics using
ATI's proprietary screens based on proteins involved in apoptosis, or programmed
cell death for two groups of targets, the SScl-2 family of proteins and the
insuline-like growth factor receptor (IGFR-1).
In the area of antivirals, BioChem has synthesized a number of nucleoside
analogs and is exploring these compounds to identify activity against HBV and
HIV. BioChem has a research program in the field of hepatitis C virus and HIV in
collaboration with OSI, Inc. Four separate molecular targets have been
identified for hepatitis C drug discovery. High throughput screening has been
initiated and early chemical leads have begun to emerge for further evaluation.
In collaboration with XTL Biopharmaceuticals Ltd., BioChem has co-developed an
animal model for hepatitis C screening. In December 1997, BioChem also obtained
exclusive rights to drug candidates in Scriptgen Pharmaceuticals, Inc.'s
hepatitis B and dimerescent receptor research programs and made a US$20 million
equity investment in Scriptgen Pharmaceuticals, Inc.
BioChem has also entered into development and marketing agreements for
Canada with Vertex Pharmaceuticals, Inc. (VX-710), Unimed Pharmaceuticals, Inc.
(Nitazoxanide, DHT-gel, Testosterone gel) and Cell Therapeutics, Inc.
(lisofylline and CT-2584). VX-710 is being developed to resensitize tumours to
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treatment with chemotherapeutic agents in patients with cancer complicated by
multidrug resistance. BioChem is conducting two Phase II clinical trials in
patients with soft tissue sarcoma and ovarian cancer. Lisofylline is presently
being studied in Phase III trials to determine its effectiveness in reducing the
incidence of serious infections and treatment-related mortality among patients
receiving high-dose chemotherapy and/or radiation therapy. Nitazoxanide is being
developed to treat cryptosporidiosis in HIV/AIDS patients, a potentially
life-threatening parasitic infection in this patient population. On May 6, 1998,
an FDA advisory panel voted that Unimed Pharmaceuticals, Inc. failed to
demonstrate the efficacy of Nitazoxanide to treat diarrhea associated with
crystosporidiosis in AIDS patients. This may limit the possibility of this
product being approved in Canada. Dihydrotestosterone gel (DHT-gel) is in Phase
I clinical trials for treatment of HIV/AIDS wasting. DHT-gel is also in Phase
II/III to study its safety and efficacy for hormonal replacement in elderly
hypogonadal men. The testosterone gel (T-gel) is presently in Phase III clinical
trials to evaluate its safety and efficacy as hormone replacement therapy in men
suffering from hypogonadism.
VACCINES
BioChem is engaged in the research, development, production and marketing
of vaccines for human use in Canada and internationally. The Company currently
manufactures and markets in Canada the following vaccines: whole and split
influenza virus, tuberculosis and combined diphtheria and tetanus. The Company
also distributes, in Quebec, a number of vaccines produced by other companies.
In 1997, the Company also started to export its split influenza vaccine to
Argentina following the signing of a distribution agreement with Argent C.
Comercio Internacional S.A.
The Company has also developed an immunotherapeutic that is effective in
the treatment of certain superficial bladder cancers. This BCG (Bacillus
Calmette-Guerin) formulation is marketed by Faulding (Canada) Inc. under the
trademark PACIS in Canada. In December 1994, the Company signed a distribution
agreement for PACIS in the United States with Urocor, Inc. In May 1995, the
Company also signed a distribution agreement for PACIS in Spain with Grupo
Ferrer S.A. The Company filed a Product License Application ("PLA") and an
Establishment License Application ("ELA") in the United States in April 1995 for
PACIS. The FDA has since advised the Company on two subsequent occasions that
its application was not approvable and requested additional data regarding
certain aspects of manufacturing and testing of the product. The Company has
provided the requested additional data to the FDA. An inspection by the FDA is
scheduled for the second quarter of 1998. Notwithstanding the two non-approval
letters from the FDA, the Company believes it can satisfy FDA requirements and
procure approval for marketing in the United States; however, there can be no
assurance that such approval will be obtained. See "Government Regulation."
BioChem is also involved in the development of a new tissue culture-based
influenza vaccine using a novel proprietary cell line and cell culture process
described as a "high density microcarrier technology". BioChem believes that
this manufacturing technology will allow for a more profitable production
process and for better flexibility in the case of an increased demand for an
influenza vaccine which would be required during a pandemic. BioChem completed
in April 1997 a Phase I clinical trial of a vaccine produced with the new cell
culture process and containing two influenza virus strains (B/Harbin and
A/Texas). The results of this first clinical trial conducted in Canada, showed
that the safety and immunogenicity of the new vaccine was equal to that found
with the conventional egg-derived vaccine. BioChem began a phase II/III clinical
trial program in Canada in November 1997. This Phase II/III program includes
three trials involving 1,000 patients. The objectives of these trials are to
compare the immunogenicity and safety of the new vaccine with the Company's
commercially available classical influenza vaccine in three different patient
populations: healthy adults, adults 65 years of age or older, and children three
to 12 years of age. The Company expects to have a final report around the middle
of 1998.
On May 12, 1997, Vaccines concluded a strategic agreement with BioVector
Therapeutics S.A. ("BioVector") aimed at developing novel human vaccines for
nasal administration by combining BioChem's expertise in vaccines with
BioVector's innovative supra molecular biovector technology in development. On
April 28, 1998, the Company announced the beginning of a Phase I clinical
testing on an influenza vaccine designed for nasal administration. The
randomized double-blind controlled Phase I study is being conducted in Canada in
60 healthy adult subjects and has the objectives to assess the safety of the
vaccine and to evaluate local and systemic immune response (immunogenicity) to
the vaccine.
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Through a research collaboration with the Vaccine Research Unit of the
Laval University Hospital Research Center, the Company is also involved in
research and development of new recombinant protein-based bacterial vaccines.
Specific proteins have been identified as immunogens for their potential use for
development in bacterial vaccines. This program will be pursued by CliniChem
Development Inc. under agreements with BioChem.
The Company recently completed a new vaccine production center in Ste-Foy
in the Quebec City area. This new $35 million center has an overall area of
approximately 118,000 square feet and houses new R&D, production,
quality-control laboratories and warehousing as well as administrative offices.
Commercial vaccine production in Ste-Foy is scheduled to start in the first half
of 1998.
On April 23, 1998, BioChem acquired the 25% equity interest in Vaccines
held by SOFINOV Societe financiere d'innovation inc.
DIAGNOSTICS
The Company's international diagnostics operation is engaged in the
development, manufacturing and marketing of diagnostic systems and products. In
June 1994, the Company acquired 100% of the shares of Ares Diagnostics
(Holdings) B.V. and its subsidiaries, comprising the diagnostics business unit
of Ares-Serono Group of Switzerland, for a total purchase price of $84.7
million.
The Company develops, manufactures and markets reagents and instrument
systems primarily for the immunology, endocrinology and hematology segments of
the diagnostic market. Its manufacturing facilities are located in the United
States, Italy, the United Kingdom and Canada. The Company has direct marketing
operations in the United States, Germany, Italy, France, Argentina, Japan,
Singapore and Canada, and also sells its products through a complementary
worldwide distributor network.
The Company's diagnostics operations had sales of $114.5 million for the
year ended December 31, 1997. The Company's major markets include the United
States, Italy, Germany and France. The Company's major product lines include the
LABOTECH instruments and corresponding assays, the SR1 analyzer and assays,
hematology analyzers and reagents and Radioimmunoassay ("RIA") products.
LABOTECH: The LABOTECH instrument is an open system which automates the
processing of diagnostic test kits in the microtiter plates ("MTP") format.
LABOTECH is marketed through original equipment manufacturers, BioChem's direct
sales force and distributors. The Company supports its LABOTECH analyzer with a
complete line of diagnostic kits that include BioChem peptide-based kits,
hormones and other MTP detection kits.
PERSONAL LAB: Personal Lab, an automated smaller version of Labotech, was
introduced at the end of 1996. This new system works with all existing
diagnostic kits already developed for Labotech but is designed for users with
smaller numbers of specimens.
INFECTIOUS DISEASE KITS: In addition to its existing testing kits for
pathogenic agents present in blood, such as HIV-I/II, the hepatitis C virus as
well as human t lymphocyte virus-I/II (HTLV-I/II), the Company is now offering a
new array of diagnostic kits including tests for toxoplasma, rubella,
cytomegalovirus, herpes and tuberculosis and a complete range of diagnostic
testing kits for hepatitis B.
HORMONE KITS: The Company has developed and is producing and marketing MTP
tests for the measurement of steroid hormone levels important in monitoring
ovulation and pregnancy, and in the diagnosis of a number of metabolic disorders
involving the malfunction of the endocrine system.
ALLERTECH: The ALLERTECH instrument is a fully-automated, walk-away,
enzyme-linked immunoassay ("ELISA") MTP analyzer dedicated to allergy testing
commercialized by the Company with a broad range of allergen assays.
SRI: The SRI analyzer is a fully-automated enzyme immunoassay system with a
differentiating menu which meets the specific needs of reproductive
endocrinologists, fertility specialists, in vitro fertilization centers and
OB/GYN group practices. The SRI offers reproductive endocrinology assays
routinely performed in infertility diagnostic procedures, assays for evaluating
thyroid function, tumor marker testing assays, as well as other assays.
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Series 9100+ HEMATOLOGY ANALYZERS: The Company manufactures and markets the
Series 9100+ Hematology Analyzers that are modular in concept. These automated
analyzers offer a wide range of diagnostic capabilities ranging from complete
blood count analysis to full blood cell morphology and are for physician office
laboratories and medium volume hospital laboratories.
SPIRIT: At the end of 1997 the Company new hematology analyzer, Spirit, was
introduced to the market. Spirit, a compact, full-featured automated system
targeted toward low to medium volume hospital laboratories, rounds out the
Company's existing product line. Because Spirit offers a number of features
within one unit, it is cost effective for users, and provides significant
flexibility.
RIA PRODUCTS: The Company manufactures and markets over 50 different RIA
test kits for fertility/infertility, pregnancy, growth and metabolism and tumor
markers testing. In addition, the Company offers a full line of thyroid assays,
including specialty tests such as kits for thyroid auto-antibodies.
INVESTMENTS
NAVA
As of December 31, 1997, BioChem held approximately 35% of the outstanding
common shares and 50% of the outstanding convertible preferred shares of North
American Vaccine, Inc. ("NAVA"), a publicly traded biotechnology company listed
on the American Stock Exchange. The Company shares control of NAVA pursuant to
the terms of a shareholders' agreement. NAVA is engaged in the research,
development and production of vaccines for the prevention of infectious diseases
in children and adults.
GENECHEM
In March 1997, BioChem agreed to make an investment of $30 million in
GeneChem Technologies Venture Fund L.P., a venture capital fund sponsored by the
Company's newly created subsidiary, GeneChem Financial Corporation. This $100
million fund invests in academic projects and early-stage private or public
companies in the area of genomics and related technologies for human
application. The Company's partners in this fund are a select group of financial
investors.
SIGNIFICANT AGREEMENTS
The Company develops products both independently and in collaboration with
established pharmaceutical companies or other suitable partners. Collaborative
partners may provide financial resources, research and development and
manufacturing capabilities, and sales and marketing infrastructure, to aid in
the commercialization of the Company's potential products. Presented below is a
brief description of BioChem's most significant collaborative agreements.
GLAXO WELLCOME
By an agreement dated January 31, 1990 and amended as of November 15, 1995,
the Company licensed to Glaxo Wellcome, the worldwide rights, with the exception
of Canada, to develop, manufacture and sell the nucleoside analogs 3TC and
lamivudine (3TC and lamivudine referred to herein as the "3TC Products"). A
partnership exists between Glaxo Wellcome's Canadian subsidiary, Glaxo Wellcome
Inc., and the Company to supply, market and sell the 3TC Products in Canada.
Glaxo Wellcome has agreed to manufacture all of the 3TC Products required to be
supplied in Canada by the partnership.
In consideration for the grant of such rights, Glaxo Wellcome agreed to
undertake and fund the development of the 3TC Products and to pay the Company a
royalty on sales of the 3TC Products. In addition, it was agreed that milestone
payments would be made to the Company in installments as Glaxo Wellcome
progressed in the development and approval process. The amount of any patent
prosecution costs and 50% of milestone payments are deductible from any
royalties payable to the Company by Glaxo Wellcome. The milestone payments and
its related deductions from royalties have been completed. The amount of certain
contractual costs and certain litigation costs may be deducted from royalties
payable to the Company by Glaxo Wellcome. If Glaxo Wellcome terminates the
license agreements upon certain events of default by the Company, Glaxo Wellcome
will retain a non-exclusive, paid-up license from the Company to make, have
made, use and sell the 3TC Products worldwide.
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ASTRA
On August 31, 1992, Astra AB of Sweden ("Astra") and the Company entered
into a series of agreements for an initial period of three years (the "Astra
Agreements") providing for the research development and commercialization of a
new class of analgesic compounds for the control of pain. Pursuant to the Astra
Agreements, BioChem transferred and assigned its rights to the relevant
proprietary technology to Astra and retained a right to re-acquire the Canadian
rights in exchange for the payment of royalties to Astra. In addition, a
collaborative research agreement and a supply agreement provide for Astra and
the Company to jointly research the field of opioid peptides. Astra will retain
commercial rights worldwide except for Canada. In consideration for the grant of
such rights to Astra, Astra made an upfront payment, agreed to fund research and
development, to make milestone payments to BioChem and to pay BioChem a royalty
on future product sales. Astra may, in its sole discretion, terminate the Astra
Agreements. If Astra terminates the Astra Agreements, BioChem will have a
two-year option to reacquire the relevant intellectual property rights in
exchange for reimbursing funding to date.
As of January 1, 1996, the Company and Astra have agreed to continue the
research program for a further period of three years. The extended research
program will be directed to the discovery of orally-absorbed,
peripherally-acting pain control agents.
OSI
In May 1996, BioChem and OSI, Inc. ("OSI") entered into a five-year joint
collaborative research, development and commercialization agreement for novel
antiviral drugs for the treatments of hepatitis C and HIV. Under the terms of
the agreement, BioChem and OSI have committed, each at its own costs, a team of
research scientists to discover novel compounds. In addition, BioChem and OSI
will share equally the development costs for the candidate drugs arising from
the research program. BioChem and OSI will share equally in the
commercialization rights of the resulting drugs. In February 1997, this
agreement was expanded to include additional viral targets utilizing OSI's
platform of drug discovery technologies.
BIOVECTOR
On May 12, 1997, BioChem concluded a strategic agreement with Biovector
Therapeutics S.A. ("Biovector"), a privately owned French company specializing
in drug and vaccine delivery technologies. The objective of this alliance is to
develop novel human vaccines for nasal administration using Biovector's
innovative supra molecular biovector technology in development. For the right to
use Biovector's vaccine delivery technology and rights to commercialize the
vaccines incorporating this technology, BioChem has taken a minority equity
interest in Biovector and is assuming product development and registration costs
for the vaccines involved, and will pay a royalty on sales.
ATI
A collaboration was announced on August 1, 1997 between the Company and
ImmunoGen Inc.'s subsidiary, Apoptosis Technology, Inc. ("ATI") for the
discovery and development of novel anticancer therapeutics. BioChem was granted
an exclusive, worldwide licence to ATI's proprietary screens based on two
families of proteins involved in apoptosis, for use in identifying leads for
anticancer drug development. Identification of novel targets and development of
new screens in the same two areas are also covered by this agreement. BioChem is
responsible for the development of all products arising from the collaboration,
is investing in ATI's equity in order to finance ATI's research activities over
a minimum three-year period, and is making milestone payments for each product
over the course of development. ATI will receive royalties on the worldwide
sales of products resulting from the collaboration.
SCRIPTGEN
On December 19, 1997, BioChem concluded a license agreement and an equity
investment of US$20 million in Scriptgen Pharmaceuticals, Inc. ("Scriptgen").
Pursuant to the license agreement, BioChem has exclusive rights to drug
candidates in Scriptgen's hepatitis B and dimerescent receptor research
programs. Scriptgen is responsible for all aspects of drug discovery and has to
provide BioChem with small molecule drug candidates for novel molecular targets
in the hepatitis B research program. BioChem is
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responsible for conducting preclinical and clinical development and seeking
regulatory approvals and will retain worldwide commercialization rights,
although profits from any commercialized products will be equally shared.
BioChem also obtained options to acquire Scriptgen's dimerescent receptor
program directed to the discovery of novel small molecule drugs which act as
mimics of therapeutic proteins by activating dimerization of certain receptors
such as the erythropoietin receptor. Milestone payments to Scriptgen are
attached to the exercise of the options. In consideration for its US$20 million
equity investment in Scriptgen, BioChem obtained 20% of Scriptgen's equity and
five-year warrants exercisable for an additional 5% of Scriptgen's equity.
CLINICHEM
On February 9, 1998, the Company announced that it has filed a registration
statement with the United States Securities and Exchange Commission, and a
corresponding prospectus with Canadian Securities Administrators on behalf of
newly-formed CliniChem Development Inc. ("CliniChem") relating to the
distribution, by way of dividend, of Class A Common Shares of CliniChem to the
Company's shareholders.
BioChem will contribute $150 million to CliniChem as a capital
contribution. CliniChem was formed by the Company for the purpose of conducting
the clinical development of certain of its therapeutic and vaccine products with
a goal of commercializing such products. After the distribution is made,
CliniChem will continue the development of a number of therapeutic and vaccine
candidates initially discovered and, as the case may be, developed by BioChem.
Such activities will be contracted by CliniChem to BioChem.
At the time of the capital contribution, BioChem will record an investment
in CliniChem of $150 million. Under Canadian generally accepted accounting
principles ("GAAP"), BioChem will charge the carrying value of the distribution
to retained earnings on the date of the declaration of the distribution. Under
U.S. GAAP, BioChem will charge the fair market value of the distribution to
retained earnings and will expense the excess of the carrying value of its
investment in CliniChem Class A Common Shares over the fair market value of
these shares. The fair market value of the CliniChem Class A Common Shares will
be determined by BioChem based on their closing price on relevant stock
exchanges on the distribution date. This difference between the Canadian and
U.S. GAAP treatment of the distribution will be disclosed in a reconciling note
to BioChem's financial statements. BioChem will recognize as revenue the
payments from CliniChem under a Research and Development Agreement between the
parties and the research and development costs incurred by BioChem to perform
its obligations under the Research and Development Agreement will be expensed as
research and development expenses under Canadian and U.S. GAAP.
If BioChem exercises the purchase option of all the outstanding CliniChem
Class A Common Shares, the purchase option exercise price will be allocated
between capitalized intangibles (for the value of completed CliniChem products)
and in-process research and development (for the value of research and
development on-going under the CliniChem research and development programs).
Under U.S. GAAP, the value attributed to in-process research and development
will be immediately written off as an expense, while under the Canadian GAAP it
will be amortized over the period benefited.
The therapeutic and vaccine development programs to be conducted by
CliniChem under agreements with BioChem are discussed in the following section
"The CliniChem Programs".
BioChem will hold an option to acquire commercialization rights with
respect to individual products developed by CliniChem on a country-by-country
basis. BioChem will also hold an option to purchase all of the outstanding
CliniChem Class A Common Shares at a price to be set according to a
predetermined formula. Under the terms of such option, BioChem may elect to
issue its common shares in satisfaction of the purchase price.
THE CLINICHEM PROGRAMS
BCH-4556
BCH-4556 is a nucleoside analog being developed to treat various forms of
cancer. Nucleoside analogs, such as gemcitabine and Ara-C, are used in the
treatment of cancer. Nucleoside analogs inhibit tumor growth by preventing cell
replication. Currently marketed nucleoside analogs have two major disadvantages
that impair their anti-cancer activity and have limited their use to date.
First, they are rapidly deaminated, which
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leads to a loss of efficacy and to the resistance of the cancer to treatment.
Second, existing nucleoside analogs are typically unable to completely stop cell
division and therefore do not optimally treat cancer. BCH-4556 is a nucleoside
analog which the Company and CliniChem believe will provide significant benefits
in treating various forms of cancer due to its novel structure. Discovered and
synthesized by BioChem scientists, BCH-4556 is structurally different from
currently marketed nucleoside analogs. BCH-4556 is not vulnerable to deamination
and may be able to completely stop cell division. The Company and CliniChem
believe that both of these characteristics could lead to improved efficacy
compared to other currently marketed nucleoside analogs. BCH-4556 is planned to
be administered initially by intravenous injections, but oral formulation is
also examined.
BCH-4556 was selected for clinical development based on the activity it
demonstrated against a variety of human tumors grown in immunocompromised mice
and against human tumor cells taken directly from patients. Phase I safety and
pharmacokinetic studies are currently in progress in advanced stage cancer
patients with solid cancer tumors. A single dose regimen is being evaluated in
collaboration with the National Cancer Institute of Canada. Two additional
multiple dose regimens are being conducted in the United States. CliniChem plans
to conduct Phase II clinical trials with BCH-4556 in 1998 targeting various
types of cancer (e.g. renal, prostate, breast, ovarian, colorectal, non-small
cell lung, pancreatic, head and neck, leukemia and melanoma). CliniChem hopes
the initial pilot Phase II studies to demonstrate the types of cancer in which
BCH-4556 shows activity. If it obtains positive results, CliniChem will then
focus on certain types of cancer in the Phase II/III trials.
According to DataMonitor Healthcare Reports, 1997; Cancer to 2005,
approximately 8 million people worldwide are diagnosed each year with cancer.
The worldwide market for anti-cancer treatments in 1996 was approximately
US$10.2 billion, or 4.3% of the global pharmaceutical market. In 1996, the
anti-cancer market grew by approximately 12% over the previous year. Factors
influencing the strong growth in the cancer market include: (a) increased
incidence of cancer; (b) improved diagnosis; and (c) development of effective
adjunct therapies which enable more intense, more effective and more widespread
use of chemotherapy. The increased incidence of cancer is due to many factors,
including: (a) worldwide population growth; (b) longer life expectancies; and
(c) increased exposure to carcinogenic environmental or dietary factors.
BCH-10652
BCH-10652 is a compound being developed for the treatment of HIV infection
and AIDS which has been shown to stop the replication of the HIV virus in vitro.
BCH-10652 is a nucleoside analog with a novel structure which targets the HIV
reverse transcriptase enzyme. By targeting the reverse transcriptase enzyme,
BCH-10652 appears to interfere with the transcription of viral RNA to viral DNA,
a process necessary for HIV replication. Other nucleoside analogs, such as AZT
and 3TC, also inhibit the reverse transcriptase enzyme. However, BCH-10652
appears to be capable of inhibiting the replication of HIV viruses that have
become resistant to 3TC and AZT and to some protease inhibitors. In addition,
based on in vitro studies, resistance to BCH-10652 appears slow to develop.
CliniChem believes these properties may give BCH-10652 a role in the treatment
of both HIV-infected patients in whom standard triple combination regimens are
no longer effective and patients who have never received anti-HIV therapy
(first-line therapy). The current approach to HIV treatment usually relies on
triple combination therapy, typically two nucleoside analogs and a protease
inhibitor.
Various pre-clinical tests performed to assess the safety of BCH-10652 have
indicated a good safety profile for this compound. Because of the long-term use
of HIV infection treatments, a safe compound has a significant competitive
advantage. A Phase I clinical trial in healthy volunteers has been initiated in
the U.S. on May 6, 1998. This study is to assess the safety and pharmacokinetics
of BCH-10652. The results of this trial should enable CliniChem to select two or
three doses for the subsequent Phase II trials, which will be designed to assess
the safety and efficacy of BCH-10652 in HIV-infected individuals.
According to Worldwide Antiretroviral Sales, IMS Report, for 1997, the
antiretroviral (anti-HIV) market was approximately US$2 billion in sales,
divided between reverse transcriptase inhibitors (US$1.2 billion) and protease
inhibitors (US$800 million). The vast majority of the sales were generated in
North America, Western Europe and Japan. The WHO estimates that, as of the end
of 1997, over 30 million people worldwide had been infected with HIV, the virus
that causes AIDS. It is generally believed that the
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vast majority of individuals infected with HIV will ultimately develop AIDS,
which currently has a very high fatality rate. Assuming that trends in many
parts of the world will continue, the WHO estimates that, by the year 2000, more
than 40 million people worldwide will have been infected with HIV.
ANGIOGENESIS INHIBITORS
Angiogenesis is the process whereby new blood vessels are formed. Over the
last few years, it has been recognized that tumor growth is dependent upon the
formation of new blood vessels to supply the cancer mass with oxygen and
nutrients and to remove carbon dioxide and other metabolic products.
Consequently, angiogenesis is required for the growth and proliferation of
cancer tumors. The inhibition of angiogenesis, therefore, may prevent tumor
growth.
One of the required elements of the angiogenic process is the activation of
the a(v)b(3) receptor. BioChem is pursuing the discovery and development of
small molecules that block the receptor and thus should inhibit solid cancer
tumor growth and progression. Such molecules are expected to be utilized in
combination with standard chemotherapeutic agents to treat a wide variety of
solid cancer tumors. BioChem scientists are currently collaborating with Beth
Israel Deaconess Hospital in Boston, Massachusetts to develop assays and with
Amrad Natural Products Pty Ltd ("ANP") in Melbourne, Australia to identify and
characterize novel, small molecules that inhibit tumor-associated angiogenesis.
To date, BioChem has identified two classes of small molecules that have
demonstrated activity in in vitro angiogenesis models through a(v)b(3)
antagonism. CliniChem will continue to pursue the angiogenesis inhibitor program
with the objective of identifying drug candidates suitable for clinical
development.
There is no product currently marketed which has been approved for the
treatment of cancer by inhibiting angiogenesis. However, there are a number of
agents in pre-clinical and clinical development which are being studied alone or
in conjunction with chemotherapeutic agents. Due to the nature of the angiogenic
process, these agents are likely to be administered over a long period of time
to prevent angiogenesis. If effective in preventing the recurrence of cancer
tumors, BioChem and CliniChem believe that the market for these angiogenesis
inhibitors may be substantial. BioChem and CliniChem also believe that such
products, if successfully developed, could be used as: (a) an adjunct to
chemotherapy or radiotherapy; (b) a follow-up to chemotherapy to prevent
recurrence of the tumors and metastases; (c) therapy for large, slow-growing
tumors that are less responsive to cytotoxic chemotherapy; and (d) first-line
therapy to bypass drug resistance.
VACCINES
Vaccines are antigens, frequently formulated with an adjuvant (an agent
added to antigens to enhance their immunogenicity), that stimulate the immune
system to induce protective immunity. CliniChem intends to develop recombinant
protein vaccines against numerous bacterial infections for which there are no
vaccines currently available or for which existing vaccines have low efficacy.
CliniChem will initially focus its efforts on the development of candidate
vaccines against bacterial diseases related to infections of Neisseria menin-
gitidis (bacterial meningitis) and Streptococcus pneumoniae (pneumonia,
meningitis, otitis media (acute middle ear infections)) and will also be
developing vaccines against infections of Neisseria gonorrhoeae (gonorrhea),
Haemophilus influenzae non typeable (otitis media), Streptococcus Group B and
Chlamydia pneumoniae.
Most bacterial vaccines available today are polysaccharide vaccines or
conjugate polysaccharide vaccines. Polysaccharide vaccines suffer from a number
of disadvantages. First, polysaccharide vaccines are T-cell independent
antigens, which give rise to no immune memory effect. They therefore only
produce short-term immunity. Second, the existing polysaccharide vaccines
generally are poorly immunogenic in children. Therefore, they do not produce
strong or long lasting immunity in young children, and are non-immunogenic in
children under two years of age. Third, they do not elicit good secondary
responses and, therefore, they cannot be used to produce a booster effect.
Furthermore, there is a strong antigenic variation between the polysaccharides
of different bacterial strains of the same bacteria which necessitates the
combination of multiple antigens to ensure a broader immunity. In other words,
different bacterial strains have unique polysaccharides, making it difficult for
a single polysaccharide vaccine to provide global protection against a broad
range of strains of bacterium. Consequently, numerous polysaccharide antigens
must be administered to protect against multiple strains of a bacterium. The
production of such multi-valent vaccines is time
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consuming and expensive. Finally, there are certain infections for which no
polysaccharide vaccines currently exist.
In part to overcome certain limitations of polysaccharide-based vaccines,
conjugate polysaccharide vaccines have been and are currently being developed.
One such vaccine to protect against Haemophilus influenzae type B is currently
marketed. These conjugate polysaccharide vaccines couple a polysaccharide-based
vaccine with a protein carrier. Because of the protein carrier, conjugate
polysaccharide vaccines induce a T-cell dependent response, which induces a
memory effect and can be used to produce a booster effect. These conjugate
polysaccharide vaccines, however, have their own limitations. Because of the
limited number of conjugate polysaccharide vaccines that can be combined in a
single dose, current conjugate polysaccharide vaccines provide protection
against only a limited number of strains of a bacterium. In addition, because of
the conjugation process, conjugate polysaccharide vaccines are expensive, time
consuming and difficult to manufacture.
BioChem is currently developing recombinant protein vaccines that attempt
to overcome the problems and limitations of both polysaccharide vaccines and
conjugate polysaccharide vaccines. BioChem's recombinant protein vaccines are
T-cell dependent. BioChem and CliniChem hope these vaccines will produce (a)
immunogenicity in children under the age of two and (b) a better and
long-lasting immunity in people of all ages. In addition, BioChem and CliniChem
believe that the development of a vaccine based on a common and conserved
antigen in all the strains of a given bacteria should allow the design of a
single protein vaccine that could provide global protection against multiple
strains of a bacterium. Furthermore, such vaccines should be easier to
manufacture and could be more easily combined with other existing or developed
vaccines for other diseases.
BioChem under agreements with CliniChem is working on the development of
recombinant protein vaccines against the following bacterial infections:
NEISSERIA MENINGITIDIS
Neisseria meningitidis ("N. meningitidis") causes both endemic and epidemic
disease, principally meningitis and meningococcal septicemia. The current
polysaccharide vaccine has antigens associated with only four (A, C, W135 and Y)
of the twelve serogroups (groups of bacterial strains that share a common
capsular polysaccharide antigen) of N. meningitidis. BioChem has discovered a
protein that appears to hold potential for the development of a new human
vaccine against all strains of N. meningitidis, including serogroup B strains,
which are prevalent and for which no vaccine currently exists. BioChem and
CliniChem believe that this protein is present in all meningococcal isolates and
that it is exposed at the surface of intact meningococcal cells, where it is
accessible to antibodies. BioChem and CliniChem believe that this vaccine will
have all the benefits of recombinant protein vaccines described above.
In research experiments, BioChem used its candidate vaccine to immunize
mice in order to evaluate the vaccine's ability to confer protection against an
infection by injection of a lethal dose of N. meningitidis strain of serogroup
B. This pre-clinical work showed that the purified protein was immunogenic and
protective when administered with an adjuvant. The antibodies present in the
serum fraction of the blood obtained from the immunized mice recognized
BioChem's recombinant protein as well as the native N. meningitidis protein.
Work done in research laboratories showed that the antibodies killed N.
meningitidis bacteria. This type of bactericidal activity is commonly recognized
as being indicative of protection. The recombinant vaccine was also injected
into monkeys. The monkeys, like the mice, developed antibodies that were shown
to kill N. meningitidis bacteria. BioChem has developed a manufacturing process
in anticipation of clinical trials which CliniChem expects to begin toward the
end of 1998 should the ongoing pre-clinical development program confirm the
safety and efficacy of the vaccine.
Acute meningitis and meningococcal septicemia have a high rate of
mortality. The latest outbreak in Sub-Saharan Africa, in 1996, affected over
100,000 people and claimed at least 10,000 lives. The WHO estimates that
approximately 35,000 of the 310,000 cases reported worldwide each year are
fatal. The development of a highly effective vaccine against meningococcal
infection is a research priority identified by the WHO and by the Committee of
the Children's Vaccine Initiative of the United States.
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In the United States, infection by N. meningitidis is the second most
common cause of bacterial meningitis (approximately 20% of all cases), affecting
approximately 4,000 people each year. The fatality rate is approximately 10% for
meningococcal meningitis and 20% for meningococcal septicemia, despite therapy
with antimicrobial agents such as penicillin. The incidence of endemic
meningococcal meningitis is highest among children aged 6-12 months and then
steadily declines with age. By 5 years of age, the incidence approximates that
for adults. Serogroup B, for which no vaccine exists, accounts for about 50%-55%
of all cases of infection by N. meningitidis. While serogroup A causes only a
small portion of endemic disease in the United States, it is the most common
cause of epidemics in developing countries.
NEISSERIA GONORRHOEAE
Infections due to Neisseria gonorrhoeae ("N. gonorrhoeae") are a major
cause of pelvic inflammatory disease, tubal infertility, ectopic pregnancy and
chronic pelvic pain in the United States. Based upon evaluations made by Centers
for Disease Control ("CDC"), approximately 326,000 cases of gonorrhea were
reported in the United States in 1996, a rate of 124 cases per 100,000 persons.
Because 29% of the N. gonorrhoeae isolates collected in 1996 were resistant to
penicillin, tetracycline or both, antimicrobial resistance remains an important
consideration in the treatment of gonorrhea.
BioChem believes it has discovered a conserved surface protein that is a
candidate for a recombinant vaccine against infection by N. gonorrhoeae. This
protein is present at the surface of all gonococcal strains evaluated by BioChem
to date. BioChem scientists have sequenced the gene coding for this conserved
protein and have injected animals with the recombinant protein.
In pre-clinical work, BioChem used its candidate recombinant vaccine to
immunize mice in order to evaluate the protein's ability to confer protection
against bacterial infection of N. gonorrhoeae in an animal model. This
pre-clinical work showed that the recombinant gonococcal protein was immunogenic
in mice. BioChem is evaluating this recombinant gonococcal protein in further
experimental animal models of injection.
HAEMOPHILUS INFLUENZAE
Haemophilus influenzae ("H. influenzae") is a bacterium that is considered
a major human pathogen. There are two types of H. influenzae: the encapsulated
form that has six antigenetically distinct capsular types (types a to f) and the
unencapsulated form (non typeable) that may cause diseases of less virulence
than the encapsulated form. The unencapsulated form is recognized as responsible
for acute respiratory infections, chronic bronchitis, otitis media (40% of all
cases), bacteremia and meningitis (5% of all cases). H. influenzae non typeable
is among the five most common causes of community-acquired pneumonia (between 5%
to 15% of the 500,000 hospital admissions annually in the United States).
Annually, there are typically approximately 4,000 cases of invasive disease in
adults including bacteremic pneumonia (70%), obstetric infections, epiglottis,
meningitis and tracheobronchitis listed to H. influenzae non-typeable. A
conjugate polysaccharide vaccine effective against H. influenzae type B exists
but there is no vaccine currently available against H. influenzae non typeable.
BioChem has identified a membrane surface exposed protein of H. influenzae
that is highly conserved at the surface of various H. influenzae strains.
CliniChem believes that this protein is common and conserved in all the strains
of H. influenzae.
In pre-clinical work, BioChem used its candidate recombinant vaccine to
immunize mice in order to evaluate the protein's ability to confer protection
against H. influenzae bacteria. This pre-clinical work showed that the HI-15
protein used with QuilA as an adjuvant is immunogenic in mice. Vaccination of
mice with the HI-15 recombinant protein enhanced respiratory clearance in an
experimental animal model of pulmonary infection. In a similar experimental
model, intravenous administration of specific antibodies to the HI-15 protein
was also shown to increase respiratory clearance. In a systemic model of
infection, vaccination with the recombinant HI-15 protein conferred protection
against injection of a lethal dose of H. influenzae.
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STREPTOCOCCUS GROUP B
Streptococcus Group B ("Strep B") is classified under seven serotypes based
on their capsular polysaccharide antigenicity and two subtypes based on the
antigenic characteristics of their surface proteins. Strep B causes invasive
disease and is the most common cause of sepsis and meningitis in newborns in the
United States. Two of every 1,000 infants in the United States develop Strep B
infection within the first three months of life. Case fatality rates are
estimated to be between 5% and 20% for newborns and between 15% and 32% for
adults.
In pre-clinical work, BioChem used its candidate recombinant vaccine to
immunize mice in order to evaluate the protein's ability to confer protection
against Strep B bacteria. This pre-clinical work showed that the recombinant
GBS-1 protein is immunogenic and protective in mice. The protein has been
sequenced by BioChem scientists. The presence of the protein has been observed
so far in all serotypes evaluated.
STREPTOCOCCUS PNEUMONIAE
Streptococcus pneumoniae ("S. pneumoniae") infections are among the leading
causes worldwide of illness and death in young children, persons with underlying
debilitating medical conditions, and the elderly. S. pneumoniae infection is a
cause of meningitis, pneumonia and otitis media. S. pneumoniae has 90 different
serotypes. A polysaccharide vaccine against the 23 most common serotypes has
been available since the early 1980s. It is only 60% effective in preventing S.
pneumoniae-caused meningitis and pneumonia and is not currently used to prevent
otitis media. BioChem has discovered two promissing candidate proteins vaccines.
Further work to confirm the protection potential of these proteins is ongoing.
This project is at an early stage.
Each year, S. pneumoniae accounts for three to six thousand cases of
meningitis, 500,000 cases of pneumonia and seven to ten million cases of otitis
media in the United States alone. Case fatality rates vary by age and the
underlying illness of the patient. According to the CDC, the case fatality rates
for some immunocompromised and other high-risk patients have been reported to be
higher than 55% for meningitis and 40% for pneumonia, despite appropriate
antibiotic therapy. In children, S. pneumoniae causes approximately 30% of
otitis media.
CliniChem believes that S. pneumoniae-caused diseases will become more
difficult to effectively manage as strains resistant to antibiotic therapies
become more prevalent. In the past, S. pneumoniae was almost uniformly
susceptible to penicillin, allowing most physicians to treat persons with severe
infections with penicillin alone without testing for antibiotic resistance.
However, since the late 1980s, resistance to penicillin and other antibiotic
agents has spread rapidly. Investigations by CDC of S. pneumoniae-caused
diseases have revealed that, in some areas of the United States, as many as 30%
of disease causing S. pneumoniae strains are not susceptible to penicillin. A
smaller percentage of disease causing S. pneumoniae strains are also resistant
to multiple antibiotic therapies.
CHLAMYDIA PNEUMONIAE
According to 1994 estimates of the American Heart Association,
approximately 57.5 million Americans have one or more forms of cardiovascular
disease, among whom approximately 13.7 million have coronary heart disease and
approximately 3.9 million have strokes. Cardiovascular diseases claimed
approximately 955,000 lives in 1994. Coronary heart disease is most commonly
caused by atherosclerotic narrowing of the coronary arteries. It is likely to
produce angina pectoris, heart attack or both.
Chlamydia pneumoniae ("C. pneumoniae") infections may play a role in
atherosclerosis in heart diseases. The organism is often presented in upper and
lower respiratory tract infections and has been thought recently to contribute
to the process of atherosclerosis. However, substantially more research will be
needed in order to confirm this hypothesis. A vaccine against C. pneumoniae
would offer a viable alternative or supplement to current management of heart
diseases.
BioChem's research program on Chlamydia pneumoniae is at an early stage.
RELIANCE ON COLLABORATIVE RELATIONSHIPS
The Company can make no assurances regarding the future results or
performance of its existing or future agreements and collaborations.
Additionally, there can be no assurance that the Company will be able to
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negotiate other acceptable arrangements in the future or that any existing or
future collaborations will be successful.
There can be no assurance that the collaborators' interests are or will
remain consistent with those of the Company or that they will succeed in
developing any new marketable products or obtaining requisite government
approvals. Should BioChem and its collaborators fail to develop any new
marketable products, obtain the requisite regulatory approvals or market any of
such products successfully, the Company's business, financial condition and
results of operations may be materially and adversely affected. In addition, the
Company cannot control the amount and timing of resources which its
collaborators devote to the Company's programs. Certain of these agreements do
not prevent the collaborators from pursuing alternative technologies that could
result in their developing products competitive with those products developed
under the Company's collaborative agreements. The agreements may be terminated
by the collaborators in certain circumstances with limited notice, and the
collaborators may thereupon acquire certain rights to the products under
development.
MARKETING
Glaxo Wellcome is responsible for all commercial activities for 3TC and
will be responsible for all commercial activities for lamivudine worldwide
except for Canada where 3TC is sold and lamivudine will be sold (if and when it
is approved) by BioChem in partnership with Glaxo Wellcome. The partnership is
responsible for Canadian sales and marketing, with both BioChem and Glaxo
Wellcome allocating sales and marketing personnel to act on behalf of the
partnership. Glaxo Wellcome is responsible for the other activities, such as
distribution and manufacturing, on behalf of the partnership. A similar
arrangement will be made for lamivudine if and when it is approved in Canada.
The Company achieved profitability in 1996 due in large part to Glaxo
Wellcome's successful commercialization of 3TC. The profit growth of the Company
is dependent upon growth in 3TC sales and successful registration and launch of
lamivudine. 3TC has become the cornerstone of combination therapy for the
treatment of HIV/AIDS around the world. The further growth for this product is
dependent in large part on initiating new patients on the therapy, the
competitive situation and the ability of patients and third party payers to pay
for the therapy.
BioChem plans to market and sell certain of its therapeutic products, if
successfully developed and approved, directly in North America and elsewhere
through co-promotion arrangements or other licensing arrangements with third
parties. In North America, in cases where BioChem has sole or shared marketing
rights, it plans to build a small, focused sales force if and when such products
approach marketing approval. Implementation of this strategy will depend on many
factors, including the market potential of any products the Company develops as
well as on the Company's financial resources. To the extent the Company has
entered or will enter into co-promotion or other licensing arrangements,
revenues received by the Company will be dependent on the efforts of third
parties.
The Company markets its diagnostic products through direct marketing
operations in the United States, Germany, Italy, France, Japan, Singapore,
Argentina, the United Kingdom and Canada. The Company also markets its
diagnostic products through a worldwide network of distributors. The Company
currently markets its vaccines only in Canada, Argentina and Spain, primarily
through a direct marketing operation.
MANUFACTURING
Except for the PACIS (BCG therapeutic) product, the Company currently has
no manufacturing facilities for commercial production of any of its therapeutic
products approved or under development. The Company is relying on Glaxo
Wellcome's manufacturing capabilities and resources for the manufacture of 3TC
and lamivudine pursuant to the terms of the agreements entered into with Glaxo
Wellcome. The Company believes that Glaxo Wellcome presently has the facilities
available to manufacture an amount of 3TC and lamivudine to supply sufficient
commercial quantities of the compound.
For the BCH-4556 and BCH-10652 products, the Company is working with
contract manufacturers to supply quantities sufficient to conduct its clinical
trials. The Company also intends to rely on third parties for the commercial
production of these products, if and when approved. For its potential
therapeutic products, the
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Company is looking at reducing the production costs and at improving the
synthetic and purification yields for use on a larger scale in order to conduct
human clinical trials and produce such products for commercial sale at an
acceptable cost. For the BCH-3963, the Company is relying on Astra's
manufacturing capabilities.
The Company currently manufactures its diagnostic products in several
facilities located in Europe and North America. Hematology instruments and
reagents as well as SRI analyzers are manufactured in Allentown, Pennsylvania,
United States in leased facilities. EIA and ELISA kits are manufactured both in
Montreal, Canada as well as in Rome, Italy in owned facilities. LABOTECH,
Personal Lab and ALLERTECH analyzers are manufactured also in Rome, Italy in a
leased facility. SRI reagents and RIA products are manufactured in Rome in an
owned facility.
The Company's vaccine manufacturing, quality control and warehousing
operations are currently located in several leased buildings in Canada and are
approved by the Ministry of Health of Canada. In addition, these premises are
used for the warehousing of vaccine products of other manufacturers which are
distributed by the Company in the Province of Quebec. A portion of these
premises are also used for administrative and research and development purposes.
The Company recently completed a new vaccine production center in Ste-Foy
in the Quebec City area. This new $35 million center has an overall area of
approximately 118,000 square feet and houses new R&D, production,
quality-control laboratories and warehousing as well as administrative offices.
Commercial vaccine production in Ste-Foy is scheduled to start in the first half
of 1998 once its validation process is completed. See "Vaccines." The Company,
when judged more appropriate, intends to rely partly or entirely on strategic
partners' manufacturing and distribution capabilities for some of its vaccines.
In the vaccine and diagnostics areas, the Company must continue to develop,
adapt or acquire the facilities, production technology and technical and
managerial personnel to manufacture products in commercial quantities and in
compliance with applicable quality assurance and environmental and local
government regulations. In the therapeutics area, the Company will have to
develop or acquire the facilities, production technology and technical and
managerial personnel to manufacture products unless it decides to rely
exclusively on third parties for the manufacture of its products. Certain
products that the Company is attempting to develop have never been manufactured
on a commercial scale and there can be no assurance that such products can be
manufactured by the Company or any other party at a cost or in a quantity to
render such products commercially viable. Production of such products may
require the development of new manufacturing technologies and expertise.
PATENTS AND PROPRIETARY INFORMATION
BioChem pursues a policy of seeking patent protection for valuable
patentable subject matter of its proprietary technology. BioChem believes that
patent and trade secret protection is important in its business, and that its
success will depend, in part, on its ability to obtain and enforce strong
patents, to maintain trade secret protection and to operate without infringing
the proprietary rights of others. The Company has certain patents issued and a
number of applications pending in the areas of therapeutics, vaccines and
diagnostics in the United States, most European countries, Canada, Japan and
selected countries worldwide depending on the patent application in question.
No assurance can be given that patents will issue from any pending
applications or that claims now or in the future, if any, allowed under issued
patents will be sufficiently broad to protect the Company's technology. In
addition, no assurance can be given that any patents issued or licensed by the
Company will not be challenged, invalidated, infringed or circumvented, or that
the rights granted thereunder will provide competitive advantages to the
Company. The commercial success of the Company will also depend in part on the
Company not infringing patents or proprietary rights of others and not breaching
the licenses granted to the Company. The degree of patent protection afforded to
pharmaceutical or biotechnological inventions around the world is uncertain. A
number of products important to BioChem are subject to this uncertainty. BioChem
is aware of certain issued patents and patent applications of others, and there
may be other patents and patent applications, containing subject matter which
the Company or its licensees or collaborators may require in order to research,
develop or commercialize certain of the Company's products. There can be no
assurance that the Company will be able to obtain a license to any third-party
technology or patents that it
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may require to conduct its business or that such technology or patents can be
licensed at a reasonable cost. Failure by the Company or its collaborators to
obtain a license to any technology or patents that it may need to commercialize
its technologies or products may result in delays in marketing the Company's
proposed products or the inability to proceed with the development, manufacture
or sale of products requiring such licenses and may have a material adverse
effect on the Company.
BioChem currently has thirteen issued patents in the United States claiming
nucleoside analogs, methods of treatment using nucleoside analogs and processes
for producing these nucleoside analogs. These patents include claims covering
the chemical composition of 3TC, BCH-4556, BCH-10652 and related nucleoside
analogs and methods of treating viral infections, including HIV and hepatitis B,
with 3TC and related nucleoside analogs. BioChem also has issued patents and
pending applications covering 3TC/lamivudine, BCH-4556, BCH-10652 or other
nucleoside analogs, processes for their preparation and methods of using same,
in over 100 countries, including issued patents or pending applications in the
United States, most European countries, Japan, Australia and Canada.
Emory University has filed oppositions to BioChem's examined patent
applications in Europe and Japan which cover 3TC or BCH-4556, related nucleoside
analogs and use of these analogs for treating viral infections. BioChem believes
that these oppositions are unfounded and is vigorously defending its
applications. However, there can be no assurance that BioChem will be successful
in defending the published claims against these oppositions. There is a
possibility that some or all of the claims could be held invalid by the
opposition boards.
On July 23, 1996, Emory University filed a complaint in the United States
alleging infringement by the Company and Glaxo Wellcome Inc., the Company's
exclusive licensee in the U.S. for the Company's patents, patent applications
and know how relating to 3TC, of an Emory University U.S. patent granted that
same day. BioChem considers this patent infringement suit to be without merit
and is vigorously challenging the validity of Emory University's patent. For a
complete discussion of this matter see "Item 3. Legal Proceedings".
Examined patent applications filed by Emory University claiming 3TC
(lamivudine) have been published for opposition in Australia and Japan. BioChem
has filed oppositions in these countries and is currently vigorously opposing
both applications. BioChem is also aware that Emory University has filed patent
applications in other countries, which the Company believes may claim similar
subject matter. BioChem intends to challenge such patent applications; however
there can be no assurance that BioChem will be successful in challenging such
patent applications in all countries where Emory University has sought patent
rights. In the event that the Company were to be unsuccessful in opposing such
patent applications or any patents which may be issued, the Company's business,
financial condition and results of operations could be materially adversely
affected.
In July of 1996 BioChem obtained a United States Patent claiming methods of
treating hepatitis B using 3TC. Vion Pharmaceuticals, Inc. ("Vion"), formerly
known as OncoRx, Inc., a New Haven, Connecticut-based company, had previously
announced that it held exclusive rights to a pending United States patent
application filed by Yale University claiming the use of 3TC in the treatment of
HBV. Should Vion continue to seek a patent for the same subject matter in the
United States, it is possible that an interference may be declared by the United
States Patents and Trademarks Office with BioChem's issued patent. In such a
case, BioChem's position will be as the senior party, but there can be no
assurance that BioChem will be successful. BioChem is not aware of corresponding
patent applications by Yale University or Vion in countries other than the
United States.
BioChem is aware that others, including various universities and
biotechnology companies, have also filed patent applications or have obtained
granted patents in the United States and other countries claiming subject matter
potentially useful or necessary to BioChem's business. Some of these patents and
applications claim specific products or methods of making such products, while
others claim more general processes or techniques useful or now used in the
pharmaceutical and biotechnology industries. With respect to the patents
directed to general processes or techniques, BioChem believes that non-exclusive
licenses have been made available under several of these patents to the industry
for many, but not all, fields of use. The ultimate scope and validity of these
patents and other existing patents or patent applications which may be granted
to third parties in the future, the extent to which the Company may desire or be
required to acquire rights under such
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patents, and the availability and costs of acquiring such rights presently
cannot be determined by BioChem. In the event it is necessary for the Company to
obtain such rights or, if such rights are not available on reasonable terms, the
Company's business, financial condition and results of operations may be
adversely affected. There can be no assurance that others have not obtained or
will not obtain patent protection that will preclude BioChem from
commercializing its products.
Litigation, which could result in substantial cost to the Company, may also
be necessary to enforce any patents issued to the Company or to determine the
scope and validity of other parties' proprietary rights, which may affect the
Company's products and technology. If the outcome of any such litigation is
adverse to the Company, the Company's business could be materially adversely
affected. To determine the priority of invention, the Company may also have to
participate in interference proceedings declared by the United States Patent and
Trademark Office, which could result in substantial cost to the Company.
Under United States patent law, with respect to inventions made prior to
January 1, 1996, a patent is issued to the person who made the invention first,
rather than to the first person to file an application therefor, as is common in
other countries. In determining who is entitled to a United States patent on a
particular technology, acts in the United States prior to January 1, 1996 may be
important. As a result, since the Company conducts substantially all of its
research activities outside of the United States, it is at a disadvantage as to
inventions made prior to January 1, 1996 with respect to obtaining United States
patents, as compared to companies that maintain research facilities in the
United States.
The Company is presently in litigation with Institut Pasteur and Pasteur
Sanofi Diagnostics ("Pasteur"), which have alleged that the marketing of certain
of the Company's diagnostic kits for the detection of HIV infringes Pasteur's
patent rights.
There has been, and the Company believes that there may be in the future,
significant litigation in the industry regarding patent and other intellectual
property rights and that, if the Company becomes involved in such litigation, it
could consume substantial resources. Significant legal issues remain as to the
extent to which patent protection may be afforded in the field of biotechnology
in Canada, the United States and other countries, and the scope of any such
protection has not yet been broadly tested. The Company, therefore, also relies
upon trade secrets, know-how, and continuing technological advancement to
develop and maintain its competitive position. Disclosure and use of the
Company's know-how is generally controlled in part under confidentiality
agreements with the parties involved. In addition, the Company has
confidentiality agreements with its key employees, consultants, officers and
directors. There can be no assurance, however, that all confidentiality
agreements will be honored, that others will not independently develop
equivalent technology, that disputes will not arise as to the ownership of
intellectual property, or that disclosure of the Company's trade secrets will
not occur. Furthermore, there can be no assurance that others have not obtained
or will not obtain patent protection that will exclude the Company from using
its trade secrets and confidential information. BioChem supports and
collaborates in research conducted in universities and in government research
organizations. There can be no assurance that the Company will have or be able
to acquire exclusive rights to inventions or technical information derived from
such collaboration or that disputes would not arise as to rights in derivative
or related research programs conducted by the Company. In addition, in the event
of the Company's contractual breach or bankruptcy, certain of the Company's
collaborative research contracts provide for transfer of technology (including
any patents or patent applications) to the collaborators. See "Significant
Agreements". To the extent that consultants or research collaborators use
intellectual property owned by others in their work with the Company, disputes
may also arise as to the rights to related or resulting know-how or inventions.
COMPETITION
The pharmaceutical and biotechnology industries are characterized by
rapidly evolving technology and intense competition. BioChem anticipates that it
will face increased competition in the future as new products enter the market
and advanced technologies become available. There can be no assurance that
existing products or new products developed by the Company's competitors will
not be more effective, or be more effectively marketed and sold, than any that
may be developed by the Company. Competitive products may render BioChem's
technology and products obsolete and non-competitive prior to the Company's
recovering
24
<PAGE> 25
research, development or commercialization expenses incurred with respect to any
such products. The Company's competitors include major pharmaceutical,
diagnostic, chemical and biotechnology companies, many of which have financial,
technical and marketing resources significantly greater than those of the
Company. Many of the Company's existing or potential competitors, particularly
large pharmaceutical, vaccine and diagnostic companies, also have significantly
greater experience than the Company in undertaking research, preclinical studies
and human clinical trials of new pharmaceutical products, obtaining FDA and
other regulatory approvals, and manufacturing and marketing such products.
Accordingly, the Company's competitors may succeed in commercializing products
more rapidly or effectively than the Company, which could have a material
adverse effect on the Company's business, financial condition or results of
operations.
In addition, many biotechnology companies have formed collaborations with
large, established pharmaceutical companies to support research, development and
commercialization of products that may be competitive with those of the Company.
Academic institutions, government agencies and other public and private research
organizations are also conducting research activities and seeking patent
protection and may commercialize products on their own or through joint
ventures. The Company is aware of certain products manufactured or under
development by competitors that are used for the prevention, treatment or
detection of certain diseases which the Company has targeted for product
development. The existence of these products, or other products or treatments of
which the Company is not aware, or products or treatments that may be developed
in the future, may adversely affect the marketability of products developed by
the Company.
Many pharmaceutical and biotechnology companies, alone and in collaboration
with larger pharmaceutical companies, have developed and are marketing, or are
developing, various products for infectious diseases and cancer. In the field of
HIV infection, many products are currently approved for marketing in the United
States and most have also been approved in Canada, Europe and many other
countries. Medicines for the treatment of HIV infection fall into three
categories: nucleoside analogs reverse transcriptase inhibitors, non-nucleosides
reverse transcriptase inhibitors and protease inhibitors. There are four
nucleoside analogs reverse transcriptase inhibitors on the market, other than
3TC. They are AZT, d4T, ddI and ddC. Two non-nucleosides are approved:
nevirapine and delavirdine. Lastly, there are four protease inhibitors being
marketed: indinavir, saquinavir, ritonavir and nelfinavir. All of these agents
are being used in combination regimens. Market research data from January 1997
(ISIS) indicate that in Canada, Europe and the United States, the majority of
HIV-infected patients on therapy are receiving triple combinations of
antiretroviral agents, while the remaining patients on therapy are prescribed
either double or quadruple combinations.
In the field of chronic hepatitis B therapy, Schering-Plough Corporation
has obtained final approval for and is marketing Intron-A (alpha interferon).
Glaxo Wellcome and Hoffmann-LaRoche also manufacture and market alpha
interferon. The Company is also aware that SmithKline Beecham plc is in Phase
III clinical development for famciclovir, a nucleoside analog which is currently
approved for the treatment of herpes zoster and which is also being developed as
a treatment for chronic hepatitis B infection and for use in liver transplant
patients. Also, SciClone Pharmaceuticals Inc. is developing an immunomodulator
Zadaxin (thymosin alpha-1) which is in Phase III clinical trials for the
treatment of chronic hepatitis B in many countries although the product has been
approved for marketing in several countries. Cytel Corporation is developing a
therapeutic vaccine Theradigm-HBV. Bristol Myers Squibb is developing two
nucleoside analogs: lobucavir and BMS-200,475 for the treatment of chronic
hepatitis B. Another potential competitor is adefovir dipivofil, a nucleoside
analogue in development by Gilead Sciences for hepatitis B, HIV and CMV
infections. The product is currently in Phase III clinical trials for HIV and in
Phase II for HBV. Several other companies are at various stages of research and
development with a broad range of anti-HBV therapeutic approaches, including
nucleoside and nucleotide analogs, therapeutic vaccines, immunomodulators,
cytokines, antisense and other oligonucleotides and ribozymes.
Many biotechnology companies and several pharmaceutical companies with
established vaccine development and marketing programs are researching and
developing vaccine products for infectious diseases. Pasteur Merieux Connaught,
SmithKline Beecham plc, Merck & Co. Inc. and Lederle/American Home Products
Corporation dominate the market for vaccines. These companies have been leaders
in developing classical vaccines and are also developing new generation of
vaccines predominantly to prevent childhood diseases. In
25
<PAGE> 26
the diagnostics market, the Company faces numerous large competitors who have
substantial resources and innovative technologies.
For certain of the Company's potential products, an important factor in
competition may be the timing of market introduction of the Company's or
competitors' products. Accordingly, the relative speed with which BioChem, Glaxo
Wellcome or BioChem's other present and future collaborative partners can
develop products, complete the clinical trials and approval processes, and
supply commercial quantities of the products to the market are key factors for
competitiveness. The Company's competition will be determined in part by the
potential indications for which the Company's products are developed and
ultimately approved by regulatory authorities. The development by competitors of
new treatment methods for those indications for which the Company is developing
products could render the Company's products non-competitive or obsolete. The
Company expects that competition among products approved for sale will be based,
among other things, on product efficacy, safety, reliability, availability,
price and intellectual property protection.
The Company's competitive position also depends upon the success of
clinical trials, obtaining regulatory approvals and its ability to secure market
acceptance of lamivudine. There can be no assurance that lamivudine or any of
the Company's products in development will achieve market acceptance. The degree
of market acceptance will depend upon a number of factors, including the receipt
of regulatory approvals, the establishment and demonstration in the medical
community of the clinical efficacy and safety of the Company's product
candidates, and the establishment and demonstration of the potential advantages
over existing and new treatment methods and reimbursement policies of government
and third-party payors. There can be no assurance that physicians, patients,
payors or the medical community in general will accept and utilize any existing
or new products that may be developed by the Company. Additionally, the
Company's competitive position depends on its ability to attract and retain
qualified personnel, obtain patent protection, or otherwise develop proprietary
products or processes, establish collaborative relationships and secure
manufacturing.
GOVERNMENT REGULATION
Regulation by governmental authorities in Canada, the United States and
other countries is a significant factor in the production and marketing of the
Company's products and in its ongoing research and development activities.
Pharmaceutical and biological products intended for diagnostic, therapeutic
or prophylactic use for humans are governed by the FDA in the United States, by
the HPB in Canada and by comparable agencies in other countries. For most of
these products, the regulations require extensive clinical trials and other
testing and government review and final approval prior to marketing the product.
This procedure is likely to take a number of years and involves the expenditure
of substantial resources. For example, as a general rule, before obtaining
regulatory approval for the commercial sale of any products under development,
the Company must demonstrate through preclinical studies and clinical trials
that the product is safe and efficacious. The results from preclinical studies
and early clinical trials may not be predictive of results obtained in large
scale clinical trials, and there can be no assurance that the Company's or its
collaborators' clinical trials will demonstrate safety and efficacy, achieve
regulatory approvals or result in marketable products. A number of companies in
the biotechnology industry have suffered significant setbacks in advanced
clinical trials, even after achieving promising results in earlier trials. In
addition, government regulations specify standards for manufacturing and
marketing pharmaceutical products. Any failure by the Company or its
collaborators or licensees to obtain, or any delay in obtaining, regulatory
approvals could adversely affect the marketing of any products developed by the
Company and its ability to receive product or royalty revenue. There can be no
assurance that any of the Company's planned products will be approved by the
FDA, HPB or any other governmental agency on a timely basis, if at all.
The Center for Biologics Evaluation and Research in the United States, the
Bureau of Biologics in Canada, and similar agencies in other countries regulate
the manufacturing, marketing and use of vaccines. Product License Applications
and Establishment License Applications or equivalent documentation are required
to be submitted to the governmental authorities for review prior to obtaining
marketing approval. Government regulations specify standards for manufacturing
and marketing vaccines and biological products.
26
<PAGE> 27
These regulations set standards for proof of safety and effectiveness, establish
good manufacturing practices, require inspection of vaccine manufacturing
facilities and require reporting of adverse events to regulatory authorities.
These government authorities also conduct pre-release testing of vaccines and
authorize the sale of each lot of vaccines.
Sales of therapeutic, vaccine and diagnostic products outside Canada and
the United States are subject to regulatory requirements that vary widely from
country to country. Whether or not FDA or HPB approval has been obtained, final
approval of a product by comparable regulatory authorities of other countries
must be obtained prior to the commencement of marketing the product in those
countries. The time required to obtain any such approval may be longer or
shorter than that required for FDA or HPB approval. The expected date of
approval of lamivudine will depend on the decision from the regulatory
authorities whether to review the application in an expedited or normal manner.
The first regulatory filing submission seeking marketing approval of lamivudine
was made in China by BioChem's licensee, Glaxo Wellcome on August 25, 1997
followed by filings in numerous other countries including the countries of the
European Union and Canada in March 1998.
The FDA, HPB and similar agencies in other countries also regulate the
manufacturing, marketing and use of medical devices such as LABOTECH. In the
United States and Canada, diagnostic products are also considered medical
devices and therefore are subject to these regulations. Generally, these
regulations set standards for medical devices, require proof of safety and
effectiveness, establish good manufacturing practices and require inspections of
device manufacturing facilities, and require reporting of device defects to
regulatory authorities. The Company is also subject to various Canadian federal,
provincial, and local laws, regulations, and recommendations relative to safe
working conditions, laboratory and manufacturing practices, and the use and
disposal of hazardous or potentially hazardous substances, including radioactive
compounds and infectious disease agents, used in connection with the Company's
research. The Company may be subject to additional government regulations
resulting from future legislation or administrative action.
PHARMACEUTICAL PRICING AND REIMBURSEMENT
The business and financial condition of diagnostic, pharmaceutical, vaccine
and biotechnology companies will continue to be affected by the efforts of
governments and third-party payors to contain or reduce the costs of healthcare
through various means. For example, in certain foreign markets pricing or
profitability of prescription pharmaceuticals is subject to government control.
In the United States there have been, and the Company expects that there will
continue to be, a number of federal and state proposals to implement similar
government control. In addition, an increasing emphasis on managed care in the
United States has and will continue to increase the pressure on pharmaceutical
pricing. While the Company cannot predict whether such legislative or regulatory
proposals will be adopted or the effects such proposals or managed care efforts
may have on its business, the announcement of such proposals and the adoption of
such proposals or efforts could have a material adverse effect on the Company's
business and financial condition. Further, to the extent such proposals or
efforts have a material adverse effect on other pharmaceutical companies that
are prospective corporate partners for the Company, the Company's ability to
establish a strategic alliance may be adversely affected. In addition, in
Canada, the United States and elsewhere, sales of prescription pharmaceuticals,
vaccines and diagnostic products are dependent, in part, on the availability of
reimbursement to the consumer from third-party payors, such as government and
private insurance plans. Third-party payors are increasingly challenging the
prices charged for medical products and services. To the extent the Company
succeeds in bringing products to market, there can be no assurance that these
products will be considered cost-effective and that reimbursement to consumers
will be available or will be sufficient to allow the Company to sell its
products on a competitive basis.
TECHNOLOGY
Except for 3TC, the Company's potential therapeutic products, including
lamivudine for use as a treatment against chronic hepatitis B, are in research
or development. The Company is devoting its efforts to the research and
development of potential therapeutic, vaccine and diagnostic products based upon
various technological approaches. The development of new products is subject to
a number of significant risks. Potential products that appear to be promising in
various stages of development may not reach the market for
27
<PAGE> 28
a number of reasons. Such reasons include the possibilities that the potential
product will be found ineffective or unduly toxic during preclinical or clinical
trials, will fail to receive necessary regulatory approvals, will be difficult
to manufacture in a large scale, will be uneconomical to market or not achieve
market acceptance, or will be precluded from commercialization by proprietary
rights of third parties. Competitive products may render BioChem's technology
and products obsolete and non-competitive prior to potential products reaching
the market. Most of the Company's potential products will require significant
additional research and development efforts and significant additional
preclinical and clinical testing, prior to any commercial use. There can be no
assurance that the Company will successfully address any of these technological
challenges, or others that may arise in the course of development.
PRODUCT LIABILITY
The use of any of the Company's potential products in clinical trials, and
the sale of any approved products, may expose the Company to liability claims
resulting from the use of its products. These claims might be made directly by
consumers, healthcare providers or by pharmaceutical companies or others selling
such products. The Company currently has liability insurance which does not
exclude product liability claims with respect to sales of therapeutic,
diagnostic and vaccine products. No assurance can be given that the Company will
be able to maintain insurance coverage at a reasonable cost or in sufficient
amounts to protect the Company against losses due to liability. There can also
be no assurance that the Company will be able to maintain or obtain additional
commercially reasonable product liability insurance for any products approved
for marketing. A successful product liability claim or a series of claims
brought against the Company could have a material adverse effect on its
business, financial condition or results of operations.
INTERNATIONAL OPERATIONS
Most of the Company's diagnostic product sales are made, and the Company
expects that they will continue to be made, in international markets. The
Company also expects that most of its therapeutic products will be sold in
international markets. Sales of the Company's products in international markets
are subject to certain risks common to such sales, including government
regulation, export and import license requirements, risks of tariffs or trade
barriers and political and economic instability. Although these risks have not
had any material effect on the Company to date, there can be no assurance these
risks will not materially adversely affect the Company in the future.
The Company generally prices its diagnostic products, and currently expects
to price any therapeutic products, in the currency of the country in which they
are sold. Accordingly, the prices of such products in Canadian dollars will vary
as the value of the Canadian dollar fluctuates against such local currencies. In
addition, royalty payments to be made to BioChem by Glaxo Wellcome on 3TC and
lamivudine sales worldwide (excluding Canada) will be made as a percentage of
sales of 3TC and lamivudine denominated in the currency of the country where
sales are made. There can be no assurance that there will not be increases in
the value of the Canadian dollar against such currencies, reducing the Canadian
dollar return to the Company on the sales of its products. Furthermore, there
can be no assurance that significant fluctuations in foreign currency values
will not occur that will create sufficient differences in the relative prices of
the products in different countries, such that the Company or Glaxo Wellcome
will find it necessary to reduce its prices in certain local currencies in order
to bring the relative cost of its products into line. As at December 31, 1997,
the Company did not utilize any foreign currency hedging instruments.
EMPLOYEES
As at December 31, 1997, the Company had a total of 797 employees divided
as follows: Therapeutic 144 employees; ImmunoSystems, 491 employees; Vaccines,
109 employees; and BioChem 53 employees. NAVA employs 260 employees.
ITEM 2. DESCRIPTION OF PROPERTIES
The Company and its subsidiaries own and lease space for research,
development, manufacturing, marketing and administrative purposes. The Company's
corporate headquarters, administration and therapeutic operations are currently
located in one owned facility in Laval, Quebec, Canada, totaling 150,000 square
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<PAGE> 29
feet. Vaccines' operations are located in three leased facilities in Laval,
Quebec, Canada, totaling 30,000 square feet. New and owned vaccines
manufacturing, research and development and office facilities having an overall
area of approximately 118,000 square feet were recently completed in Sainte-Foy,
Quebec, Canada. See "Vaccines" and "Manufacturing" in Item 1. ImmunoSystems is
located in a 22,000 square-foot owned facility located in Montreal, Quebec,
Canada, a 7,000 square foot owned facility in Laval, Quebec, Canada and a 70,000
square-foot owned facility in Rome, Italy. ImmunoSystems also leases nine
facilities totaling 238,246 square feet in seven different countries: Italy,
United States, Germany, Switzerland, France, the United Kingdom and Singapore.
ITEM 3. LEGAL PROCEEDINGS
On July 23, 1996, Emory University ("Emory") filed a complaint in the
United States District Court for the Northern District of Georgia, alleging
infringement of Emory's U.S. Patent Number 5,539,116 (the " '116 patent") by the
Company and Glaxo Wellcome Inc., the Company's exclusive licensee in the U.S. to
the Company's patents, patent applications and know how relating to 3TC. Emory
University v. Glaxo Wellcome Inc. and BioChem Pharma Inc., Civil Action No.
1:96-CV-1868 GET (N.D. Georgia). Emory alleged that the Company is infringing
the '116 patent through its relationship with Glaxo Wellcome and by inducing and
facilitating Glaxo Wellcome's sales and offers for sale of 3TC in the U.S. Emory
requested a jury trial.
The Company filed its Answer, Affirmative Defenses and Counterclaims on
October 15, 1996, denying Emory's allegations of patent infringement and
asserting in its affirmative defenses that Emory's '116 patent is invalid and
not infringed by the Company. The Company also asserted in its Counterclaims:
(1) a request for a declaratory judgment that the '116 patent is invalid and not
infringed; (2) a claim that Emory and Dr. Raymond Schinazi, an Emory professor,
misappropriated BioChem's trade secrets relating to the Company's 3TC patent;
and (3) a claim that Emory and Dr. Schinazi have committed unfair competition,
commercial disparagement and deceptive trade practices through
misrepresentations to the public, financial analysts and others in the financial
community. The Company requested a jury trial of the issues raised by its
affirmative defenses and counterclaims.
Emory and Dr. Schinazi denied the allegations in BioChem's counterclaims.
On June 5, 1997, Glaxo Wellcome filed a motion for summary judgment that
the '116 patent is invalid for lack of a written description and as obvious. The
Company submitted a brief in support of this motion. After the motion was fully
briefed, the Court denied the motion on July 14, 1997.
After completing discovery, BioChem elected to dismiss counts (2) and (3)
of its counterclaims. The parties agreed to a Stipulated Order of Dismissal,
which the Court entered on February 5, 1998.
Glaxo Wellcome filed three motions for summary judgment on January 15,
1998. The Court denied Glaxo Wellcome's motion for summary judgment that the
'116 patent is invalid for lack of a written description as required by 35
U.S.C. para.112, but has not yet ruled on the other two motions for summary
judgment that the '116 patent is invalid because: (a) it does not state a
practical utility for the claimed invention as required by 35 U.S.C. para.101;
and (b) it was not timely filed as required by 35 U.S.C. para.135(b).
The pretrial order in this case is scheduled to be filed within 30 days of
the Court's ruling on the last of these motions for summary judgment, and trial
will begin after the pretrial order has been filed.
Although complex litigation always involves risks and uncertainties, the
Company believes that it is likely ultimately to prevail following the trial or
any appeal in this action. However, there can be no assurances that this action
will be resolved favorably to the Company or in a timely manner. If the Company
does not prevail in this litigation, the Company's business, financial condition
and results of operations may be materially adversely affected.
On October 2, 1997, Emory filed an Application in the Federal Court of
Australia of New South Wales District Registry General Division alleging that
BioChem's Australian Patent No. 630,913, covering 3TC, is invalid and seeking an
order revoking BioChem's patent. The Company filed a defense denying Emory's
allegations on February 17, 1998 and will vigorously defend its patent.
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<PAGE> 30
BioChem is not a party to any other material litigation. See "Patents and
Proprietary Information" in Item 1.
ITEM 4. CONTROL OF REGISTRANT
As far as known to BioChem, it is not directly or indirectly owned or
controlled by another corporation or by any government and no shareholder
directly or indirectly owned more than 10% of the Company other than Glaxo
Wellcome Inc.
The principal shareholders are as of March 31, 1998:
<TABLE>
<CAPTION>
COMMON SHARES
NAME OF BENEFICIAL OWNER OWNED PERCENTAGE
------------------------ ------------- ----------
<S> <C> <C>
Glaxo Wellcome Inc. ........................................ 15,850,880 14,64%
7333 Mississauga Road North
Mississauga, Ontario, Canada
L5N 6L4
Caisse de depot et placement du Quebec...................... 7,428,610 6,86%
Fonds de solidarite des travailleurs du Quebec (F.T.Q.)..... 5,023,692 4,64%
Officers and directors as a group........................... 4,142,192 3,82%
---------- -----
32,445,374 29,96%
========== =====
</TABLE>
ITEM 5. NATURE OF TRADING MARKET
The common shares have been authorized for quotation in the United States
on the Nasdaq National Market since March 20, 1991, and are traded under the
symbol "BCHE." The common shares are traded in Canada on The Montreal Exchange
and The Toronto Stock Exchange under the symbol "BCH". The following table sets
forth, for the periods indicated, the range of high and low closing sales prices
of the common shares on The Montreal Exchange (the Company's principal
non-United States exchange) and the Nasdaq National Market.
<TABLE>
<CAPTION>
THE MONTREAL
EXCHANGE NASDAQ (U.S.$)
------------------------ ------------------------
HIGH LOW HIGH LOW
--------- --------- --------- ---------
<S> <C> <C> <C> <C>
1996
First Quarter....................................... 35.75 24.69 26.19 18.07
Second Quarter...................................... 34.45 22.75 25.07 16.69
Third Quarter....................................... 27.63 17.75 20.25 13.00
Fourth Quarter...................................... 34.50 26.08 25.50 19.13
1997
First Quarter....................................... 41.05 29.50 30.38 21.50
Second Quarter...................................... 34.75 22.40 25.25 16.00
Third Quarter....................................... 44.10 28.05 31.75 20.25
Fourth Quarter...................................... 44.15 29.50 32.00 20.50
</TABLE>
The following table indicates, as of March 31, 1998, the approximate total
number of holders of record of common shares, the total number of common shares
outstanding, the number of holders of record of common shares with United States
addresses, the portion of the outstanding common shares held in the United
States, and the percentage of common shares held in the United States:
<TABLE>
<CAPTION>
TOTAL NUMBER TOTAL NUMBER OF PORTION OF COMMON PERCENTAGE OF
OF HOLDERS COMMON SHARES NUMBER OF U.S. SHARES HELD IN COMMON SHARES
OF RECORD(1) OUTSTANDING HOLDERS OF RECORD(2) THE U.S.(2) HELD IN THE U.S.
------------ --------------- -------------------- ----------------- ----------------
<S> <C> <C> <C> <C>
239 108,275,690 109 64,983,238 60%
</TABLE>
- ------------
(1) A substantial number of the common shares are held by depositories,
brokerage firms and financial institutions in "street name". Based upon the
number of annual reports and proxy statements requested by such nominees,
management of the Company estimates
30
<PAGE> 31
that the total number of beneficial holders of common shares is approximately
15,400 holders of which approximately 8,500 could be United States residents.
(2) The computation of the portion of common shares held in the United States
is based upon the number of holders of record with United States addresses.
United States residents may beneficially own common shares owned of record
by non-United States residents.
On February 9, 1998, the Company announced its intention to issue a
dividend-in-kind to its shareholders. The Company plans to distribute, by way of
dividend, the Class A Common Shares of CliniChem Development Inc. ("CliniChem")
to which capital, the Company will contribute $150 million. CliniChem was formed
for the purpose of conducting the clinical development of certain therapeutic
and vaccine products of BioChem with the goal of commercializing such products.
The clinical development activities will be contracted by CliniChem to BioChem.
BioChem holds an option to acquire commercialization rights with respect to
individual products on a country-by-country basis, as well as an option to
purchase all of the outstanding CliniChem Class A Common Shares at a price to be
set according to a predetermined formula.
The Company has not paid any cash dividends since its inception. The
Company currently does not intend to pay any cash dividends in the foreseeable
future but intends to retain any future earnings to finance its development and
growth. The Company's dividend policy will be reviewed periodically depending on
the Company's financial position and on other factors.
The market prices for the securities of biopharmaceutical and biotechnology
companies, including BioChem, have historically been highly volatile, and the
market has from time to time experienced significant price and volume
fluctuations that are unrelated to the operating performance of particular
companies. Factors such as fluctuations in the Company's operating results,
announcements of technological innovations or new therapeutic products by the
Company or its competitors, clinical trial results, governmental regulation,
developments in patent or other proprietary rights, public concern as to safety
of drugs developed by the Company or others and general market conditions can
have an adverse effect on the market price of the Common Shares. In particular,
the realization of any of the risks described herein could have a material
adverse impact on such market price.
ITEM 6. EXCHANGE CONTROLS AND OTHER LIMITATIONS AFFECTING HOLDERS
OF COMMON SHARES
There is no law or governmental decree or regulation in Canada that
restricts the export or import of capital, or affects the remittance of
dividends, interest or other payment to a non-resident holder of common shares,
other than withholding tax requirements. See "Item 7. Taxation".
There is no limitation imposed by Canadian law or by the Articles or other
charter documents of the Company on the right of a non-resident to hold or vote
common shares, other than as provided by the Investment Canada Act (Canada) (the
"Investment Act") as amended by an Act to implement the Agreement establishing
the World Trade Organization (Canada) (the "WTO Implementation Act"). The
following summarizes the principal features of the Investment Act for
non-residents who propose to acquire common shares.
Under the Investment Act, an investment by an individual, a government or
an agency thereof or an entity that is not a "Canadian" (as defined in the
Investment Act) (a "non-Canadian") may be subject to certain notification
requirements or review by the minister responsible for the administration of the
Investment Act (the "Minister"). Except as set forth below, an investment in
common shares by a non-Canadian would be reviewable under the Investment Act if
(i) such investment constitutes an acquisition of direct control of the Company
where the value of the assets of the Company is at least five million dollars,
or an acquisition of indirect control of the Company where the value of the
assets of the Company is at least fifty million dollars, or (ii) the Federal
cabinet is of the opinion that an investment that constitutes an acquisition of
control is related to Canada's cultural heritage or national identity. All
investments subject to review require that the Minister be satisfied that the
investment is likely to be of net benefit to Canada.
Pursuant to the WTO Implementation Act, an investment made by a WTO
Investor (as defined in the Investment Act) (a "WTO Investor") in common shares
would be reviewable under the Investment Act if such investment constitutes an
acquisition of direct control of BioChem and the value of the assets of
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<PAGE> 32
BioChem is at least $179 million. An indirect acquisition of control by a WTO
Investor is no longer subject to review.
The Investment Act states that a non-Canadian shall acquire control or
shall be deemed to acquire control if he acquires a majority of the common
shares. An acquisition of less than a majority but more than one-third of the
common shares will be presumed to be an acquisition of control unless it can be
established that, upon the acquisition, the Company is not in fact controlled by
the acquiror through the ownership of common shares.
The notification requirements which would be applicable in the event of a
proposed acquisition of control not otherwise subject to review require the
potential investor to supply certain information concerning the proposed
investment prior to the consummation thereof. However, the Federal cabinet
retains the right to require the review of any such proposed investment that is
related to cultural heritage and national identity if, within a specified
period, the Federal cabinet considers it in the public interest on the
recommendation of the Minister to issue an order for the review of the
investment.
In certain limited circumstances transactions are exempt from both the
review and notification requirements of the Investment Act, including the
acquisition of common shares by a person in the ordinary course of that person's
business as a trader or dealer in securities.
ITEM 7. TAXATION
A holder of the Company's common shares who resides in the United States
will not be subject to tax under the Income Tax Act (Canada) on capital gains
realized on the disposition of such common shares unless they are deemed to be
"taxable Canadian property". Such common shares will be deemed to be taxable
Canadian property if they are used by the non-resident holder in carrying on a
business in Canada or if, at any time during the five year period immediately
preceding the disposition, 25% or more of the Company's outstanding securities
of any class were owned by such holder, or any group consisting of such holder
and persons with whom such holder did not deal at arms' length. If the Company's
shares are deemed to be "taxable Canadian property" to shareholders residing in
the United States, with any resulting capital gain realized on the disposition
of such shares subject to tax in Canada, the gain will be exempt from tax in
Canada under the tax treaty between Canada and the United States, provided that
the shares do not form part of the business property of a permanent
establishment or fixed base through which the United States shareholder carries
on business or performs independent personal services in Canada.
Dividends paid on the Company's common shares held by shareholders residing
in the United States will be subject to Canadian withholding tax. Under the tax
treaty between Canada and the United States, a withholding rate of 5% is
applicable to corporations resident in the United States, who do not have a
permanent establishment in Canada, and who are beneficial owners of at least 10%
of the voting stock of the Company. Under the same treaty, a withholding rate of
15% is applicable to corporations resident in the United States, who do not have
a permanent establishment in Canada, and with a beneficial ownership of less
than 10% in the voting stock of the Company, and to individuals.
ITEM 8. SELECTED FINANCIAL DATA
The following selected consolidated financial data of the Company are
qualified by reference to and should be read in conjunction with the
consolidated financial statements, related notes thereto and other financial
data included elsewhere herein. In 1994, the Company changed its fiscal year end
from January 31 to December 31. The consolidated statement of earnings data for
the years ended December 31, 1995, 1996 and 1997 are derived from, and are
qualified by reference to, the audited consolidated financial statements
included elsewhere in this document. The consolidated statement of earnings data
for the years ended January 31, 1994 as well as December 31, 1994 are derived
from the audited consolidated financial statements not included herein. The
consolidated balance sheet data for the year ended December 31, 1996 and 1997
are derived from, and are qualified by reference to, the audited consolidated
financial statements included elsewhere in this document. The consolidated
balance sheet data for the years ended January 31, 1994 as well as December 31,
1994 and 1995 are derived from the audited consolidated financial statements not
included herein.
32
<PAGE> 33
<TABLE>
<CAPTION>
(in thousands of dollars except per share information)
YEARS ENDED
--------------------------------------------------------------
1994-01-31 1994-12-31 1995-12-31 1996-12-31 1997-12-31
---------- ---------- ---------- ---------- ----------
(12 MONTHS) (11 MONTHS) (12 MONTHS) (12 MONTHS) (12 MONTHS)
<S> <C> <C> <C> <C> <C>
CONSOLIDATED STATEMENT OF EARNINGS DATA:
Operating Revenue
Sales...................................... $32,015 $97,630 $162,470 $156,941 $134,641
Royalties.................................. 1,872 5,181 12,596 57,062 124,130
Research and development contracts......... 4,992 4,099 6,569 2,782 4,004
Interest................................... 2,824 1,378 2,976 13,008 12,285
Other...................................... 493 1,351 2,780 3,825 5,722
--------- --------- --------- ---------- ----------
Total Operating Revenue............. 42,196 109,639 187,391 233,618 280,782
--------- --------- --------- ---------- ----------
Expenses
Cost of sales 15,429 50,217 74,241 75,759 67,450
Selling and administrative................. 13,223 36,998 58,486 62,968 72,480
Milestone repayments....................... -- -- 1,825 4,552 --
Research and development................... 11,715 15,967 22,087 32,186 37,387
Financial.................................. 1,066 3,801 8,649 7,527 5,863
Depreciation and Amortization.............. 3,032 6,199 13,042 11,457 11,092
--------- --------- --------- ---------- ----------
Total Expenses...................... 44,465 113,182 178,330 194,449 194,272
--------- --------- --------- ---------- ----------
Earnings before income taxes and other....... (2,269) (3,543) 9,061 39,169 86,510
Income taxes................................. (1,410) (3,647) (5,443) (1,451) (2,064)
Non-controlling interest..................... (145) (85) (484) (211) 1,987
Share of loss of an affiliated company, net
of gain on dilution........................ (5,888) (6,881) (8,101) (4,113) (6,595)
--------- --------- --------- ---------- ----------
Net income (loss)............................ (9,712) (14,156) (4,967) 33,394 79,838
========= ========= ========= ========== ==========
Earnings (loss) per common share............. (0.11) (0.15) (0.05) 0.31 0.74
========= ========= ========= ========== ==========
Weighted average number of common shares
outstanding................................ 92,343,360 93,055,518 97,044,458 106,485,028 108,152,816
========= ========= ========= ========== ==========
</TABLE>
QUARTERLY CONSOLIDATED FINANCIAL INFORMATION (UNAUDITED) FOR THE COMPANY IS
AS FOLLOWS:
<TABLE>
<CAPTION>
(in thousands of dollars except per share information)
YEAR ENDED DECEMBER 31, 1996
-------------------------------------------------------------
4TH 3RD 2ND 1ST
QTR QTR QTR QTR
------------- ------------- ------------- -------------
<S> <C> <C> <C> <C>
Sales revenue..................... $ 37,851 $ 37,690 $ 41,052 $ 40,348
Total operating revenue........... 64,965 60,809 56,936 50,908
Earnings (loss) before certain
items(1)........................ 12,217 13,201 9,788 3,963
Net income........................ 19,908 7,961 4,097 1,428
Earnings per common share......... 0.18 0.08 0.04 0.01
<CAPTION>
(in thousands of dollars except per share information)
YEAR ENDED DECEMBER 31, 1997
-------------------------------------------------------------
4TH 3RD 2ND 1ST
QTR QTR QTR QTR
------------- ------------- ------------- -------------
<S> <C> <C> <C> <C>
Sales revenue..................... $ 33,035 $ 32,014 $ 34,978 $ 34,614
Total operating revenue........... 74,742 69,329 73,369 63,342
Earnings (loss) before certain
items(1)........................ 25,076 19,767 23,476 18,191
Net income........................ 25,187 20,508 21,516 12,627
Earnings per common share......... 0.23 0.19 0.20 0.12
</TABLE>
- ---------------
(1) Earnings before income taxes, non-controlling interest and share of loss of
an affiliated company.
33
<PAGE> 34
<TABLE>
<CAPTION>
(in thousands of dollars)
AS AT AS AT AS AT AS AT AS AT
JANUARY 31, DECEMBER 31, DECEMBER 31, DECEMBER 31, DECEMBER 31,
1994 1994 1995 1996 1997
--------------- --------------- --------------- --------------- ---------------
<S> <C> <C> <C> <C> <C>
CONSOLIDATED BALANCE SHEET DATA:
Working capital........................ $ 60,848 $ 73,601 $ 102,466 $ 362,742 $ 365,283
Total assets........................... 144,892 245,240 285,220 572,265 655,272
Long-term debt, excluding current
portion.............................. 14,003 80,126 69,662 57,706 58,269
Shareholders' equity................... 105,691 99,343 134,594 415,832 498,068
</TABLE>
SUMMARY OF DIFFERENCES BETWEEN GENERALLY ACCEPTED ACCOUNTING PRINCIPLES ("GAAP")
IN CANADA AND IN THE UNITED STATES
<TABLE>
<CAPTION>
(in thousands of dollars except per share information)
YEARS ENDED
-------------------------------------------------------------------------------
1994-01-31 1994-12-31 1995-12-31 1996-12-31 1997-12-31
------------- --------------- ------------- ------------- -------------
(12 months) (11 months) (12 months) (12 months) (12 months)
<S> <C> <C> <C> <C> <C>
CONSOLIDATED STATEMENT OF EARNINGS:
Net income (loss) -- Canadian GAAP............ $ (9,712) $ (14,156) $ (4,967) $ 33,394 $ 79,838
Deferred foreign exchange gains (losses) on
long-term debt.............................. -- (652) 2,023 324 (3,649)
Realization of foreign currency translation
adjustment.................................. -- -- 701 -- --
Deferred income taxes......................... -- -- (533) (204) 984
------------- --------------- ------------- ------------- -------------
Net income (loss) -- U.S. GAAP................ (9,712) (14,808) (2,776) 33,514 77,173
============= =============== ============= ============= =============
Earnings (loss) per common share -- U.S. GAAP
Primary.............................. (0.11) (0.16) (0.03) 0.31 0.71
============= =============== ============= ============= =============
Fully-diluted........................ (0.11) (0.16) (0.03) 0.31 0.70
============= =============== ============= ============= =============
</TABLE>
For a complete discussion of this matter see Note 21 to the Consolidated
Financial Statements annexed hereto.
34
<PAGE> 35
ITEM 9. MANAGEMENT'S DISCUSSION AND ANALYSIS OF FINANCIAL CONDITION AND RESULTS
OF OPERATIONS
OVERVIEW
BioChem Pharma Inc. ("BioChem" or the "Company") is an international
biopharmaceutical company engaged in the research, development, manufacturing
and marketing of innovative products for the prevention, detection and treatment
of human diseases.
For BioChem, 1997 was a remarkable year with net income more than doubling,
reaching $79.8 million or $0.74 per share, compared to $33.4 million or $0.31
per share for the year ended December 31, 1996. For the year ended December 31,
1995 the Company's net loss amounted to $5.0 million or $0.05 per share. The
continued growth of the Company is largely attributable to the steady stream of
royalty revenues on increasing worldwide sales of 3TC, a drug for the treatment
of HIV infection and AIDS, marketed under the brand name Epivir in most markets.
In addition, 3TC is a component with AZT, of the combination tablet, marketed
under the brand name Combivir, to date only available in the United States. For
the year ended December 31, 1997 worldwide sales of 3TC amounted to $973.3
million (U.S.$703.0 million). Furthermore, the Company's commitment to move
research forward and to advance the development of products in the pipeline will
contribute to continued growth in the future. Confirming this commitment, the
Company posted a record level of research and development expenses of $37.4
million for the year ended December 31, 1997.
Through BioChem's asset and liability management function, the Company
maintains a disciplined approach to the management of liquidity, capital and
overall financial stability. As at December 31, 1997, the Company's cash and
temporary investments amounted to $310.4 million, total assets amounted to
$655.3 million and shareholders' equity amounted to $498.1 million. This
illustrates BioChem's favorable positioning to explore exciting long-term growth
opportunities in order to further strengthen the Company's position as a leader
in the biopharmaceutical field.
FINANCIAL ANALYSIS
OPERATING REVENUE
OPERATING REVENUE for 1997 reached $280.8 million, an increase of $47.2
million or 20%, compared to the preceding year. In 1996, operating revenue
amounted to $233.6 million, compared to $187.4 million in 1995. These increases
are due to the increase in royalty revenue.
The distribution of operating revenue by industry segments demonstrates the
importance of the royalty revenue from worldwide sales of 3TC on the Company's
overall operating revenue. In fact, the therapeutic industry segment, which
includes royalty revenue on sales of 3TC, contributed 50% of the Company's
overall operating revenue in 1997, compared to 28% and 9% in 1996 and 1995
respectively. The diagnostic industry segment contributed 42% of the Company's
operating revenue in 1997, compared to 62% in 1996 and 85% in 1995.
Diagnostic product SALES amounted to $114.5 million in 1997, $141.3 million
in 1996 and $156.9 million in 1995. These decreases are mainly due to the strong
competition in the hematology products sector of the diagnostics industry as
well as the negative effect of currency fluctuations on the conversion of
foreign sales. Sales of vaccines amounted to $5.9 million in 1997, compared to
$7.1 million in 1996 and $5.6 million in 1995. Higher sales in 1996 were
attributable to sales of measles vaccines and international sales of influenza
vaccines. Therapeutic product sales amounted to $14.2 million in 1997, compared
to $8.5 million in 1996, the Company's first year of therapeutic product sales
in Canada. These sales represent the Company's share, pursuant to the
partnership with Glaxo Wellcome for the commercialization of 3TC in Canada.
ROYALTY REVENUE more than doubled during 1997 and amounted to $124.1
million, an increase of $67.0 million, compared to the preceding year. In 1996
royalty revenue was $57.1 million, compared to $12.6 million in 1995. These
increases are due to royalties received from Glaxo Wellcome on sales of 3TC
worldwide. In 1997 the worldwide sales of 3TC amounted to $973.3 million
(U.S.$703.0 million), of which $28.4 million were in Canada, $543.5 million
(U.S.$392.6 million) in the United States, $279.2 million (U.S.$201.6 million)
in Western Europe and $122.2 million (U.S.$88.3 million) in the rest of the
world. In 1996 the worldwide sales of 3TC were $429.3 million (U.S.$314.8
million).
35
<PAGE> 36
INTEREST INCOME amounted to $12.3 million in 1997, a decrease of $0.7
million or 5%, compared to the preceding year. In 1996, interest income amounted
to $13.0 million, compared to $3.0 million in 1995. The decrease in 1997
compared to 1996 is reflective of the decrease in interest rates during 1997.
The 1996 increase compared to 1995 was mainly due to a higher average cash
balance resulting from the February 1996 offering of common shares, which
produced net proceeds of $238.9 million.
OTHER REVENUE amounted to $9.7 million, an increase of $3.1 million or 47%,
compared to the preceding year. In 1996, other revenue amounted to $6.6 million,
compared to $9.3 million in 1995. Other revenue includes mainly revenue from
research and development contracts in addition to distribution and grant
revenue. The increase in 1997 is due to higher activity in research and
development contracts which generated increased revenue as well as management
fees earned from GeneChem Technologies Venture Fund, L.P. (see Review of
Operations -- Therapeutic). The decrease in 1996 compared to 1995 was mainly due
to a decrease in revenue from research and development contracts.
EXPENSES
COST OF SALES as a percentage of sales amounted to 50%, 48% and 46% for
1997, 1996 and 1995 respectively. These increases reflect the strong competition
in the hematology products sector of the diagnostics industry, resulting in
decreased selling prices.
SELLING AND ADMINISTRATIVE EXPENSES amounted to $72.5 million in 1997, an
increase of $9.5 million or 15%, compared to the preceding year. In 1996 selling
and administrative expenses amounted to $63.0 million, compared to $58.5 million
in 1995. The increases in 1997 and 1996 are attributable to the increased
activity of the Company, and in particular legal fees related to the Company's
ongoing intellectual property protection. As a percentage of operating revenue,
selling and administrative expenses were respectively 26%, 27% and 31% in 1997,
1996 and 1995.
MILESTONE REPAYMENTS represent amounts payable to Glaxo Wellcome pursuant
to the agreement for the development and marketing of 3TC. These repayments were
due as royalties were earned on 3TC sales, at the rate of 50% of these
royalties, to a maximum of 3.0 million British pounds sterling ($6.4 million).
The final balance, amounting to $4.6 million, was repaid in 1996 and repayments
of $1.8 million were made in 1995.
RESEARCH AND DEVELOPMENT EXPENSES, net of related tax credits, amounted to
$37.4 million in 1997, an increase of $5.2 million or 16%, compared to the
preceding year. In 1996, the research and development expenses amounted to $32.2
million, compared to $22.1 million in 1995. These increases resulted mainly from
therapeutic operations. The distribution of these expenses amongst the different
operations, in 1997, is as follows; 69% related to therapeutic operations, 20%
related to vaccine operations and 11% related to diagnostic operations. In 1996
the distribution was as follows; 66% related to therapeutic operations, 13%
related to vaccine operations and 21% related to diagnostic operations. For
1997, 1996 and 1995, the research and development expenses were respectively
13%, 14% and 12% of operating revenue.
FINANCIAL EXPENSES amounted to $5.9 million in 1997, a decrease of $1.6
million or 21%, compared to the preceding year. In 1996, these expenses amounted
to $7.5 million, compared to $8.6 million in 1995. The decrease in 1997 is due
to lower average debt compared to 1996 in addition to operating exchange gains
realized, which are presented as a reduction of financial expenses. The decrease
in 1996, compared to 1995 was attributable to operating exchange gains realized
during 1996.
INCOME TAX expense amounted to $2.1 million in 1997 compared to $1.6
million in 1996. The Company is a multinational enterprise which consolidates
its accounts for reporting purposes but files separate tax returns for each
subsidiary in the various jurisdictions. Because the Company's tax strategy is
to optimize its tax position worldwide, the Company may not realize the benefit
of its deferred tax assets, which assets are principally derived from losses
experienced by the Canadian-based parent and carried forward. The Company and
other subsidiaries have accumulated tax losses but their use against future
income is uncertain due to ongoing tax losses created by the research and
development programs of the Group. Due to the uncertainty when, if ever, the
accumulated tax losses may be used to offset future taxable income, the deferred
tax assets have been almost fully offset by income tax valuation allowances.
36
<PAGE> 37
EARNINGS
The Company posted NET INCOME of $79.8 million or $0.74 per share in 1997,
compared to $33.4 million or $0.31 per share in 1996 and a net loss of $5.0
million or $0.05 per share in 1995. These improvements are due to the increase
in royalty revenue on sales of 3TC.
The therapeutic industry segment contributed $84.4 million to the Company's
overall net income in 1997, compared to a net income of $29.5 million in 1996
and a net loss of $2.4 million in 1995. These increases are attributable to
royalty revenue on sales of 3TC, as previously discussed. The diagnostic
industry segment posted a $1.9 million net loss in 1997, compared to a net
income of $2.0 million and a net income of $4.6 million in 1996 and 1995
respectively. These decreases for the diagnostic industry segment reflect the
strong competition in the hematology products sector of the diagnostics
industry. However, the introduction of new products in 1997 in addition to a
more focused target market should improve this situation in the future. The
vaccine industry segment posted a net loss of $5.3 million in 1997, compared to
a net loss of $0.6 million in 1996 and a net income of $0.1 million in 1995.
This results from the substantial funding that is currently being required for
the development of promising new vaccine candidates. The research and
development expenses in the vaccine industry segment amounted to $7.5 million
for the year ended December 31, 1997, compared to $4.2 million for the year
ended December 31, 1996 and $2.6 million for the year ended December 31, 1995.
LIQUIDITY AND FINANCIAL POSITION
For the year ended December 31, 1997 OPERATING CASH FLOW amounted to $97.2
million, compared to $48.5 million for the year ended December 31, 1996 and
$14.5 million for the year ended December 31, 1995. These changes in operating
cash flow are directly attributable to the increases in net income. Operating
cash flow represents the cash flows generated from net income, excluding
revenues and expenses not affecting cash, principally depreciation, amortization
and share of loss of an affiliated company.
As at December 31, 1997 the Company posted TOTAL ASSETS of $655.3 million,
compared with $572.3 million as at December 31, 1996. This increase is mainly
due to an increase in capital assets and investments. The increase in capital
assets is attributable to the construction of a vaccine development, production
and headquarters facility. The increase in investments is mainly due to the
Company's strategic investments in Scriptgen Pharmaceuticals, Inc., Apoptosis
Technology, Inc., GeneChem Technologies Venture Fund, L.P. and Biovector
Therapeutics SA (see Review of Operations).
WORKING CAPITAL amounted to $365.3 million as at December 31, 1997,
compared with $362.7 million the previous year. Working capital ratios were
5.46:1 as at December 31, 1997 and 5.66:1 as at December 31, 1996.
As at December 31, 1997, the Company's SHAREHOLDERS' EQUITY amounted to
$498.1 million which translates into a common equity ratio of 90% as at December
31, 1997, compared to 88% as at December 31, 1996.
OTHER
During 1997, the Company generated revenues and incurred expenses in the
following currencies and proportions:
<TABLE>
<CAPTION>
REVENUES EXPENSES
-------- --------
<S> <C> <C>
U.S. dollars................................................ 45% 31%
Canadian dollars............................................ 15% 28%
Italian lira................................................ 15% 24%
British pounds sterling..................................... 15% 6%
Other....................................................... 10% 11%
</TABLE>
Since inception, the Company has financed research and development,
operations and investment activities from public and private sales of equity,
revenue from research and development contracts, sale of products, interest
revenue, bank loans and more recently and more significantly royalty revenue.
37
<PAGE> 38
In February 1998, BioChem announced the formation of a new company,
CliniChem Development Inc. ("CliniChem"). This company was formed for the
purpose of continuing the research and development of a number of therapeutic
and vaccine candidates, initially discovered or in-licensed by BioChem, with the
goal of commercializing such products. CliniChem will contract with BioChem to
perform all such activities. BioChem will hold an option to acquire
commercialization rights with respect to individual products developed and will
also hold an option to purchase all of the outstanding common shares of
CliniChem at any time, but no later than March 31, 2003. BioChem will
contribute, from current cash resources, $150.0 million to CliniChem as a
capital contribution. Shares of CliniChem will then be distributed to the
shareholders of BioChem as a dividend-in-kind. At the time of the capital
contribution, BioChem will record an investment in CliniChem of $150 million.
Under Canadian generally accepted accounting principles ("GAAP"), BioChem will
charge the carrying value of the distribution to retained earnings on the date
of the declaration of the distribution. Under U.S. GAAP, BioChem will charge the
fair market value of the distribution to retained earnings and will expense the
excess of the carrying value of its investment in CliniChem common shares over
the fair market value of these shares. The fair market value of the CliniChem
class A common shares will be determined by BioChem based on their closing price
on relevant stock exchanges on the distribution date. This difference between
the Canadian and U.S. GAAP treatment of the distribution will be disclosed in a
reconciling note to BioChem's financial statements. BioChem will recognize as
revenue the payments from CliniChem under a Research and Development Agreement
between the parties and the research and development costs incurred by BioChem
to perform its obligations under the Research and Development Agreement will be
expensed as research and development expenses under Canadian and U.S. GAAP.
Biopharmaceutical product development programs, particularly at the
clinical development stage, require the investment of substantial resources. The
CliniChem distribution should enable BioChem's short-term results to continue to
reflect principally the established therapeutic, vaccine and diagnostic
businesses. This distribution also separates the risks associated with
conducting the CliniChem programs from those associated with BioChem's
established businesses. By exercise of BioChem's product options, it should be
possible for BioChem to capture a greater return on the products developed
within CliniChem than would otherwise be possible from products developed for
commercialization with third parties.
Based on current operating budgets, the management of BioChem believes that
the resources of the Company are sufficient for current requirements. The
Company's future requirements will depend on several factors, as discussed in
the section "Outlook".
REVIEW OF OPERATIONS
THERAPEUTICS
BioChem's discovery, 3TC (marketed under the brand name Epivir in most
markets) is the cornerstone of combination therapy for the treatment of HIV
infection and AIDS and has become the most prescribed antiretroviral therapy
worldwide. As at December 31, 1997 3TC is available in 80 countries with
worldwide sales in 1997 totalling $973.3 million (U.S.$703.0 million). In
November 1995, the U.S. Food and Drug Administration ("FDA") approved 3TC for
use in the United States. This was followed by the approval from the Canadian
Health Protection Branch in December 1995 for use in Canada and subsequently in
numerous other countries during 1996 and 1997. Furthermore, in September 1997,
the FDA approved, for use in the United States, Combivir the first tablet to
combine two antiretroviral drugs, 3TC and AZT, in a single tablet. In November
1997, the European Union's Committee for Proprietary Medicinal Products
recommended the approval of Combivir to the European Commission, which has the
final decision-making authority. Regulatory filings have also been made in
several other countries.
During 1997, the first regulatory filings were made by Glaxo Wellcome
seeking approval of BioChem's discovery, lamivudine, a product for the treatment
of chronic hepatitis B. With the first product approvals expected in 1998,
lamivudine is anticipated to be an important contributor to the Company's future
revenue growth.
The Company receives royalties on sales of 3TC and will receive royalties
on the future sales of lamivudine when approval is received, by virtue of a
collaborative agreement signed in 1990 with Glaxo, now Glaxo Wellcome. The
agreement covers the development and marketing of 3TC for the treatment of HIV
38
<PAGE> 39
infection and lamivudine for the treatment of hepatitis B infection. Under the
terms of this agreement, Glaxo Wellcome assumes responsibility for developing
these products with the goal of obtaining the necessary approvals from the FDA
and from other similar regulatory authorities around the world. Presently, Glaxo
Wellcome manufactures and markets 3TC worldwide, with the exception of Canada,
where the Company and Glaxo Wellcome entered into a partnership to market and
sell 3TC. Glaxo Wellcome holds approximately 15% of the Company's shares as at
December 31, 1997.
In July 1996, Emory University ("Emory") filed legal proceedings in the
United States against BioChem and Glaxo Wellcome for alleged patent infringement
regarding 3TC and is seeking monetary damages. The U.S. patent granted in 1996
to Emory does not affect BioChem's original patent, which was granted in 1991.
The Company believes that Emory's patent is invalid and, with Glaxo Wellcome, is
vigorously challenging this action in court.
The year 1997 can be considered a success for the Company's therapeutic
operations. In the cancer research area, BCH-4556, a novel nucleoside analogue
to treat cancer, continues to progress through the development process with
three Phase I trials ongoing and Phase II trials anticipated to begin in the
middle of 1998. In addition, the Company continues to devote resources to HIV
research and plans to file an Investigational New Drug application, in Canada in
the first quarter of 1998, seeking authorization to begin clinical trials with
BCH-10652, a novel nucleoside analogue to treat HIV infection and AIDS.
Furthermore, several research and development collaborations have been signed
and strategic investments made with the goal to further develop the therapeutic
business segment.
In February 1997, BioChem and OSI Pharmaceuticals, Inc. ("OSI"), formerly
Oncogene Science, Inc., announced an expansion of their research, development
and marketing collaboration where the two companies will pursue additional viral
targets in the areas of HIV infection and hepatitis C. The original agreement
signed in 1996, calling for each company to assign a team of researchers, is for
a period of five years and the marketing rights will be shared equally between
the two companies. Also during 1996, the Company acquired common shares of OSI
for consideration totalling $6.2 million.
In March 1997, BioChem announced a total subscription of $30.0 million in
GeneChem Technologies Venture Fund, L.P. ("GeneChem"), a new $100.0 million fund
established to invest in academic projects and early-stage companies involved in
genomics and related technologies. The Company has invested $6.0 million in
GeneChem as at December 31, 1997. GeneChem will operate for a term of ten years
and is managed by a subsidiary of BioChem.
In August 1997, BioChem and Apoptosis Technology, Inc. ("ATI"), a 95% owned
subsidiary of ImmunoGen, Inc., a publicly traded company, announced a
collaboration in the area of cancer. The agreement grants BioChem an exclusive,
worldwide license to ATI's proprietary screens based on proteins involved in
apoptosis, or programmed cell death. BioChem is responsible for the development
of all products arising from the collaboration and will retain exclusive
worldwide rights. In addition, the Company will invest in ATI in order to
finance the research activities over a minimum three year period, making
milestone payments for each product over the course of development and will pay
royalties to ATI on worldwide sales of the resulting products. As at December
31, 1997, the Company has invested $3.9 million in ATI.
In December 1997, BioChem and Scriptgen Pharmaceuticals, Inc. ("Scriptgen")
concluded a license agreement which gives BioChem exclusive rights to drug
candidates in Scriptgen's hepatitis B and dimerescent receptor research
programs. Scriptgen will be responsible for all aspects of drug discovery and
BioChem will be responsible for preclinical and clinical development, seeking
regulatory approval and retaining worldwide commercialization rights. In
addition, BioChem invested U.S.$20.0 million in Scriptgen, representing 20% of
the equity in this privately-held company, in addition to receiving five-year
warrants for an additional 5% of Scriptgen's equity.
During 1996, agreements were signed with Vertex Pharmaceuticals, Inc. and
Unimed Pharmaceuticals, Inc. under which the Company has acquired the marketing
rights, for Canada, of certain products in clinical development.
The Company also has a strategic collaboration with Astra AB ("Astra"),
under a 1992 agreement covering the research and development of pain control
compounds pioneered by BioChem. This agreement
39
<PAGE> 40
calls for Astra to pay BioChem an initial milestone payment, to undertake the
research and development expenses and to pay milestone payments to BioChem once
the compound(s) reach certain agreed-upon development milestones. Development
and commercialization efforts will be carried out principally by Astra. The
Company will receive royalties on the eventual sales of products arising from
this collaboration. During the first quarter of 1998, an IND filing by Astra is
anticipated in Europe, seeking to begin Phase I clinical trials for the pain
control agent known as BCH-3963.
Therapeutic research and development is conducted by BioChem Therapeutic
Inc., a wholly-owned subsidiary.
VACCINES
During 1997, BioChem, through its subsidiary BioChem Vaccines Inc.
(formerly IAF BioVac Inc.) moved into the new $35 million vaccines development,
production and headquarters facility. Once licensed for manufacturing, this
facility will place BioChem in a position to manufacture our currently marketed
vaccines at this new location and to scale up manufacturing for BioChem's
vaccine candidates in development. The facility, expected to be fully functional
in 1998, has been financed through capital injections from the Company and a
shareholder, Sofinov, Societe financiere d'innovation inc., through loans and
grants from government agencies and a bank loan.
In November 1997, BioChem announced the approval from Canadian regulatory
authorities to proceed with Phase II/III clinical trials of its novel
cell-culture based influenza vaccine. This new cell-culture vaccine
manufacturing technology once approved, will allow BioChem to produce the
vaccine more rapidly and at a lower cost and, in the case of a pandemic, to
manufacture the vaccine in greater volume with less lead time.
In May 1997, BioChem and Biovector Therapeutics SA("Biovector"), a
privately-held French company specializing in drug and vaccine delivery
technologies, concluded an agreement aimed at developing novel human vaccines
for nasal administration. BioChem will develop a nasally-delivered vaccine using
Biovector's technology and will give priority to the development of a
nasally-delivered vaccine against influenza. In exchange for the right to use
Biovector's vaccine delivery technology and rights to commercialize the vaccines
incorporating this technology, BioChem has taken a 6.6% equity interest in
Biovector for $5.6 million, will oversee product development and registration
costs for the vaccines involved, and will pay Biovector royalties on sales. A
nasally-delivered, egg-derived influenza vaccine candidate is anticipated to
begin Phase I clinical trials during the first half of 1998.
In 1995, the Company concluded an agreement with the Vaccines Research Unit
of the Laval University Hospital Research Center ("CRCHUL") for the development
of new vaccines for the prevention of infections such as bacterial meningitis
and bacterial pneumonia. Under the agreement, extending to December 1998,
BioChem will fund the Vaccines Research Unit of CRCHUL. In return, the Company
retains the intellectual property rights on new vaccines discovered and
developed and will pay royalties on eventual sales of these products. A second
quarter 1998 IND filing is planned for a recombinant protein vaccine to protect
against Neisseria meningitidis infection.
Research, development, production and marketing of vaccines is conducted by
BioChem Vaccines Inc., a 75% owned subsidiary.
In 1990, BioChem acquired an interest in the affiliated company, North
American Vaccine, Inc. ("NAVA"). As at December 31, 1997, BioChem owned 11.2
million common shares and 1.0 million preferred shares each convertible into two
common shares and, therefore, the equivalent of 13.2 million common shares or
36.7% of NAVA. As at December 31, 1997, the market value of the Company's
investment in NAVA, based on the closing market price at the balance sheet date,
amounted to $470.1 million.
DIAGNOSTICS
BioChem has launched two new instruments, the Personal Lab and the Spirit,
which are expected to contribute to increased revenue in the future. With these
two new instruments, BioChem's diagnostic division has focused attention on the
immunoassay and hematology markets.
40
<PAGE> 41
In 1991, the Company expanded the diagnostic operations by acquiring a 70%
interest in each of IFCI CloneSystems S.p.A. and Chemila S.p.A., two Italy-based
companies. In 1992, the Company reorganized its diagnostic operations by
transferring all diagnostic operations, including its investments in IFCI
CloneSystems S.p.A. and Chemila S.p.A., to its subsidiary, BioChem ImmunoSystems
Inc. ("ImmunoSystems"). In 1992, ImmunoSystems acquired an additional 29% of
these Italy-based companies, thereby increasing the ownership in each of these
companies to 99% of their share capital. The consideration for this additional
investment was paid through an issuance of ImmunoSystems' shares.
In 1994, ImmunoSystems acquired 100% of the share capital of Ares
Diagnostics (Holdings) B.V. and its subsidiaries which was the diagnostics
business unit of the Ares-Serono Group of Geneva, Switzerland. The purchase
price of $84.7 million was financed through a $24.7 million balance of purchase
price, bank loans of $39.2 million and a loan from BioChem to ImmunoSystems for
$20.8 million.
In 1996, the Company and Nippon Shoji Kaisha Ltd. ("NSK") concluded an
agreement for exclusive distribution, in Japan, of certain products of the
Company's diagnostic products subsidiary. NSK also received a 50% share of the
Japanese division of this diagnostic products subsidiary.
During 1997, the Company proceeded with the merger of the three Italian
operating subsidiaries into one subsidiary. This merging will stream-line the
operations and is expected to add value to the diagnostics business.
Research, development, manufacturing and marketing of diagnostic products
is conducted by BioChem ImmunoSystems Inc., a 91% owned subsidiary.
OUTLOOK
BioChem's objective is to further assume a leadership role in the research
and development of innovative new therapeutic, vaccine and diagnostic products
that will address significant medical needs. This objective, as well as the
objectives of increased revenue and profitability, will be achieved through
expansion of existing businesses, acquisitions and research and development
collaborations. In particular, in the area of therapeutics, the numerous
collaborations and strategic investments, as discussed earlier, attest to
BioChem's strong involvement in new discoveries, especially in the areas of
antivirals and anticancer. Furthermore, the state-of-the-art vaccine development
and production facility as well as the higher level of vaccine research and
development expenses during 1997 demonstrate the commitment to the vaccine
industry segment. In the area of diagnostics, BioChem's newest instrumentation
together with a more focused target market should position this industry segment
for future growth.
The Company believes that it has laid a foundation for sustainable
long-term growth. 3TC is the cornerstone of HIV combination therapy and is now
the most frequently prescribed drug for HIV therapy worldwide. The Company
believes that the next impetus for growth in the anti-HIV therapy market and for
3TC should come from earlier treatment of persons living with HIV who are
diagnosed and not yet on treatment. This should be facilitated by the
introduction of new drugs into the market that are as potent, easy to administer
and well-tolerated, as 3TC. The Company believes that lamivudine should become
the standard of care for the treatment of chronic hepatitis B and that this
should provide a further stage of growth for revenues and profit. Finally the
Company's therapeutic and vaccines research and development pipelines are
starting to bring new products into clinical trials, showing the promise for
long-term growth.
The future performance of BioChem is dependent upon a number of factors
including royalty revenue, product sales levels, initiation or termination of
collaborative agreements, research and development programs and timely
regulatory approvals for various products. It should be further noted with
respect to royalty revenue, that the royalties received are based on the level
of product sales by the licensee, over which the Company has no control.
Significant funding is required for ongoing research and development,
clinical trials, commercial manufacture of the products and the establishment of
sales and marketing teams necessary for the launch and ongoing sales of new
products. In addition, major financial resources are necessary until such time
as the products are developed and sold successfully and sales are sufficient to
generate profits.
41
<PAGE> 42
Product research and development involves a high degree of risk, and
returns to investors are dependent upon successful development of the Company's
products. There can be no assurance that development of any product will be
successfully completed or that regulatory approval of any of the Company's
products under development will be obtained. Furthermore, there can be no
assurance that existing products or new products developed by BioChem's
competitors will not be more effective, or more effectively marketed and sold,
than any that may be developed by the Company.
Because of the length of time and expense associated with bringing new
products through development and regulatory approval to the marketplace, the
Company places considerable importance on obtaining and ensuring patent and
trade secret protection for its significant discoveries. There can be no
assurance that any pending patent application filed by the Company will mature
into issued patents. Furthermore, there can be no assurance that the Company's
existing or pending patent claims will offer protection against competition, or
will not be designed around or infringed upon by others. The outcome of the
legal proceedings initiated by Emory University against the Company and Glaxo
Wellcome for alleged patent infringement could or could not have a significant
impact on the Company.
The Company, amongst all other companies worldwide, is exposed to the risks
and uncertainties associated with the Year 2000 problem, where a computer may
erroneously interpret the year "2000" as "1900". BioChem is currently in the
process of evaluating the potential impact relating to the Year 2000 issue. The
Company is assessing both internal and external risks associated with the Year
2000. More specifically, the internal risks include mainly computers hardware
and software, diagnostic instrumentation and other electronic equipments.
External risks relate to the Company's relationship with third party such as
major suppliers and strategic collaborators. This assessment, which is expected
to be completed shortly, will determine the Company's action plan to rectify any
issues. The Company expects that any conversion required will be complete before
the year 2000. Presently, the Company does not believe that compliance will
result in material investments, nor does BioChem anticipate that this problem
will have material adverse effects on the business operations or financial
performance. However, there can be no assurance that this problem will not
adversely affect the Company and its business.
The Company believes that cash, temporary investments and long-term
investments, together with funds provided by operations, will be sufficient to
meet operating cash requirements including development of existing and new
products through internal research and development activities, selective product
in-licensing, research and development collaborations, capital expenditures and
long term debt repayment. Furthermore, funds provided by operations should
increase in the future mainly due to an increase in royalty revenue from
worldwide sales of 3TC as well as the potential royalties on sales of
lamivudine, assuming regulatory approvals are obtained. The emerging products
from the Company's research and development pipeline will also contribute to
achieving this increase.
Worldwide changes in health-care policies are an ongoing source of
challenge not only for BioChem, but for other pharmaceutical and
biopharmaceutical companies. In general, the pressure to contain health-care
costs worldwide is an ongoing source of uncertainty and challenge.
In the past, the market price of the Company's shares have been subject to
significant volatility. The expectations of securities analysts about the
Company's financial or scientific results could have a significant effect on the
trading price of the Company's shares.
42
<PAGE> 43
ITEM 10. DIRECTORS AND OFFICERS OF THE COMPANY
DIRECTORS
The name, municipality of residence and position with the Company of each
of the directors and their respective holding of Common Shares of the
Corporation owned, controlled or directed as at March 31, 1998 are presented
below:
<TABLE>
<CAPTION>
NUMBER OF VOTING
DIRECTOR SHARES OWNED OR
NAME AND MUNICIPALITY OF RESIDENCE POSITION SINCE CONTROLLED
---------------------------------- -------- -------- ----------------
<S> <C> <C> <C>
Francesco Bellini, Ph.D (1)(3)............ Chief Executive Officer and 1986 2,883,600
Town of Mount-Royal, Quebec Director
Bernard Canavan, M.D.(1).................. Director 1997 --
Tequesta, Florida
Gervais Dionne, Ph.D (1).................. Executive Vice-President, Research 1991 877,752
Saint-Laurent, Quebec and Development and Director
Jean-Louis Fontaine (1)................... Chairman of the Board 1986 273,760
Westmount, Quebec
Jean-Francois Formela (3)................. Director 1997 --
Boston, Massachusetts
The Honorable James A. Grant, P.C., Q.C. Director 1986 2,000
(1)(3)..................................
Westmount, Quebec
Roderick L. Henry (2)(4).................. Director 1992 4,000
Westmount, Quebec
Jacques R. Lapointe (5)................... President and Chief Operating 1998 --
Hudson, Quebec Officer and Director
Guy Lord, (2)(4).......................... Vice-Chairman of the Board of 1989 2,500
Westmount, Quebec Directors
Paul N. Lucas (4)......................... Director 1995 800
Oakville, Ontario
Michel Perron, (2)........................ Director 1993 14,000
Westmount, Quebec
Guy Savard (2)(3)......................... Director 1995 --
Outremont, Quebec
</TABLE>
- ------------
(1) Member of the Executive Committee.
(2) Member of the Audit Committee.
(3) Member of the Human Resources and Compensation Committee.
(4) Member of the Corporate Governance Committee.
(5) Since 1986, Mr. Lapointe was President and Chief Executive Officer of Glaxo
Canada Inc. until 1994 when he took over as Managing Director and Chairman
of Glaxo Wellcome UK Limited. In 1995, he became Regional Director for Glaxo
Wellcome plc with responsibilities for Australia, New Zealand and South
Africa, and in 1996, he was appointed Business Development and Information
Systems Director for Glaxo Wellcome plc with responsibilities for Global
Commercial Development, OTC and Information Systems worldwide.
43
<PAGE> 44
OFFICERS
The name, municipality of residence and position held of each of the
officers of the Company are presented below:
<TABLE>
<CAPTION>
NAME AND MUNICIPALITY OF RESIDENCE POSITION
---------------------------------- --------
<S> <C>
Frederick J. Andrew......................... Chief Financial Officer
Morin Heights, Quebec
Greg Arnsdorff.............................. President of BioChem ImmunoSystems Inc.
Montreal, Quebec
Francesco Bellini, Ph.D..................... Chief Executive Officer and Director
Town of Mount-Royal, Quebec
Alan DeSousa................................ Vice-President, Corporate Finance
Saint-Laurent, Quebec
Gervais Dionne, Ph.D........................ Executive Vice-President Research and
Saint-Laurent, Quebec Development and Director
Michael G. Grey............................. President of BioChem Therapeutic Inc.
Town of Mount-Royal, Quebec
Daniel Hetu, M.D. .......................... Vice-President, Corporate Development
Outremont, Quebec
Jacques R. Lapointe......................... President and Chief Operating Officer and
Hudson, Quebec Director
Francois Legault............................ Executive Vice-President, Investments, and
Outremont, Quebec Subsidiaries
Christine Lennon............................ Vice-President, Corporate Communications
Montreal West, Quebec
Charles-A. Tessier.......................... Vice-President Legal Affairs and Corporate
Ile-Bizard, Quebec Secretary
Claude H. Vezeau............................ President of BioChem Vaccines Inc.
Sillery, Quebec
</TABLE>
FREDERICK J. ANDREW, joined BioChem in 1997 as Chief Financial Officer.
Prior to joining BioChem, he was Vice-President and Treasurer of BCE Inc. from
1991 to 1997, Corporate Treasurer of Bell Canada from 1984 to 1991 and occupied
various positions within the BCE Inc. group of companies from 1964 to 1984. Mr.
Andrew received a B.A. in economics from York University in 1964.
GREG ARNSDORFF joined the Company in September 1997 as the President of
BioChem ImmunoSystems Inc. Prior to joining the Company, Mr. Arnsdorff was with
Abbott Laboratories' Diagnostic Division since 1981, in his last role from 1994
as Director, Abbott Diagnostics Canada. Mr. Arnsdorff holds a Bachelor of
Science in Medical Technology from Armstrong State College, Savannah, Georgia.
FRANCESCO BELLINI, PH.D., a co-founder of the Company, joined the Company
as President and Chief Executive Officer in September 1986. From 1984 to
September of 1986, Dr. Bellini was the Director of the Biochemicals Division at
the Institut Armand-Frappier, and from 1968 to 1984, he was a research scientist
with Ayerst Laboratories. Dr. Bellini is Vice-Chairman of the Board of NAVA and
is a director of Molson Companies, Societe Generale de Financement, and Uniforet
Inc. Dr. Bellini received in 1972 a B.Sc. in chemistry from Loyola College in
Montreal, and a Ph.D. in chemistry from the University of New Brunswick in 1977.
BERNARD CANAVAN, M.D., is a retired executive of American Home Products
Corporation where he worked from 1969 to 1994 and was its President and Chief
Operating Officer from 1990 until his retirement in 1994. Mr. Canavan received
in 1960 an M.B. Ch.B. and has a Bachelor of Medicine and Surgery from the
University of Edinburgh.
44
<PAGE> 45
ALAN DESOUSA joined the Company as Director of International Taxation in
1994. Prior to joining the Company, he was a senior corporate tax consultant
with Ernst & Young which he joined in 1988. Mr. DeSousa practiced as a chartered
accountant with Arthur Andersen from 1981 to 1986, and in his own firm from 1986
to 1988. Mr. DeSousa received a Bachelor of Commerce in accounting and finance
and a Graduate Diploma in Public Accountancy from McGill University in 1981 and
1982 respectively. He was admitted as a Chartered Accountant to the Ordre des
Comptables Agrees du Quebec in 1984.
GERVAIS DIONNE, PH.D., a co-founder of the Company, joined the Company as
Vice-President, Research and Development, in 1986. From 1985 to 1986, he was the
Chemical Products Director at the Institut Armand-Frappier, and from 1984 to
1985, he was a Group Leader Research Scientist with Bio-Mega Inc. From 1976
until 1984, Dr. Dionne was a research scientist with Ayerst Laboratories. Dr.
Dionne is chairman of Briana Bio-Tech Inc. and a director of Scriptgen
Pharmaceuticals Inc. and of NAVA. Dr. Dionne received a B.Sc. in chemistry from
the University of Montreal in 1971 and a Ph.D. in organic chemistry from Laval
University in 1976.
JEAN-LOUIS FONTAINE is Chairman of the Board of Directors. He has been a
director of the Company since 1986. Mr. Fontaine also serves as the
Vice-Chairman of Bombardier Inc. He was a Vice-President with Bombardier Inc.
from June 1977 until August 1988. Bombardier Inc. is engaged in the design,
development, manufacturing and marketing of transportation equipment, civil and
military aerospace products and motorized consumer products. Mr. Fontaine is
Chairman of the Board of l'Universite de Sherbrooke and is also a director of
AXA Insurance Inc. and Heroux Inc. Mr. Fontaine received a B.Sc. in mechanical
engineering from the University of Sherbrooke in 1963, and an M.B.A. from the
University of Western Ontario in 1977.
JEAN-FRANCOIS FORMELA, M.D., has been the General Partner of Atlas Venture
Fund III, L.P. since 1993 and was previously the Senior Director, Medical
Marketing and Scientific Affairs for Schering-Plough U.S., which he joined in
1989. Mr. Formela graduated in 1984 as a medical doctor from the Ecole de
medecine de l'Universite de Paris and received an M.B.A. in 1989 from the
Columbia Business School.
THE HONORABLE JAMES A. GRANT, P.C., Q.C. has been a director of the Company
since 1986. He is a partner with the law firm of Stikeman, Elliott and has been
with that firm since 1962. He is a director of United Dominion Industries Ltd,
CAE Industries Ltd., and a Canadian bank. Mr. Grant received a B.A. in arts in
1958 and a B.C.L. in law in 1961, both from McGill University.
MICHAEL G. GREY joined the Company as President of BioChem Therapeutic Inc.
in 1994. Prior to joining the Company, he was Senior Vice-President, Corporate
Development of Titan Pharmaceuticals, Inc. and President of Ansan Inc. Prior to
that, he held a number of positions in Glaxo from 1974 to 1993, including
Vice-President, Corporate Development of Glaxo Inc. Mr. Grey received a B.Sc. in
chemistry from the University of Nottingham in 1974.
RODERICK L. HENRY has been a director of the Company since 1991. He is the
President of Henrod Investments Inc., an investment company. Mr. Henry was the
Chairman and Chief Executive Officer of Wire Rope Industries, a manufacturer of
wire rope. He also serves as a director of CAE Industries Ltd, Atlas Copco
Canada Ltd, Westroc Industries Ltd. and Brome Lake Ducks Ltd.
DANIEL HETU, M.D., joined the Company as Vice-President, Corporate
Development in 1995. Prior to joining the Company, he was a Vice-President,
Investment Banking with Burns Fry Inc. (now Nesbitt Burns Inc.) which he joined
in 1987. Mr. Hetu received an M.D. from Sherbrooke University in 1979 and an MBA
from Ecole des Hautes Etudes Commerciales in Montreal in 1987.
JACQUES R. LAPOINTE joined the Company on May 4, 1998 as President and
Chief Operating Officer. Prior to joining the Company, he was with Glaxo
Wellcome, since 1986 as President and Chief Executive Officer of Glaxo Canada
Inc., then from 1994 as Managing Director and Chairman of Glaxo Wellcome UK
Limited, then for Glaxo Wellcome plc as Regional Director with responsibilities
for Australia, New Zealand and South Africa until October 1996 when he took over
as Business Development and Information Systems Director with responsibilities
for Global Commercial Development, OTC and Information Systems worldwide. Mr.
Lapointe has a B. Commerce and MBA (Finance) from Concordia University.
45
<PAGE> 46
FRANCOIS LEGAULT joined the Company in 1987 as Vice-President, Finance and
Treasurer, then became the Executive Vice-President, Finance, Administration and
Treasurer until September 1997 when he was named Executive Vice-President,
Investments and Subsidiaries. Prior to joining the Company, he was Finance
Director of Societe Quebecoise des Transports from 1984 to 1987, and was a
chartered accountant with Coopers & Lybrand from 1978 to 1984. Mr. Legault
received a BAA. in business and accounting from Ecole des Hautes Etudes
Commerciales in Montreal in 1978 and was admitted as a Chartered Accountant to
the Ordre des Comptables Agrees du Quebec in 1980.
CHRISTINE LENNON, joined the Company as Director, Investor Relations in
1994. Prior to joining the Company, she held several marketing and sales
positions within Sandoz Canada Inc. (now Novartis) from 1987 to 1994. Ms. Lennon
received a B.Sc. -- Joint Honors from McGill University in 1986 where she also
obtained her MBA in 1994.
GUY LORD has been a director of the Company since 1989 and he also has been
a partner with the law firm of Desjardins Ducharme Stein Monast since 1993 and
was with the law firm of Clark Lord Rochefort Fortier from 1989 to 1993. Prior
to that, Mr. Lord was a partner and National Director of Research in Taxation
with the accounting firm of Samson Belair/Deloitte & Touche from 1986 to 1989.
Mr. Lord is a director of Novicourt Inc. Mr. Lord received a B.A. in 1959 from
the University of Montreal, a law degree in 1962 from the University of Montreal
and a D. Phil. from Oxford University in 1969.
PAUL N. LUCAS has been a director of the Company since 1995. He has been
President and Chief Executive Officer of Glaxo Wellcome Inc. (formerly Glaxo
Canada Inc.) since 1994. Prior to that he held a number of positions in Glaxo
Canada Inc. from 1986 to 1994 including Executive Vice-President and Chief
Operating Officer, Senior Vice-President Corporate Marketing and Vice-President
Marketing. Mr. Lucas received a B.Sc. Hon. in 1972 from Queen's University.
MICHEL PERRON has been a director of the Company since 1993. He is Chairman
and Chief Executive Officer of Somiper Inc., an investment company. Mr. Perron
was Chairman and Chief Executive Officer of Uniforet Inc., a lumber business,
and was also President and Chief Executive Officer of Normick Perron Inc., a
lumber business, until 1990. Mr. Perron is a director of Natcan Trust, and a
Canadian bank. Mr. Perron received a degree in Commerce from St-Jerome College,
Kitchener, Ontario.
GUY SAVARD has been a director of the Company since 1995. In February 1995,
he was appointed President -- Quebec, Vice-Chairman and director of Midland
Walwyn Capital Inc. and director of Midland Walwyn Inc. From 1990 to January
1995, he was President, Chief Operating Officer and Director of Caisse de depot
et placement du Quebec. Mr. Savard is also a director of COBEPA S.A.,
Industrial-Alliance Life Insurance Company, Reno-Depot inc., Ritvik Toys Inc.,
and the Business Development Bank of Canada. Mr. Savard is a Fellow of l'Ordre
des Comptables Agrees du Quebec. He graduated from l'Universite Laval with a
Bachelor of Commerce, a Master's degree in Commercial Sciences and Accounting
Sciences. He perfected his management training at Harvard University in Boston.
CHARLES-A. TESSIER joined the Company as Vice-President, Legal Affairs and
Corporate Secretary in 1996. Prior to joining the Company, he was practicing
commercial law in his own law firm from 1980 to 1988, and from 1988 until 1996,
he was Vice-President, Secretary and General Counsel of DMR Group Inc., a
multinational company in information technology. Mr. Tessier received a B.A. in
Administration in 1976 and a law degree in 1979 from the University of Ottawa.
He is a member of the Barreau du Quebec and the Canadian Bar Association.
CLAUDE H. VEZEAU, PHARM.D., joined the Company as President of BioChem
Vaccines Inc. in 1996. Prior to joining the Company, Dr. Vezeau was
Vice-President, Scientific Affairs of BioCapital Inc. and held a number of
positions in Searle Canada Inc. including Director of Corporate Affairs, Quebec,
from 1990 to 1995. Dr. Vezeau received a B.Sc. in pharmacy from the University
of Montreal in 1976 and a Pharm.D. from the University of Minnesota in 1979.
All members of the Board of Directors hold office until the next annual
meeting of shareholders or the election of their successors. Executive officers
serve at the discretion of the Board of Directors. There are no family
relationships among any of the directors and executive officers of the Company.
46
<PAGE> 47
The Executive Committee consists of five directors who are elected annually
by the Board of Directors. The Executive Committee may exercise all of the
powers of the Board of Directors in respect of the management and direction of
the business affairs of the Company between meetings of the Board of Directors,
subject to certain restrictions under the Canada Business Corporations Act. The
Executive Committee is also responsible for the administration of the Stock
Option Plan. See Item 12.
The Audit Committee consists of four directors who are appointed annually
by the Board of Directors. None of the members of the Audit Committee is an
officer or employee of the Company or its affiliates. This committee reviews the
internal accounting procedures of the Company, reviews and approves the
financial statements and proposes the nomination of auditors and their
remuneration.
The Human Resources and Compensation Committee consists of five directors
who are appointed annually by the Board of Directors. The Human Resources and
Compensation Committee reviews and recommends to the Board the compensation and
benefits of all officers of the Company and reviews general policy matters
relating to compensation and benefits of employees of the Company.
The Corporate Governance Committee consists of three directors who are
appointed annually by the Board of Directors. This committee is responsible for
formulating the approach of the Company to governance issues. This committee
examines any issue related to corporate governance and makes recommendations to
the Board of Directors.
The Company maintains directors and officers liability insurance against
claims made in the aggregate amount of $75,000,000 per occurrence and a maximum
of $75,000,000 per year.
ITEM 11. COMPENSATION OF DIRECTORS AND OFFICERS
COMPENSATION OF EXECUTIVE OFFICERS
The following table sets out details of the total compensation paid during
the past three years to the Chief Executive Officer and to the four other most
highly compensated executive officers (collectively the "named executive
officers").
COMPENSATION SUMMARY
<TABLE>
<CAPTION>
LONG-TERM
COMPENSATION
ANNUAL COMPENSATION AWARDS
------------------------------------ ------------
SECURITIES
UNDER
SALARY BONUS(6) OTHER(1) OPTIONS(2)
NAME AND PRINCIPAL POSITION YEAR ($) ($) ($) (#)
--------------------------- ---- ------- -------- -------- ------------
<S> <C> <C> <C> <C> <C>
Francesco Bellini(3)............................. 1997 772,935 740,000 -- 1,500,000
Chief Executive Officer 1996 475,218 667,886 -- --
1995 466,590 -- -- --
Gervais Dionne................................... 1997 210,000 63,000 -- 20,000
Executive Vice-President, Research and 1996 185,000 15,000 -- 70,000
Development
1995 181,000 15,000 -- 10,000
Michael G. Grey.................................. 1997 305,000 73,200 -- --
President, BioChem Therapeutic Inc. 1996 296,000 29,600 -- --
1995 290,000 -- -- --
Francois Legault................................. 1997 190,000 74,100 -- 20,000
Executive Vice-President, Investments and 1996 150,000 17,000 -- 70,000
Subsidiaries
1995 145,000 17,000 -- 10,000
Claude H. Vezeau(4)(5)........................... 1997 230,000 37,950 34,129 --
President, BioChem Vaccines Inc. 1996 147,554 75,000 -- 100,000
</TABLE>
NOTES:
(1) Except for Dr. Vezeau (see note (5)), the perquisites and other personal
benefits do not exceed the lesser of $50,000 and 10% of the total of the
annual salary and bonus for any of the named executive officers.
47
<PAGE> 48
(2) The securities under options represent shares which may be acquired pursuant
to the exercise of the stock options granted in 1997 under the Stock Option
Plan. (See Item 12.)
(3) The Corporation has entered into an employment agreement with Francesco
Bellini, Ph.D. to serve as Chief Executive Officer for a fixed term
commencing on February 1, 1997 and terminating on January 31, 2000. The
agreement is renewable annually thereafter unless either party gives at
least three months' notice to the other. This employment agreement provides
for an annual base salary of $800,000 and for the payment of an annual bonus
equal to $400,000 provided Dr. Bellini has performed his duties as Chief
Executive Officer for the entire year, and an amount not to exceed $400,000
calculated in function of the Corporation's results in achieving the
forecasted net earnings for the year in question. For the second and third
year of the employment term, the base salary and the bonus will be subject
to annual increases based on the percentage increase over the previous year
in prevailing compensation packages for chief executive officers of leading
North American biotechnology companies, in accordance with a formula to be
agreed upon by Dr. Bellini and the Board of Directors. If specific strategic
objectives of the Corporation specified in the employment agreement are met,
Dr. Bellini is eligible to a special bonus calculated on an agreed upon
formula. The employment agreement also provides for the payment of the
greater of (i) Dr. Bellini's salary and bonuses to the expiration of the
agreement and (ii) a lump sum payment of two years' salary and bonuses, in
the event of termination other than for cause in accordance with the laws of
the Province of Quebec or in the event of the non-renewal at the demand of
the Corporation of the employment agreement. In the event of termination or
resignation for good reason (as defined under the agreement) following a
change of control, the agreement provides for the payment to Dr. Bellini of
a lump sum severance amount equal to three times his full base salary and
bonuses at the rate in effect at the time of termination or resignation for
good reason. Dr. Bellini was also granted, at signature of the agreement,
options to purchase a total of 1,500,000 common shares at $35.625 per share.
(See Item 12.)
(4) Dr. Vezeau was hired in May 1996 and received a signing bonus of $75,000.
(5) Dr. Vezeau received personal benefits totaling $34,129 of which, $17,093
were for the reimbursement of moving expenses and $9,520 were for car
allowance.
(6) The bonus is an incentive tied to performance, according to the objectives
made at the Company level and objectives of the officers and their
respective groups.
The following table sets forth information concerning the grant of options
in the fiscal year ended December 31, 1997 to the named executive officers.
OPTION GRANTS DURING THE FISCAL YEAR
<TABLE>
<CAPTION>
% OF MARKET VALUE OF
SECURITIES UNDER TOTAL OPTIONS SECURITIES ON THE
OPTIONS GRANTED GRANTED IN EXERCISE PRICE DATE OF GRANT
NAME (#) FINANCIAL YEAR ($/SECURITY) ($/SECURITY) EXPIRATION DATE
---- ---------------- -------------- -------------- ----------------- ---------------
<S> <C> <C> <C> <C> <C>
Francesco Bellini 1,500,000 73.15% 35.625 35.625 Jan. 2007
Gervais Dionne 20,000 0.98% 35.625 35.625 Jan. 2007
Michael G. Grey -- -- -- -- --
Francois Legault 20,000 0.98% 35.625 35.625 Jan. 2007
Claude H. Vezeau -- -- -- -- --
</TABLE>
The following table sets forth the exercise of options to purchase common
shares during the fiscal year ended December 31, 1997 to the named executive
officers.
AGGREGATED OPTION EXERCISES DURING THE FISCAL YEAR
<TABLE>
<CAPTION>
VALUE OF UNEXERCISED
UNEXERCISED OPTIONS IN-THE-MONEY OPTIONS
SECURITIES ACQUIRED AGGREGATE VALUE AT FISCAL YEAR-END AT FISCAL YEAR-END
ON EXERCISE REALIZED EXERCISABLE/UNEXERCISABLE EXERCISABLE/UNEXERCISABLE
NAME (#) ($) (#) ($)
---- ------------------- --------------- ------------------------- -------------------------
<S> <C> <C> <C> <C>
Francesco Bellini -- -- 1,500,000/1,500,000 29,062,500/0
Gervais Dionne -- -- 156,000/94,000 2,293,625/410,125
Michael G. Grey -- -- 270,000/200,000 6,361,875/4,712,500
Francois Legault -- -- 100,800/95,200 1,510,100/307,400
Claude H. Vezeau -- -- 20,000/80,000 0/0
</TABLE>
The aggregate compensation paid by the Company and its subsidiaries to the
Company's eleven full-time executive officers for services rendered during the
year ended December 31, 1997 was $3,544,142.
48
<PAGE> 49
The value of the benefits received in respect of the year ended December
31, 1997 by these executive officers of the Company did not exceed 10% of the
above-mentioned cash remuneration.
COMPENSATION OF DIRECTORS
In 1997, external Directors received fees of $18,000 per year as well as
$1,000 for each meeting of the Board of Directors or of a committee of the
Board. The Chairman of the Board also received an extra $7,000 fee per year. The
aggregate amount of such compensation was $186,267 for the fiscal year ended
December 31, 1997.
External Directors are granted annually under the Stock Option Plan (See
Item 12.) 1,000 options each, plus 1,000 options in the case of the Chairman of
the Board. When an external director is first elected to the Board, he/she is
granted 7,500 options. For the fiscal year ended December 31, 1997, 24,000
options were as such granted at an exercise price equal to the closing price on
the day preceding the grant, which was $31.00.
ITEM 12. OPTIONS TO PURCHASE SECURITIES FROM THE COMPANY OR SUBSIDIARIES
STOCK OPTION PLAN
The Stock Option Plan of the Company (the "Plan") provides for the granting
of options to purchase a maximum of 19,250,000 common shares of the Company.
Beneficiaries of the Plan are the directors, officers and full-time employees or
regular employees of the Company or its subsidiaries as well as external
consultants, engaged by the Company or its subsidiaries to provide ongoing bona
fide management and consulting services.
The Board of Directors, in its discretion, grants options following the
recommendation of the Executive Committee which administers the Plan. Under the
Plan, the options may be exercised progressively but within a maximum period of
ten years from the date of the grant. The exercise price of the options, which
cannot be lower than the market price on the day immediately preceding the day
on which the options are granted, must be paid upon exercise.
As of March 31, 1998, there were outstanding under the Plan options to
purchase an aggregate of 6,941,200 common shares at prices ranging from $6.19 to
$38.75 per share, and expiring at various dates through March 2008. Of such
options, as of March 31, 1998 the directors and executive officers as a group
held 5,505,800 options to purchase common shares. The following named executive
officers have the set forth options under the Plan:
<TABLE>
<CAPTION>
EXECUTIVE OFFICER NUMBER OF OPTIONS PRICE RANGE EXPIRATION DATES RANGE
----------------- ----------------- ---------------- -------------------------------
<S> <C> <C> <C>
Francesco Bellini........... 3,000,000 $11.13 to $35.63 December 2001 to January 2007
Gervais Dionne.............. 270,000 $ 6.94 to $35.63 February 2002 to January 2008
Michael G. Grey............. 470,000 $ 6.94 September 2004
Francois Legault............ 216,000 $ 6.94 to $35.63 February 2002 to January 2008
Claude H. Vezeau............ 100,000 $31.30 June 2006
</TABLE>
For a complete discussion of the Stock Option Plan see Note 14 to the
Consolidated Financial Statements annexed hereto and which also discusses the
options of the Societe de developpement industriel du Quebec (SDI) to purchase
shares.
SHAREHOLDER RIGHTS PLAN
The shareholders of the Company approved in 1995 a Shareholder Rights Plan
("Rights Plan") which was amended with shareholder approval in April 1998. Under
the Rights Plan, one common share purchase right was issued on April 28, 1995 in
respect of each outstanding common share of the Company and a share purchase
right for each common share of the Company issued thereafter. These rights are
exercisable in a situation of a public take-over bid for voting shares of the
Company where certain conditions are not respected. Each right entitles the
holder to purchase, from the Company, one common share at a specific price,
subject to certain anti-dilution adjustments. The Rights Plan expires on June
30, 2003 or unless terminated earlier by the Company's Board of Directors. The
purpose of the Rights Plan is to require anyone, who seeks to acquire 20% or
more of the Company's voting shares, to present a bid complying with specific
49
<PAGE> 50
provisions. The objectives of the Rights Plan are to ensure that, in the event
of a takeover bid of the Company, all shareholders will receive full and fair
value for their shares and will not be subject to abusive or coercive takeover
strategies and that the Board of Directors, on behalf of the Company and all its
shareholders, will have the time and opportunity to evaluate the bid and its
effects, to seek out alternative bidders and to explore, develop and evaluate
other ways of maximizing shareholder value.
ITEM 13. INTEREST OF MANAGEMENT IN CERTAIN TRANSACTIONS
At least since January 1, 1996, there has been no material transaction
involving the Company or any of its subsidiaries and one of its directors,
officers, principal shareholders (as stated in Item 4. Control of Registrant),
or their close family, nor is any presently proposed such transaction, other
than the following:
-- Two directors, James A. Grant and Guy Lord, are partners respectively
in the Montreal law firms Stikeman, Elliott and Desjardins Ducharme
Stein Monast, and which firms provide professional services to the
Company on an on-going basis;
-- One director, Paul N. Lucas, is the senior officer of Glaxo Wellcome
Inc., the Company's partner for the distribution of 3TC and Combivir in
Canada;
-- One director, Guy Savard, is a senior officer of Midland Walwyn, one
of the underwriters in the public offering of securities of the Company
in February 1996; as such Midland Walwyn received a fee of $767,906.
For a complete discussion on this matter see Note 17 to the annexed
Consolidated Financial Statements.
Except Dr. Claude H. Vezeau, no director or officer, or any associate of
them, is or has been indebted to the Company or its subsidiaries, since at least
January 1, 1996. As the new vaccine center of the Company opened in the Quebec
City area in July 1997, the President of Vaccines, Dr. Claude H. Vezeau, was
relocated with his family to the Quebec City area. For that purpose, the Company
made a $100,000 loan to Dr. Vezeau to purchase a house. The interests on this
loan are payable monthly and the principal is reimbursable in full in June 2002.
On April 23, 1998, BioChem repurchased the 25% stake in Vaccines held
indirectly by the Caisse de depot et placement du Quebec through its subsidiary
SOFINOV Societe financiere d'innovation inc. As a result, the conversion rights
agreement referred to in Note 17 to the Annexed Consolidated Financial
Statements is no longer in force.
PART II
ITEM 14. DESCRIPTION OF SECURITIES
Not applicable.
PART III
ITEM 15. DEFAULT UPON SENIOR SECURITIES
Not applicable
ITEM 16. CHANGES IN SECURITIES AND CHANGES IN SECURITY FOR REGISTERED
SECURITIES
A two-for-one stock split of the common shares took effect as of the close
of business on April 7, 1997. On December 31, 1997, the Company completed a
legal reorganization to change its governing act from the Quebec Companies Act
to the Canada Business Corporations Act. For information regarding certain
changes in the rights of holders of common shares of BioChem, see the Company's
Management Proxy Circular dated March 31, 1997.
50
<PAGE> 51
PART IV
ITEM 17. FINANCIAL STATEMENTS
The financial statements of the Company are annexed hereto and have been
prepared by the Company in accordance with generally accepted accounting
principles in Canada, which differ in certain respects from generally accepted
accounting principles in the United States as outlined in the financial
statements. The table of contents to the consolidated financial statements and
accompanying notes to the consolidated financial statements appears on page F-1
of this Report on Form 20-F.
ITEM 18. FINANCIAL STATEMENTS
Not applicable
ITEM 19. FINANCIAL STATEMENTS AND EXHIBITS
A. FINANCIAL STATEMENTS
<TABLE>
<S> <C>
- Consolidated Statement of Earnings for the years ended
December 31, 1997, 1996 and 1995.
- Consolidated Statement of Retained Earnings for the years
ended December 31, 1997, 1996 and 1995.
- Consolidated Balance Sheet as at December 31, 1997 and 1996.
- Consolidated Statement of Changes in Financial Position for
the years ended December 31, 1997, 1996 and 1995.
- Notes to Consolidated Financial Statements.
Schedule VIII Reserves as at December 31, 1997, 1996 and 1995.
Schedule IX Short-Term Borrowings as at December 31, 1997, 1996 and
1995.
Schedule X Supplementary Earnings Statement Information for the years
ended December 31, 1997, 1996 and 1995.
</TABLE>
B. EXHIBITS ALREADY FILED IN PREVIOUS YEARS (COMMISSION FILE NUMBER
0-18781)
<TABLE>
<CAPTION>
Exhibit
Number
<S> <C>
3.1 Articles of Continuance and Articles of Amendment of the
Registrant -- incorporated herein by reference to exhibit
1(a) to the Registrant's Registration Statement on Form 20-F
(File No. 0-18701), declared effective March 14, 1991.
3.2 Articles of Amendment -- incorporated herein by reference to
Registrant's Report of Foreign Issuer on Form 10-C, filed
March 3, 1992.
3.3 By-laws of the Registrant, as amended -- incorporated herein
by reference to exhibit 1(b) to the Registrant's
Registration Statement on Form 20-F (File No. 0-18701),
declared effective March 14, 1991.
3.4 By-law No. 1992-1 reducing the authorized capital of the
Registrant.
4.1 Specimen Stock Certificate.
9.1(1) Shareholders Agreement dated January 24, 1991 by and among
Glaxo Canada Inc. and Caisse de depot et placement du Quebec
and Fonds de solidarite des travailleurs du Quebec (F.T.Q.)
and Bio-Cascades Inc. and IFCI Holding International S.A.
and Francesco Bellini and Lawrence Wilson and James McDonald
and Gervais Dionne and Francois Legault.
10.1 Form of Unit Subscription Agreement dated June 1989.
10.2 Warrant Indenture dated June 29, 1989 between Registrant and
General Trust of Canada, Trustee.
10.3(2) Sponsored Research Agreement dated January 1, 1990, between
Glaxo Canada Inc. and Registrant.
</TABLE>
51
<PAGE> 52
<TABLE>
<CAPTION>
Exhibit
Number
<S> <C>
10.4 Subscription Agreement dated as of January 24, 1991 between
the Registrant and Glaxo Canada Inc.
10.5(2) Master License Agreement dated as of January 31, 1990
between the Registrant and Glaxo Canada Inc.
10.6(2) Outline of Arrangement dated as of January 24, 1991 between
the Registrant and Glaxo Canada Inc.
10.8 Joint Venture Formation Agreement dated January 24, 1991
between Glaxo Canada Inc., Glaxo Group Limited and
Registrant.
10.9(2) Joint Venture Operation Agreement dated January 24, 1991
between Glaxo Group Limited, Glaxo Canada Inc., Registrant
and Glaxo-IAF BioChem Inc., a company to be incorporated
(Schedule 3 to the Joint Venture Formation Agreement -- item
10.8 above) Joint Venture Formation Agreement -- item 10.8
above).
10.10 Rights Agreement dated January 24, 1991 between Glaxo Group
Limited, Glaxo Canada Inc. and Registrant (Schedule 4 to the
Joint Venture Formation Agreement -- item 10.8 above).
10.11 Addendum to Master License Agreement dated January 31, 1990
between Glaxo Group Limited, Glaxo Canada Inc., Glaxo Inc.,
and Registrant (Schedule 5 to the Joint Venture Formation
Agreement -- item 10.8 above).
10.12(2) Collaborative Research Agreement dated August 1, 1991
between Glaxo-Canada Inc. and Registrant.
10.13 Share Purchase Agreement dated January 17, 1990 between
North American Vaccine, Inc. and Registrant -- incorporated
herein by reference to exhibit 2.3 to Amendment No. 2 to
North American Vaccine, Inc.'s Registration Statement on
Form S-4 (File No. 33-31512), declared effective January 24,
1990.
10.14 North American Vaccine, Inc. Shareholders Agreement dated
January 17, 1990 among Registrant, Philip Frost, M.D., IVAX
Corporation, and Frost Nevada, Limited Partnership --
incorporated herein by reference to exhibit 9.1 to Amendment
No. 2 to North American Vaccine, Inc.'s Registration State-
ment on Form S-4 (File No. 33-31512), declared effective
January 24, 1990
10.15 Technology Transfer Agreement dated January 17, 1990 between
North American Vaccine, Inc. and Registrant -- incorporated
herein by reference to exhibit 2.4 to Amendment No. 2 to
North American Vaccine, Inc.'s Registration Statement on
Form S-4 (File No. 33-31512), declared effective January 24,
1990.
10.16(2) Purchase and Sale Agreement in Respect of 522,550 Shares of
IFCI CloneSystems S.p.A. and 28,000 Shares of Chemila S.p.A.
dated August 1, 1991 between IFCI Holding International S.A.
and Registrant.
10.17 Shareholders Agreement dated August 1, 1991 between
Registrant, IFCI Holding International S.A., IFCI
CloneSystems S.p.A. and Chemila S.p.A.
10.18(1)(2) Sale by Institut Armand-Frappier to IAF BioVac Inc., dated
as of May 28, 1990.
10.19(1) Collaboration Agreement for Scientific Research Projects
between Institut Armand-Frappier and A New Vaccine Company
to be created by Registrant, dated November 28, 1989
(Schedule B to the Sale by Institut Armand-Frappier to IAF
BioVac Inc. -- Item 10.18 above).
10.20(1) Lease A between Institut Armand-Frappier and IAF BioVac Inc.
dated May 28, 1990 regarding 14,387 square feet in Buildings
1, 11, 13 and 14 (Schedule C to the Sale by Institut
Armand-Frappier to IAF BioVac Inc. -- Item 10.18 above).
</TABLE>
52
<PAGE> 53
<TABLE>
<CAPTION>
Exhibit
Number
<S> <C>
10.21(1) Lease B between Institut Armand-Frappier and IAF BioVac Inc.
dated May 28, 1990, regarding 22,468 square feet in Building
18 (Schedule C to the Sale by Institut Armand-Frappier to
IAF BioVac Inc. -- Item 10.18 above).
10.22(1) Lease C between Institut Armand-Frappier and IAF BioVac Inc.
dated May 28, 1990, regarding 11,743 square feet in Building
15, as well as the Basement Space Erected on Lot 22
(Schedule C to the Sale by Institut Armand-Frappier to IAF
BioVac Inc. -- Item 10.18 above).
10.23 BioChem Pharma Directors, Officers and Employees Stock
Option Plan.
10.24 Form of BioChem Pharma Stock Option Agreement.
10.25 [reserved].
10.26(1) Form of IAF BioVac Inc. Convention d'Options d'Achat
d'Actions Ordinaires Intervenue a Montreal, Quebec le 29 mai
1990.
10.27 Employment Agreement dated December 17, 1991, between Dr.
Francesco Bellini and Registrant.
10.28 Employment Agreement dated August 1, 1991, between Mr.
Silvio Nuzzo and Registrant.
10.29 Agreement to Amend Share Purchase Agreement between North
American Vaccine, Inc. and Registrant dated February 26,
1990.
10.30 Amendments to Master License Agreement on March 21, 1994
between Glaxo Group Limited, Glaxo Canada Inc. and BioChem
Pharma Inc.
10.31 Written Notice by Glaxo Canada Inc. terminating the
Shareholders Agreement dated November 5, 1993 and effective
May 6, 1994.
11.1 Statement regarding computation of net income per share.
13.1 Annual Report for the year ended December 31, 1995.
13.2 Notice of Annual and Special General Meeting of the
Shareholders and Management Proxy Circular dated April 22,
1996.
22.1 Subsidiaries of the Registrant.
</TABLE>
C. EXHIBITS FILED LAST YEAR
-- Revised and Restated Master License agreement(2) between Glaxo
Wellcome Inc., BioChem Pharma Inc., Tanaud Holdings (Barbados)
Limited, Tanaud International B.V. and Tanaud LLC. filed on Form 6K.
D. EXHIBITS FILED THIS YEAR (Commission file number 0-19539)
-- Annual Report for the year ended December 31, 1997.
-- Management Proxy Circular dated March 16, 1998.
ADDITIONAL INFORMATION
The following documents can be obtained upon request from the Corporate
Secretary of BioChem, at BioChem Pharma Inc., 275 Armand-Frappier Blvd,
Laval, Quebec, H7V 4A7.
(i) this Form 20-F, together with any document incorporated herein by
reference;
(ii) the Annual Report of BioChem and any interim financial statements
filed with Securities Commissions subsequent to the audited
financial statements for BioChem's most recently completed financial
year;
(iii) the Management Proxy Circular; and
(iv) any other documents that are incorporated by reference into a
preliminary short form prospectus or a short form prospectus
pursuant to which securities of BioChem are in the course of a
distribution.
53
<PAGE> 54
Except when securities of BioChem are in the course of distribution
pursuant to a short form prospectus or a preliminary short form prospectus,
BioChem may require the payment of a reasonable charge from persons, other than
security holders, of BioChem, requesting copies of these documents.
- ------------------
(1) Includes English summary or translation.
(2) Confidential treatment requested as to certain portions.
54
<PAGE> 55
SIGNATURES
Pursuant to the requirements of Section 12 of the Securities Exchange Act
of 1934, the registrant certifies that it meets all of the requirements for
filing on Form 20-F and has duly caused this Registration Statement to be signed
on its behalf by the undersigned, hereunto duly authorized.
BIOCHEM PHARMA INC.
By: (s) Charles-A. Tessier
Charles-A. Tessier
Vice-President, Legal Affairs
and Corporate Secretary
Dated: June 2, 1998
55
<PAGE> 56
ANNEX
BIOCHEM PHARMA INC.
CONSOLIDATED FINANCIAL STATEMENTS
FOR THE YEARS ENDED
DECEMBER 31, 1997, 1996 AND 1995
56
<PAGE> 57
BIOCHEM PHARMA INC.
CONSOLIDATED FINANCIAL STATEMENTS
FOR THE YEARS ENDED
DECEMBER 31, 1997, 1996 AND 1995
TABLE OF CONTENTS
<TABLE>
<CAPTION>
PAGE
----
<S> <C>
Auditor's Report........................................ F-2
Financial Statements
Consolidated Statement of Earnings.................... F-3
Consolidated Statement of Retained Earnings
(Deficit).......................................... F-3
Consolidated Balance Sheet............................ F-4
Consolidated Statement of Changes in Financial
Position........................................... F-5
Notes to Consolidated Financial Statements............ F-6 to F-21
Schedules VIII, IX, X................................... F-23 to F-26
</TABLE>
F-1
<PAGE> 58
AUDITORS' REPORT
To the Shareholders of
BioChem Pharma Inc.
We have audited the consolidated balance sheets of BioChem Pharma Inc. as
at December 31, 1997 and 1996 and the consolidated statements of earnings,
retained earnings and changes in financial position for the years ended December
31, 1997, 1996 and 1995. These financial statements are the responsibility of
the Company's management. Our responsibility is to express an opinion on these
financial statements based on our audits.
We conducted our audits in accordance with generally accepted auditing
standards in Canada. Those standards require that we plan and perform an audit
to obtain reasonable assurance whether the financial statements are free of
material misstatement. An audit includes examining, on a test basis, evidence
supporting the amounts and disclosures in the financial statements. An audit
also includes assessing the accounting principles used and significant estimates
made by management, as well as evaluating the overall financial statement
presentation.
In our opinion, these consolidated financial statements present fairly, in
all material respects, the financial position of the Company as at December 31,
1997 and 1996 and the results of its operations and the changes in its financial
position for the years ended December 31, 1997, 1996 and 1995 in accordance with
generally accepted accounting principles in Canada.
LOGO
Raymond Chabot Grant Thornton
General partnership
Chartered Accountants
Montreal, Quebec, Canada
February 10, 1998
F-2
<PAGE> 59
BIOCHEM PHARMA INC.
CONSOLIDATED STATEMENT OF EARNINGS
for the years ended December 31, 1997, 1996 and 1995
(in thousands of Canadian dollars except per share information)
<TABLE>
<CAPTION>
1997 1996 1995
------------- ------------- -------------
$ $ $
<S> <C> <C> <C>
OPERATING REVENUE
Sales.................................................... 134,641 156,941 162,470
Royalties................................................ 124,130 57,062 12,596
Interest................................................. 12,285 13,008 2,976
Other.................................................... 9,726 6,607 9,349
------------- ------------- -------------
280,782 233,618 187,391
------------- ------------- -------------
EXPENSES
Cost of sales............................................ 67,450 75,759 74,241
Selling and administrative............................... 72,480 62,968 58,486
Milestone repayments (Note 3)............................ -- 4,552 1,825
Research and development (Note 3)........................ 37,387 32,186 22,087
Financial (Note 3)....................................... 5,863 7,527 8,649
------------- ------------- -------------
183,180 182,992 165,288
------------- ------------- -------------
Earnings before depreciation, amortization and other....... 97,602 50,626 22,103
Depreciation and amortization (note 3)..................... (11,092) (11,457) (13,042)
------------- ------------- -------------
Earnings before income taxes and other..................... 86,510 39,169 9,061
Income taxes (note 4)...................................... (2,064) (1,451) (5,443)
Non-controlling interest................................... 1,987 (211) (484)
Share of loss of an affiliated company,
net of gain on dilution (note 7)......................... (6,595) (4,113) (8,101)
------------- ------------- -------------
NET INCOME (LOSS).......................................... 79,838 33,394 (4,967)
============= ============= =============
EARNINGS (LOSS) PER COMMON SHARE........................... 0.74 0.31 (0.05)
============= ============= =============
</TABLE>
CONSOLIDATED STATEMENT OF RETAINED EARNINGS
for the years ended December 31, 1997, 1996 and 1995
(in thousands of Canadian dollars)
<TABLE>
<CAPTION>
1997 1996 1995
------------- ------------- -------------
$ $ $
<S> <C> <C> <C>
Retained earnings (deficit), beginning of year............. 1,201 (32,193) (27,226)
Net income (loss).......................................... 79,838 33,394 (4,967)
------------- ------------- -------------
Retained earnings (deficit), end of year................... 81,039 1,201 (32,193)
============= ============= =============
</TABLE>
The accompanying notes are an integral part of the consolidated financial
statements.
F-3
<PAGE> 60
BIOCHEM PHARMA INC.
CONSOLIDATED BALANCE SHEET
As at December 31, 1997 and 1996
(in thousands of Canadian dollars)
<TABLE>
<CAPTION>
1997 1996
------------- -------------
$ $
<S> <C> <C>
ASSETS
Current assets
Cash and temporary investments............................ 310,416 314,751
Accounts receivable (Note 5).............................. 101,161 91,170
Inventories (Note 6)...................................... 30,688 32,003
Prepaid expenses.......................................... 3,822 1,619
Deferred income taxes..................................... 1,100 1,100
------------- -------------
447,187 440,643
Investments (Note 7)........................................ 65,465 25,525
Capital assets (Note 8)..................................... 108,937 75,143
Other assets (Note 9)....................................... 33,683 30,954
------------- -------------
655,272 572,265
============= =============
LIABILITIES
Current liabilities
Bank indebtedness (Note 10)............................... 22,967 12,981
Accounts payable and accrued liabilities (Note 11)........ 49,898 48,571
Current portion of long-term debt (Note 12)............... 9,039 16,349
------------- -------------
81,904 77,901
Long-term debt (Note 12).................................... 58,269 57,706
Other liabilities (Note 13)................................. 4,134 8,283
Non-controlling interest.................................... 12,897 12,543
------------- -------------
157,204 156,433
------------- -------------
SHAREHOLDERS' EQUITY
Capital stock (Note 14)..................................... 404,431 401,744
Contributed surplus......................................... 10,199 10,199
Retained earnings........................................... 81,039 1,201
Foreign currency translation adjustment (Note 15)........... 2,399 2,688
------------- -------------
498,068 415,832
------------- -------------
655,272 572,265
============= =============
</TABLE>
On Behalf of the Board,
LOGO
- ---------------------------------------------------
FRANCESCO BELLINI, Director
LOGO
- ---------------------------------------------------
GUY LORD, Director
The accompanying notes are an integral part of the consolidated financial
statements.
F-4
<PAGE> 61
BIOCHEM PHARMA INC.
CONSOLIDATED STATEMENT OF CHANGES IN FINANCIAL POSITION
for the years ended December 31, 1997, 1996 and 1995
(in thousands of Canadian dollars)
<TABLE>
<CAPTION>
1997 1996 1995
------------- ------------- -------------
$ $ $
<S> <C> <C> <C>
Cash provided by (used for) the following activities:
OPERATING ACTIVITIES
Net income (loss).......................................... 79,838 33,394 (4,967)
Non-cash items (Note 16)................................... 17,376 15,145 19,442
------------- ------------- -------------
Operating cash flow........................................ 97,214 48,539 14,475
Changes in non-cash working capital items (Note 16)........ (13,349) (10,944) (11,468)
------------- ------------- -------------
Cash flow from operations.................................. 83,865 37,595 3,007
------------- ------------- -------------
INVESTING ACTIVITIES
Acquisition of investments................................. (46,641) (7,769) (4,243)
Acquisition of capital assets.............................. (44,397) (18,353) (10,574)
Disposal of capital assets................................. 477 639 877
Other...................................................... (3,794) (5,743) (503)
------------- ------------- -------------
(94,355) (31,226) (14,443)
------------- ------------- -------------
Free cash flow............................................. (10,490) 6,369 (11,436)
------------- ------------- -------------
FINANCING ACTIVITIES
Increase in long-term debt................................. 8,932 4,389 714
Repayment of long-term debt................................ (17,532) (6,303) (6,396)
Non-controlling interest................................... 2,650 7,500 2,394
Issuance of common shares.................................. 2,687 247,732 34,735
Other...................................................... 186 977 351
------------- ------------- -------------
(3,077) 254,295 31,798
------------- ------------- -------------
Foreign currency translation adjustment.................... (754) (111) (714)
------------- ------------- -------------
Increase (decrease) in cash position....................... (14,321) 260,553 19,648
Cash position, beginning of year........................... 301,770 41,217 21,569
------------- ------------- -------------
Cash position, end of year................................. 287,449 301,770 41,217
============= ============= =============
</TABLE>
Cash position comprises cash and temporary investments, less bank indebtedness.
The accompanying notes are an integral part of the consolidated financial
statements.
F-5
<PAGE> 62
BIOCHEM PHARMA INC.
NOTES TO CONSOLIDATED FINANCIAL STATEMENTS
(tabular amounts are in thousands of Canadian dollars except per share
information)
1. GOVERNING STATUTES AND NATURE OF OPERATIONS
The Company is an international biopharmaceutical company involved in the
research, development, manufacturing and marketing of innovative products
for the prevention, detection and treatment of human diseases.
During the year, the Company effected a reorganization. The results of this
reorganization are that a new company is incorporated under the Canada
Business Corporations Act which will continue operations of the former
company which was incorporated under Part 1A of the Companies Act (Quebec).
The results of operations of the new company include all the results of
operations from the former company as if the two companies have always
existed and have always been combined.
2. SIGNIFICANT ACCOUNTING POLICIES
The consolidated financial statements have been prepared in accordance with
generally accepted accounting principles in Canada and conform, in all
material respects, with International Accounting Standards. The financial
statements differ in certain respects from generally accepted accounting
principles in the United States, as described in Note 21.
PRINCIPLES OF CONSOLIDATION
The consolidated financial statements include the accounts of the Company
and those of its subsidiaries since their date of acquisition or creation.
USE OF ESTIMATES
The preparation of financial statements requires management to make
estimates and assumptions that affect the amounts presented in the
financial statements and the accompanying notes. Actual results could
differ from these estimates.
FOREIGN CURRENCY TRANSLATION
Operating revenue and expenses arising from foreign currency transactions
are translated into Canadian dollars at exchange rates in effect on the
date of the transactions. Monetary assets and liabilities are translated
into Canadian dollars at the exchange rate in effect at the balance sheet
date. Gains or losses arising from these translations are included in
earnings, with the exception of unrealized foreign exchange gains or losses
on long-term monetary items, which are amortized over the remaining period
of the related items.
Assets and liabilities of self-sustaining foreign operations are translated
into Canadian dollars at the exchange rate in effect at the balance sheet
date. Operating revenue and expense items are translated at average
exchange rates prevailing during the year. Any corresponding foreign
exchange gains and losses are disclosed separately as part of shareholders'
equity and are recognized in earnings when the interest in the foreign
operations is reduced.
INVENTORY VALUATION
Inventory valuation The raw materials inventory is valued at the lower of
cost and replacement cost. The finished goods and work in process
inventories are valued at the lower of cost and net realizable value. Cost
is determined using the first in, first out method.
LONG-TERM INVESTMENTS
Investment in the common shares of an affiliated company is accounted for
by the equity method and other investments are recorded at acquisition
cost. When there has been a decrease in value of a long-term investment
that is other than a temporary decline, the investment is written down to
recognize the loss.
F-6
<PAGE> 63
CAPITAL ASSETS
Capital assets are recorded at acquisition cost, net of related investment
tax credits and government grants.
Rights, licenses and patents include acquisition costs and the costs
incurred to register the patents as well as the costs incurred to obtain
the licenses necessary to market and manufacture products.
Depreciation and amortization are calculated as follows:
<TABLE>
<CAPTION>
METHOD ANNUAL RATES
----------------- --------------------------------
<S> <C> <C>
Buildings........................... Declining balance 5% to 10%
Equipment........................... Declining balance 10% to 40%
Leasehold improvements.............. Straight-line Over the lease terms
Rights, licenses and patents........ Straight-line 5 to 10 years, commencing in the
year in which the product is
marketed
</TABLE>
GOODWILL
Goodwill represents the excess of the cost of acquisitions over the fair
value of the net assets acquired and is evaluated for any impairment in
value. The evaluation consists of a review of the forecasted future
earnings and the discounted cash flows of the operations acquired. Any
permanent impairment in the carrying value is charged to earnings in the
year incurred. The Company concluded that the carrying value of goodwill
had not sustained a permanent impairment in value for the years ended
December 31, 1997, 1996 and 1995.
Goodwill is amortized on a straight-line basis over a period of 20 years,
ending in 2014.
DEFERRED INCOME TAXES
The Company follows the tax allocation basis of accounting for income
taxes. Deferred income taxes result from timing differences between
accounting income and taxable income.
RESEARCH AND DEVELOPMENT
Research and development expenses are recognized in the year they are
incurred, net of related tax credits, and include a share of administrative
expenses.
EARNINGS (LOSS) PER COMMON SHARE
Earnings (loss) per common share is calculated using the weighted average
number of common shares outstanding during the year.
3. INFORMATION ON THE CONSOLIDATED STATEMENT OF EARNINGS
MILESTONE REPAYMENTS
Milestone repayments were made pursuant to an agreement with Glaxo Wellcome
covering the development and marketing of 3TC and were recognized as
expenses, based on 50% of royalties earned on the sales of this product
subject to a maximum of 3 million British pounds sterling ($6,377,000). For
the year ended December 31, 1996, final payments totalling $4,552,000 have
been recognized as milestone repayments and payments totalling $1,825,000
have been recognized for the year ended December 31, 1995.
RESEARCH AND DEVELOPMENT
Research and development expenses are disclosed net of tax credits
amounting to $1,729,000 ($1,314,000 for the year ended December 31, 1996
and $1,318,000 for the year ended December 31, 1995).
F-7
<PAGE> 64
<TABLE>
<CAPTION>
1997 1996 1995
----------- ----------- -----------
$ $ $
<S> <C> <C> <C>
FINANCIAL EXPENSES
Interest on long-term debt.................................. 5,547 5,860 6,689
Other interest.............................................. 2,061 2,953 1,939
Foreign exchange loss (gain)................................ (2,895) (43) 637
Amortization of deferred foreign exchange gains and
losses.................................................... 1,543 (725) (547)
Realization of foreign currency translation adjustment...... -- -- 701
----------- ----------- -----------
6,256 8,045 9,419
Interest on long-term debt reimbursed by the Societe de
developpement industriel du Quebec........................ (393) (518) (770)
----------- ----------- -----------
5,863 7,527 8,649
=========== =========== ===========
DEPRECIATION AND AMORTIZATION
Capital assets.............................................. 8,643 9,087 11,129
Goodwill.................................................... 1,525 1,491 1,525
Deferred charges............................................ 924 879 388
----------- ----------- -----------
11,092 11,457 13,042
=========== =========== ===========
</TABLE>
4. INCOME TAXES
<TABLE>
<CAPTION>
1997 1996 1995
----------- ----------- -----------
$ $ $
<S> <C> <C> <C>
Income taxes (recovery) at combined statutory tax rates
of different jurisdictions................................ (5,689) (2,688) 1,901
Non-deductible items........................................ 489 866 520
Realization of previously unrecorded tax loss benefit....... -- (1,663) (567)
Tax benefit and deferred income taxes not recorded.......... 8,207 4,454 3,682
Large corporations tax...................................... 327 482 213
Tax rate differences on reversal of timing differences...... (1,270) -- (306)
----------- ----------- -----------
Income taxes at effective tax rates......................... 2,064 1,451 5,443
=========== =========== ===========
The provision for income taxes comprises the following:
Current: Canada............................................. 666 843 662
Foreign.......................................... 1,138 992 5,708
Deferred:Canada............................................. -- -- --
Foreign........................................... 260 (384) (927)
----------- ----------- -----------
2,064 1,451 5,443
=========== =========== ===========
</TABLE>
F-8
<PAGE> 65
The Company has research and development expenses, non-capital losses and
share issue expenses which have been deferred for tax purposes. In
addition, the net book value of the capital assets differs from their
undepreciated capital cost for tax purposes. These items, totalling
approximately $94,850,000 as at December 31, 1997 ($75,400,000 as at
December 31, 1996) may be utilized to reduce taxable income in future
years.
Operating losses carried forward at December 31, 1997 total approximately
$95 million. Approximately $59 million of such losses have no expiration
date, and the balance of the losses expire on various dates from 1998
through 2007 if not utilized.
As at December 31, 1997, the Company has investment tax credits amounting
to approximately $13,300,000 ($9,500,000 as at December 31, 1996) that have
been deferred for tax purposes and may be used to reduce future taxes
payable. These credits expire in the years 2000 to 2007.
The tax benefit in respect of these items has not been reflected in the
accounts as at December 31, 1997.
The tax effects of differences between the accounting value and the tax
value of assets and liabilities are as follows:
<TABLE>
<CAPTION>
1997 1996
------- -------
$ $
<S> <C> <C>
Deferred tax liabilities
Other..................................................... -- (1,354)
------- -------
Deferred tax assets
Operating losses carried forward.......................... 36,367 28,523
Investment tax credit..................................... 13,304 9,350
Other..................................................... 2,358 2,903
------- -------
52,029 40,776
Valuation allowance....................................... (49,600) (39,676)
------- -------
Net deferred tax assets 2,429 1,100
------- -------
Net deferred tax assets (liabilities)....................... 2,429 (254)
======= =======
</TABLE>
5. ACCOUNTS RECEIVABLE
<TABLE>
<CAPTION>
1997 1996
------------- -----------
$ $
<S> <C> <C>
Trade(a).................................................... 59,186 66,320
Royalties receivable from a shareholder..................... 34,879 20,598
Quebec tax credits.......................................... 1,771 1,406
Other....................................................... 5,325 2,846
------------- -----------
101,161 91,170
============= ===========
</TABLE>
(a) There is a geographic concentration of credit risk with regard to
operations conducted in Italy.
The allowance for doubtful accounts for trade accounts receivable for all
countries amounted to $2,635,000 as at December 31, 1997 ($3,497,000 as at
December 31, 1996).
F-9
<PAGE> 66
6. INVENTORIES
<TABLE>
<CAPTION>
1997 1996
----------- -----------
$ $
<S> <C> <C>
Raw materials............................................... 12,348 14,586
Work in process............................................. 2,179 3,340
Finished goods.............................................. 16,161 14,077
----------- -----------
30,688 32,003
=========== ===========
</TABLE>
7. INVESTMENTS
<TABLE>
<CAPTION>
1997 1996
--------- ---------
$ $
<S> <C> <C>
Investments in private companies, at cost................... 52,040 6,460
Shares of public companies, at cost......................... 8,231 6,899
Investment in an affiliated company(a)...................... 5,194 12,166
--------- ---------
65,465 25,525
========= =========
</TABLE>
(a) INVESTMENT IN THE AFFILIATED COMPANY North American Vaccine, Inc.
(NAVA) is accounted for by the equity method. NAVA is a public company
listed on the American Stock Exchange. The price per common share at the
close of the market on December 31, 1997 was $35.67 ($33.41 per share as
at December 31, 1996) which represents U.S.$24.9375 (U.S.$24.375 as at
December 31, 1996). As at December 31, 1997, the market value of the
Company's investment in NAVA based on the closing market price at the
balance sheet date amounted to $470,099,000 ($440,314,000 as at December
31, 1996) taking into consideration the conversion of preferred shares
into common shares, but excluding purchase options outstanding at the
end of the year.
The changes in the investment in an affiliated company are as follows:
<TABLE>
<CAPTION>
1997 1996
--------- ---------
$ $
<S> <C> <C>
Balance, beginning of year.................................. 12,166 15,690
Common share options exercised (231,252 in 1996)............ -- 568
Share of loss recognized.................................... (9,345) (9,637)
Gain on dilution from the issue of share capital by the
affiliated company........................................ 2,750 5,524
Foreign currency translation adjustment..................... (243) 21
Other....................................................... (134) --
--------- ---------
Balance, end of year........................................ 5,194 12,166
========= =========
Number of shares held
Common shares............................................. 11,179,114 11,179,114
========= =========
Preferred shares, each convertible into two common
shares................................................. 1,000,000 1,000,000
========= =========
</TABLE>
The Company holds 35.0% of the common shares outstanding as at December 31,
1997 (35.6% as at December 31, 1996) and 50.0% of the preferred shares
outstanding as at December 31, 1997 and 1996.
GAIN ON DILUTION FROM THE ISSUE OF SHARE CAPITAL BY THE AFFILIATED COMPANY
The gain on dilution results from the issuance of common shares by the
affiliated company. No income taxes have been recorded on this gain because
the tax value is greater than the book value as at December 31, 1997 and
1996.
COMMON SHARE PURCHASE OPTIONS HELD BY THE COMPANY
The Company holds 57,812 options to purchase common shares of NAVA, which
represent 2% of the outstanding options of NAVA as at December 31, 1997.
These options may be exercised at a price of $4.18 (U.S.$2.92) per share.
F-10
<PAGE> 67
FINANCIAL POSITION AND EARNINGS
The financial position of NAVA as at December 31, 1997, 1996 and 1995, as
well as the earnings for the years ended December 31, 1997, 1996 and 1995,
presented in accordance with generally accepted accounting principles in
the United States, in thousands of Canadian dollars, are as follows:
<TABLE>
<CAPTION>
1997 1996 1995
------------- ------------- -----------
$ $ $
<S> <C> <C> <C>
Financial position
Total assets............................................. 120,889 168,532 56,264
Total liabilities........................................ 144,957 141,423 10,982
Shareholders' equity..................................... (24,068) 27,109 45,282
Earnings(i)
Revenue.................................................. 13,431 24,149 25,028
Net loss................................................. (59,978) (26,575) (6,844)
</TABLE>
(i) Including a gain of $15,181,000 in 1995 from the sale of common shares
held in BioChem Pharma Inc.
8. CAPITAL ASSETS
<TABLE>
<CAPTION>
1997 1996
------------- -------------
$ $
<S> <C> <C>
Cost
Land...................................................... 5,899 5,812
Buildings................................................. 31,755 31,143
Equipment and leasehold improvements...................... 39,766 35,235
Equipment under capital leases............................ 5,490 4,096
Construction in progress.................................. 39,836 14,119
Rights, licenses and patents.............................. 21,820 12,666
------------- -------------
144,566 103,071
------------- -------------
Accumulated depreciation and amortization
Buildings................................................. 6,195 5,045
Equipment and leasehold improvements...................... 20,924 17,760
Equipment under capital leases............................ 4,516 2,684
Rights, licenses and patents.............................. 3,994 2,439
------------- -------------
35,629 27,928
------------- -------------
Net book value.............................................. 108,937 75,143
============= =============
</TABLE>
The acquisition of capital assets shown in the consolidated statement of
changes in financial position is presented net of construction-related
accounts payable.
9. OTHER ASSETS
<TABLE>
<CAPTION>
1997 1996
----------- -----------
$ $
<S> <C> <C>
Goodwill, at net book value................................. 21,003 24,073
Deferred charges, at net book value......................... 3,538 783
Deferred foreign exchange loss on long-term debt............ 1,954 --
Deferred income taxes....................................... 1,329 --
Other, at cost(a)........................................... 5,859 6,098
----------- -----------
33,683 30,954
=========== ===========
</TABLE>
(a) As at December 31, 1997, other items include an amount of $4,692,000
($4,133,000 as at December 31, 1996) which represents a receivable
arising from a payment in connection with a legal action involving the
use of certain patents, and bears interest at 10.25% (9.25% in 1996).
F-11
<PAGE> 68
10. BANK INDEBTEDNESS
The bank indebtedness is partially secured by the accounts receivable and
inventories of certain of the Company's subsidiaries. The maximum amount of
bank indebtedness authorized is $51,124,000 as at December 31, 1997
($60,431,000 as at December 31, 1996) of which 39% is in Italian lira (54%
as at December 31, 1996). The bank indebtedness bears interest at varying
rates from 2% to 11.75% as at December 31, 1997 (2% to 14.75% as at
December 31, 1996).
11. ACCOUNTS PAYABLE AND ACCRUED LIABILITIES
<TABLE>
<CAPTION>
1997 1996
----------- -----------
$ $
<S> <C> <C>
Accounts payable and accrued liabilities.................... 43,538 40,117
Construction-related accounts payable....................... 3,139 3,893
Unearned revenue............................................ 1,773 2,588
Income taxes payable........................................ 1,448 1,973
----------- -----------
49,898 48,571
=========== ===========
</TABLE>
12. LONG-TERM DEBT
<TABLE>
<CAPTION>
1997 1996
----------- -----------
$ $
<S> <C> <C>
Bank loan, bearing interest at the lender's prime rate,
secured by a hypothec on land and building having a net
book value of $17,789,000, repayable in a final payment of
$7,140,000 in 1998. (a)................................... 7,140 11,000
Bank loans, bearing interest at 9% and 10%, secured by a
hypothec on land and building having a net book value of
$5,023,000, repayable in semi-annual instalments, maturing
in 1999. (b).............................................. 452 801
Bank loan, bearing interest at 1.25% above bank prime rate,
secured by a hypothec on land and building having a net
book value of $1,199,000, repayable in monthly
instalments, maturing in 2002............................. 255 315
Bank loan, bearing interest at the LIBOR rate plus 0.2%
(U.S.$22,855,000), secured by investments having a net
book value of $33,389,000 and maturing in 2002............ 32,623 31,325
Balance of purchase price amounting to U.S.$8,707,000
(U.S.$17,645,000 as at December 31, 1996) bearing interest
at 10.25% (9.25% as at December 31, 1996) increasing by 1%
annually, subordinated in favor of the bank loans bearing
interest at the LIBOR rate plus 0.2%, maturing in 2002. A
subsidiary has undertaken to respect certain financial
ratios. (c)............................................... 12,456 24,184
Bank loans, bearing interest at the lender's prime rate,
secured by a hypothec on a building under construction
having a net book value of $39,836,000, repayable in
annual instalments of $940,000 and final payments
totalling $5,640,000 in 2002. A subsidiary has undertaken
to respect certain financial ratios. (d).................. 9,400 3,000
Federal and provincial government loans, with a maximum
available amount of $5,500,000, non-interest bearing and
repayable in annual instalments of $1,100,000 commencing
four years after completion of a building under
construction, estimated to be completed in 1998........... 3,452 1,270
Loans, bearing interest at rates varying from 4.5% to
11.29%, maturing on various dates from 1998 to 2004.
(b)....................................................... 1,026 1,453
Obligations under capital leases, repayable principally in
Italian lira and maturing on various dates ending in
2001...................................................... 504 707
----------- -----------
67,308 74,055
Current portion............................................. 9,039 16,349
----------- -----------
58,269 57,706
=========== ===========
</TABLE>
F-12
<PAGE> 69
(a) The Company entered into an agreement with the Societe de developpement
industriel du Quebec (SDI) whereby the SDI guarantees, until 1998, 80%
of a maximum loan of $10,000,000. SDI will reimburse the Company the
aggregate interest of this loan during the first five years of the
agreement, to a maximum of $3,125,000.
(b) These loans, totalling 1.6 billion lira (2.2 billion lira as at
December 31, 1996), are repayable by the Italy-based subsidiary.
(c) In the event that a subsidiary fails to repay the balance of purchase
price at maturity in addition to the Company's failure to repay the
balance of purchase price, the seller may choose to be repaid by the
issuance of common shares of the Company. The number of shares issued
will be based on the closing market price of the shares immediately
prior to the default, subject to a maximum of 6,000,000 shares.
(d) The Company entered into an agreement with the SDI whereby the SDI
guarantees, until 2006, 80% of a maximum loan of $4,800,000. SDI will
reimburse the Company the aggregate interest of this loan during the
first five years of the agreement, to a maximum of $1,875,000.
Payments due in each of the next five years are as follows:
<TABLE>
<CAPTION>
OBLIGATIONS UNDER
CAPITAL LEASES OTHER LOANS
----------------- -----------
$ $
<S> <C> <C>
1998........................................................ 282 8,774
1999........................................................ 252 13,800
2000........................................................ 20 1,173
2001........................................................ 12 1,108
2002........................................................ -- 39,597
---------- ---------
566 64,452
Amount representing interest................................ 62 --
---------- ---------
504 64,452
========== =========
</TABLE>
13. OTHER LIABILITIES
<TABLE>
<CAPTION>
1997 1996
--------- ---------
$ $
<S> <C> <C>
Provision for severance pay (a)............................. 4,092 4,338
Deferred foreign exchange gain on long-term debt............ -- 1,695
Deferred income taxes....................................... -- 1,354
Other....................................................... 42 896
--------- ---------
4,134 8,283
========= =========
</TABLE>
(a) The provision for severance pay is recorded by an Italy-based
subsidiary in compliance with applicable statutes. This severance pay
is paid to employees who resign, retire, or for any other reason have
their employment terminated.
F-13
<PAGE> 70
14. CAPITAL STOCK
AUTHORIZED SHARES
An unlimited number of voting common shares, without par value.
ISSUED SHARES
The changes to the Company's capital stock are as follows:
<TABLE>
<CAPTION>
1997 1996 1995
---------- ---------- ---------
<S> <C> <C> <C>
Number of shares
Balance, beginning of year......................... 108,029,740 98,566,368 94,626,868
Issued............................................. -- 8,050,000 3,000,000
Exercise of share options.......................... 225,900 1,413,372 939,500
---------- ---------- ---------
Balance, end of year............................... 108,255,640 108,029,740 98,566,368
========== ========== =========
Weighted average number of common shares
outstanding..................................... 108,152,816 106,485,028 97,044,458
========== ========== =========
Amounts $ $ $
Balance, beginning of year......................... 401,744 154,012 119,277
Issued(a).......................................... -- 238,853 28,527
Exercise of share options.......................... 2,687 8,879 6,208
---------- ---------- ---------
Balance, end of year............................... 404,431 401,744 154,012
========== ========== =========
</TABLE>
(a) Net of related expenses of $12,951,000 in 1996 and $1,473,000 in 1995.
STOCK SPLIT
A two-for-one stock split of common shares took effect on April 7, 1997.
All information relating to common shares reflects retroactively this stock
split.
STOCK PURCHASE OPTIONS
Stock option plan
The Company introduced a stock option plan in 1986, which was subsequently
modified in 1990, 1992, 1995 and 1996. It is intended for directors,
officers, employees and consultants of the Company. The total number of
options that may be granted under the terms of the plan cannot exceed ten
million. The exercise price of options granted under the plan is determined
by the Board of Directors of the Company and cannot be lower than the
market value on the date the options are granted. These options expire no
later than ten years after the date they are granted.
The changes to the number of stock options granted by the Company are as
follows:
<TABLE>
<CAPTION>
1997 1996 1995
-------- ---------- --------
<S> <C> <C> <C>
Balance, beginning of year.............................. 4,434,800 4,774,180 5,171,600
Granted................................................. 2,050,500 1,075,000 659,000
Exercised at a weighted average price of $11.89 in 1997,
$6.48
in 1996 and $6.61 in 1995............................. (225,900) (1,207,580) (939,500)
Cancelled............................................... (76,800) (206,800) (116,920)
-------- ---------- --------
Balance, end of year.................................... 6,182,600 4,434,800 4,774,180
======== ========== ========
Weighted average price of options outstanding at end of
year.................................................. $ 21.96 $ 15.14 $ 9.43
======== ========== ========
Options exercisable at end of year...................... 2,877,700 2,519,800 3,381,580
======== ========== ========
</TABLE>
F-14
<PAGE> 71
The information about stock options outstanding as at December 31, 1997 is
as follows:
<TABLE>
<CAPTION>
OPTIONS OUTSTANDING OPTIONS EXERCISABLE
---------------------------------- --------------------
WEIGHTED
AVERAGE WEIGHTED WEIGHTED
REMAINING AVERAGE AVERAGE
CONTRACTUAL EXERCISE EXERCISE
EXERCISE PRICE NUMBER LIFE PRICE NUMBER PRICE
-------------- -------- ----------- --------- -------- ---------
<S> <C> <C> <C> <C> <C>
$ $
$6.19 to $7.50........................... 784,000 6.6 YEARS 6.81 485,200 6.75
$7.51 to $10.00.......................... 394,300 5.7 YEARS 8.58 237,100 8.40
$10.01 to $15.00......................... 1,642,000 4.2 YEARS 11.17 1,642,000 11.17
$15.01 to $22.50......................... 275,000 5.7 YEARS 17.80 197,000 17.42
$22.51 to $33.00......................... 1,099,800 8.7 YEARS 29.81 316,400 29.99
$33.01 to $40.00......................... 1,987,500 9.2 YEARS 35.73 -- --
-------- --------- -------- ---------
6,182,600 21.96 2,877,700 12.69
======== ========= ======== =========
</TABLE>
Societe de developpement industriel du Quebec (SDI)
In consideration for the guarantee of a subsidiary's loan relating to a
building and reimbursement of interest on this loan, the Company has
granted the SDI an option to purchase 123,476 common shares at an exercise
price of $5.15 per share. This option expires in July 2001.
SHAREHOLDER RIGHTS PLAN
During 1995, the shareholders of the Company approved a Shareholder Rights
Plan (Rights Plan). Under the Rights Plan, one common share purchase right
was issued on April 28, 1995 in respect of each outstanding common share
and a share purchase right for each common share issued thereafter. These
rights are exercisable in a situation of public offering where certain
conditions are not respected. Each right entitles the holder to purchase,
from the Company, one common share at a specific price, subject to certain
anti-dilution adjustments. The Rights Plan expires on June 30, 2000 or
unless terminated earlier by the Company's Board of Directors. The purpose
of the Rights Plan is to require anyone, who seeks to acquire 20% or more
of the Company's voting shares, to present a bid complying with specific
provisions.
RESERVED SHARES
The Company has reserved 6,000,000 common shares for the eventual repayment
of a subsidiary's balance of purchase price and 1,500,000 common shares
under a conversion right agreement with a shareholder of a subsidiary.
15. FOREIGN CURRENCY TRANSLATION ADJUSTMENT
<TABLE>
<CAPTION>
1997 1996
--------- ---------
$ $
<S> <C> <C>
Balance, beginning of year.................................. 2,688 2,576
Effect of foreign exchange rate variations upon translation
of the net assets
of self-sustaining foreign operations, net of related
income taxes.............................................. (289) 112
--------- ---------
Balance, end of year........................................ 2,399 2,688
========= =========
</TABLE>
F-15
<PAGE> 72
16. INFORMATION ON THE CONSOLIDATED STATEMENT
OF CHANGES IN FINANCIAL POSITION
<TABLE>
<CAPTION>
1997 1996 1995
------------- ------------- -------------
$ $ $
<S> <C> <C> <C>
Non-cash items
Depreciation and amortization............................ 11,092 11,457 13,042
Share of loss of an affiliated company, net of gain on
dilution.............................................. 6,595 4,113 8,101
Non-controlling interest................................. (1,987) 211 484
Deferred income taxes.................................... 260 (384) (927)
Realization of foreign currency translation adjustment... -- -- 701
Amortization of deferred foreign exchange gains and
losses................................................ 1,543 (725) (547)
Other.................................................... (127) 473 (1,412)
------------- ------------- -------------
17,376 15,145 19,442
============= ============= =============
Changes in non-cash working capital items
Accounts receivable...................................... (15,614) (12,589) (8,034)
Inventories.............................................. (831) (1,801) (1,262)
Prepaid expenses......................................... (2,328) (81) 1,267
Accounts payable and accrued liabilities, excluding
construction-related accounts payable................. 5,424 3,527 (3,439)
------------- ------------- -------------
(13,349) (10,944) (11,468)
============= ============= =============
</TABLE>
17. RELATED PARTY TRANSACTIONS
Transactions with a shareholder are as follows:
<TABLE>
<CAPTION>
1997 1996 1995
------------- ------------- -------------
$ $ $
<S> <C> <C> <C>
Royalty revenue............................................ 124,130 56,422 10,082
============= ============= =============
Revenue from research and development contracts............ -- -- 5,000
============= ============= =============
Milestone repayments....................................... -- 4,552 1,825
============= ============= =============
</TABLE>
The Company incurred professional fees with two law firms, in which certain
of the Company's directors are partners, totalling $356,000 for the year
ended December 31, 1997 ($640,000 for the year ended December 31, 1996 and
$429,000 for the year ended December 31, 1995).
These transactions were concluded in the normal course of operations, at
the exchange amount.
The Company entered into a subscription agreement with a shareholder for
the issuance of common shares of a subsidiary to this shareholder for
$12,650,000. During the year, common shares totalling $2,650,000 were
subscribed by this shareholder ($7,500,000 for the year ended December 31,
1996 and $2,500,000 for the year ended December 31, 1995). In addition, a
conversion right agreement has been signed with this shareholder allowing
the conversion, in certain circumstances, of the common shares of the
subsidiary into common shares of the Company.
18. COMMITMENTS AND CONTINGENCIES
The Company rents premises under operating leases which expire in 2008. The
aggregate minimum rental commitment amounts to $10,437,000 and the
aggregate minimum rental commitment for each of the following five years is
$2,938,000 in 1998, $2,090,000 in 1999, $1,451,000 in 2000, $1,374,000 in
2001 and $1,394,000 in 2002.
During the year the Company has undertaken to subscribe to an interest in a
company and a partnership for an amount totalling $45,914,000. As at
December 31, 1997 an amount of $9,706,000 has been subscribed.
F-16
<PAGE> 73
In 1996, a legal proceeding was instituted in the United States against the
Company and Glaxo Wellcome for alleged patent infringement on a product
licensed to Glaxo Wellcome. The action seeks monetary damages relating to
the sale of the product in the United States. In the opinion of management,
the claim is without merit and the Company is vigorously opposing the
allegation. In addition, the Company is involved in other claims and
lawsuits in the normal course of business. It is not possible at this time
to determine the ultimate outcome of any of these claims.
19. SEGMENTED INFORMATION
The Company operates in the following industry segments:
<TABLE>
<CAPTION>
1997 1996 1995
----------------- ----------------- -----------------
$ $ $
<S> <C> <C> <C>
Operating revenue
Therapeutic........................................... 140,064 65,990 17,438
Diagnostic............................................ 117,952 143,882 158,385
Vaccine............................................... 9,471 11,566 8,484
Other................................................. 13,295 12,180 3,084
----------------- ----------------- -----------------
280,782 233,618 187,391
================= ================= =================
Net Income (loss)
Therapeutic........................................... 84,372 29,533 (2,367)
Diagnostic............................................ (1,858) 2,011 4,586
Vaccine............................................... (5,296) (566) 123
Share of loss of an affiliated company................ (6,595) (4,113) (8,101)
Other................................................. 9,215 6,529 792
----------------- ----------------- -----------------
79,838 33,394 (4,967)
================= ================= =================
Depreciation and Amortization
Therapeutic........................................... 2,491 1,601 1,506
Diagnostic............................................ 7,793 9,295 10,972
Vaccine............................................... 597 316 345
Other................................................. 211 245 219
----------------- ----------------- -----------------
11,092 11,457 13,042
================= ================= =================
Total Assets
Therapeutic........................................... 129,592 61,396
Diagnostic............................................ 167,197 165,870
Vaccine............................................... 66,152 43,135
Other................................................. 292,331 301,864
----------------- -----------------
655,272 572,265
================= =================
</TABLE>
F-17
<PAGE> 74
The Company operates in the following geographic segments:
<TABLE>
<CAPTION>
1997 1996 1995
----------------- ----------------- -----------------
$ $ $
<S> <C> <C> <C>
Operating revenue
Canada................................................ 47,976 41,203 23,089
United States......................................... 95,504 89,779 55,270
Italy................................................. 81,879 98,180 96,821
Europe, other than Italy.............................. 116,808 70,682 83,150
Other................................................. 46,208 10,594 7,468
Inter-segment......................................... (107,593) (76,820) (78,407)
----------------- ----------------- -----------------
280,782 233,618 187,391
================= ================= =================
Depreciation and Amortization
Canada................................................ 3,226 2,760 3,026
United States......................................... 1,782 2,445 2,608
Italy................................................. 3,994 4,487 5,307
Europe, other than Italy.............................. 1,001 1,235 1,811
Other................................................. 1,089 530 290
----------------- ----------------- -----------------
11,092 11,457 13,042
================= ================= =================
Total Assets
Canada................................................ 481,023 395,990
United States......................................... 46,263 74,014
Italy................................................. 107,443 114,360
Europe, other than Italy.............................. 119,785 85,059
Other................................................. 55,019 49,885
Investment in an affiliated company................... 5,194 12,166
Inter-segment......................................... (159,455) (159,209)
----------------- -----------------
655,272 572,265
================= =================
</TABLE>
20. FINANCIAL INSTRUMENTS
TEMPORARY INVESTMENTS
Temporary investments totalling $296,547,000 as at December 31, 1997
($289,885,000 as at December 31, 1996) include term deposits, bankers'
acceptances and loans maturing within three months. As at December 31,
1997, temporary investments totalling $180,577,000 ($197,865,000 as at
December 31, 1996) were invested with a Canadian chartered bank and its
subsidiaries. The Company has classified temporary investments as held to
maturity and has recorded these investments at cost.
CURRENCY FLUCTUATIONS RELATED TO INTERNATIONAL OPERATIONS
Most of the Company's diagnostic product sales are in international markets
and the Company expects that this will continue. Sales of the Company's
products in international markets are subject to certain risks associated
with such sales including government regulations, export and import license
requirements, risks of tariffs or trade barriers and political and economic
instability. Although these risks have not had any material effect on the
Company to date, there can be no assurance that these risks will not have a
material adverse effect on the Company in the future.
FAIR VALUE OF FINANCIAL INSTRUMENTS
The Company uses the following methods and assumptions to estimate the fair
value of each class of financial instruments:
CASH AND TEMPORARY INVESTMENTS, BANK INDEBTEDNESS, ACCOUNTS PAYABLE AND
ACCRUED LIABILITIES
The carrying amounts approximate fair value due to the short-term maturity
of these instruments.
F-18
<PAGE> 75
ACCOUNTS RECEIVABLE
The carrying amount approximates the fair value due to the short-term
maturity of these instruments, with the exception of the trade receivables
from certain Italian government organizations, where it is not practicable
to estimate the fair value as it is not possible to accurately predict the
timing of future payments. The original maturity date does not usually
exceed a period of 90 days, but for the Italian market, it is common
practice with government organizations to pay trade accounts receivable in
a period exceeding one year. The trade accounts receivable relating to
these organizations totalled $19,778,000 as at December 31, 1997
($25,504,000 as at December 31, 1996) and bear interest at varying rates
from 7% to 10%. Adequate provisions were recorded for potential doubtful
accounts on these trade accounts receivable.
INVESTMENTS IN PRIVATE COMPANIES
The fair value of the investments in private companies is not readily
determinable because these investments are not publicly traded. The Company
believes that the carrying amount approximates the fair value.
SHARES OF PUBLIC COMPANIES
The fair value of the shares of public companies is established based on
the closing market price as at the balance sheet date. As at December 31,
1997, the fair value of these shares amounted to $6,698,000 ($5,413,000 as
at December 31, 1996).
OTHER ASSETS
Other assets include amounts receivable with a carrying amount of
$4,692,000 ($4,133,000 as at December 31, 1996) for which the fair value is
estimated using discounted cash flow analyses based on the Company's actual
borrowing rate on loans. The fair value of these amounts receivable is
$5,048,000 ($4,465,000 as at December 31, 1996).
LONG-TERM DEBT
The fair value is estimated using discounted cash flow analyses, based on
the Company's current incremental borrowing rates for similar types of
arrangements. There is no material difference between the carrying value
and the fair value of the long-term debt as at December 31, 1997 with the
exception of the balance of purchase price of $12,456,000 as at December
31, 1997 ($24,184,000 as at December 31, 1996) for which the fair value
amounts to $13,400,000 ($26,129,000 as at December 31, 1996) and the
Federal and provincial government loans, for which the fair value is not
readily determinable without comparing to similar types of arrangements.
OTHER LIABILITIES
The other liabilities include severance pay for which the fair value
approximates the carrying amount as it is indexed according to the consumer
price index fixed by Italian law.
F-19
<PAGE> 76
21.SUMMARY OF DIFFERENCES BETWEEN GENERALLY ACCEPTED ACCOUNTING PRINCIPLES IN
CANADA AND IN THE UNITED STATES
The consolidated financial statements have been prepared in accordance with
generally accepted accounting principles (GAAP) in Canada which differ in
certain respects from those principles that the Company would have followed
had the consolidated financial statements been prepared in accordance with
U.S. GAAP. Had the Company followed U.S. GAAP, certain items on the
consolidated balance sheet would have increased (decreased) as follows:
<TABLE>
<CAPTION>
1997 1996
------------- -------------
$ $
<S> <C> <C> <C>
CONSOLIDATED BALANCE SHEET
Cash and temporary investments(a)........................... (64,788) (14,870)
Temporary investments maturing in more than three
months(a)................................................. 64,788 14,870
Investments(b).............................................. (1,425) 319
Deferred foreign exchange gains and losses on long-term
debt( (c)................................................. (1,954) (1,695)
Deferred income taxes -- liabilities(c) (d)................. (247) 737
Shareholders' equity
Retained earnings......................................... (1,575) 1,659
Share of the unrealized investment holding gains and
losses(b).............................................. (1,425) 319
Foreign currency translation adjustment(e)................ (701) (701)
</TABLE>
In addition, the net income (loss) would differ as follows:
<TABLE>
<CAPTION>
1997 1996 1995
------------- ------------- -------------
$ $ $
<S> <C> <C> <C>
CONSOLIDATED STATEMENT OF EARNINGS
Net income (loss) per Canadian GAAP......................... 79,838 33,394 (4,967)
Deferred foreign exchange gains (losses) on long-term
debt(c)................................................... (3,649) 324 2,023
Realization of foreign currency translation adjustment(e) -- -- 701
Deferred income taxes(c) (d)................................ 984 (204) (533)
------------- ------------- -------------
Net income (loss) per U.S. GAAP............................. 77,173 33,514 (2,776)
============= ============= =============
Earnings (loss) per common share per U.S. GAAP(f)
Primary................................................... 0.71 0.31 (0.03)
============= ============= =============
Fully-diluted............................................. 0.70 0.31 (0.03)
============= ============= =============
</TABLE>
(a) CASH AND TEMPORARY INVESTMENTS
Under Canadian GAAP, temporary investments whose maturity date is greater
than three months from the acquisition date are disclosed as cash in the
consolidated balance sheet and in the consolidated statement of changes in
financial position. Under U.S. GAAP, these investments would be disclosed
separately as temporary investments in the consolidated balance sheet and
as investing activities in the consolidated statement of changes in
financial position.
(b) INVESTMENTS
Under Canadian GAAP, investments in shares of public companies, including
those shares held by an affiliated company, should be recorded at cost,
less any decrease in value other than a temporary decline.
Under the U.S. GAAP, the Company would be required to record investments in
shares of public companies that represent an available-for-sale investment
at fair value and would have presented the unrealized gains or losses as a
separate item in shareholders' equity. Furthermore, the Company would have
accounted for its share of the unrealized gains or losses of the affiliated
company.
F-20
<PAGE> 77
<TABLE>
<CAPTION>
1997 1996 1995
------ ------ ------
$ $ $
<S> <C> <C> <C>
Changes in the unrealized gains or losses during the year:
Investments in public companies held by the Company....... (1,533) -- --
INVESTMENTS IN PUBLIC COMPANIES HELD BY THE AFFILIATED
COMPANY................................................ (211) (3,375) 215
------ ------ ------
(1,744) (3,375) 215
====== ====== ======
COST, HELD BY THE COMPANY................................... 8,231 6,899
====== ======
FAIR VALUE, HELD BY THE COMPANY............................. 6,698 5,413
====== ======
</TABLE>
(c) DEFERRED FOREIGN EXCHANGE GAINS AND LOSSES ON LONG-TERM DEBT
Under Canadian GAAP, unrealized foreign exchange gains and losses arising
on the translation of long-term monetary items are deferred and amortized
over the life of the item. Under U.S. GAAP, these gains or losses would be
included in earnings as they arise. The deferred foreign exchange losses on
the balance sheet amounting to $1,954,000 as at December 31, 1997 would
have been eliminated (gains of $1,695,000 as at December 31, 1996). In
addition, a foreign exchange loss amounting to $3,649,000 would have been
recognized in earnings for the year ended December 31, 1997 (foreign
exchange gains of $324,000 and $2,023,000 would have been recognized in
earnings for the years ended December 31, 1996 and 1995 respectively). The
provision for deferred income taxes would have decreased by $744,000 for
the year ended December 31, 1997 (increased by $204,000 and $533,000 for
the years ended December 31, 1996 and 1995 respectively) and is
attributable to foreign operations.
(d) DEFERRED INCOME TAXES
Under U.S. GAAP, deferred tax assets or liabilities would be recorded for
temporary differences that will result in deductible amounts or taxable
amounts in future years as well as for loss carry-forwards and deferred
investment tax credits. A valuation allowance would be recorded for the
portion of the asset considered unrealizable. In addition, the deferred tax
asset or liability must be calculated at the current rate disclosed by
government authorities. Both the deferred tax asset and valuation allowance
have been valued at $49,600,000 as at December 31, 1997 ($39,676,000 as at
December 31, 1996 and $23,330,000 as at December 31, 1995).
(e) REALIZATION OF FOREIGN CURRENCY TRANSLATION ADJUSTMENT
Under Canadian GAAP, a portion of the foreign currency translation
adjustment is recognized in earnings on repatriation of capital from
foreign operations. Under U.S. GAAP, adjustments to the foreign currency
translation adjustment are only made if there is a reduction in ownership
to a third party.
(f) EARNINGS PER SHARE
During 1997, the method of computing earnings per share under U.S. GAAP was
changed to be closer to Canadian GAAP. Under U.S. GAAP, fully-diluted
earnings per share is calculated based on the assumption that the options
have been exercised at the beginning of the year or at the date granted, if
granted during the year, and proceeds from the exercise of options were
used at the beginning of the year to acquire common shares of the Company
at the average market price. Under Canadian GAAP, fully-diluted earnings
per common share assumes that all the outstanding options at the end of the
year have been exercised at the beginning of the year or at the date
granted, if granted during the year, and proceeds from the exercise of
options have been used for investments.
(g) EARNINGS BEFORE DEPRECIATION, AMORTIZATION AND OTHER
United States GAAP does not permit the disclosure of a subtotal of the
amount of earnings before depreciation, amortization and other. Canadian
GAAP permits the disclosure of a subtotal of the amount of earnings before
the items referred to above.
F-21
<PAGE> 78
<TABLE>
<CAPTION>
1997 1996 1995
------- ------- -------
$ $ $
<S> <C> <C> <C>
Earnings before depreciation, amortization and other..... 97,602 50,626 22,103
Depreciation and amortization............................ (11,092) (11,457) (13,042)
Share of loss of an affiliated company, net of gain on
dilution (Note 7)...................................... (6,595) (4,113) (8,101)
------- ------- -------
Earnings before income taxes and minority interests...... 79,915 35,056 960
======= ======= =======
</TABLE>
CONSOLIDATED STATEMENT OF CHANGES IN FINANCIAL POSITION
Under Canadian GAAP, the bank indebtedness of $22,967,000 as at December
31, 1997 ($12,981,000 as at December 31, 1996 and $22,184,000 as at
December 31, 1995) is considered a cash reduction and therefore any
increase in bank indebtedness is not presented as a financing activity.
Under U.S. GAAP, any increase in bank indebtedness would be presented as a
financing activity.
Additional information required under U.S. GAAP:
<TABLE>
<CAPTION>
1997 1996 1995
--------- --------- ---------
$ $ $
<S> <C> <C> <C>
Interest paid............................................... 6,691 7,605 7,809
Income taxes paid........................................... 2,573 2,612 2,687
</TABLE>
ACCOUNTING FOR COMPENSATION PROGRAMS
The Company has chosen to continue to measure compensation costs related to
awards of stock options using the intrinsic value based method of
accounting. Under U.S. GAAP, the Company is required to make pro forma
disclosure of net income (loss), as if the fair value based method of
accounting had been applied. The fair value of options granted was
estimated using the Black-Scholes option-pricing model with an expected
life of 7.5 years, a risk-free interest rate of 6.42% in 1997 (7.18% in
1996 and 8.59% in 1995) and an expected volatility of 40% in 1997 (40% in
1996 and 45% in 1995).
The Company's net income, earnings per share and fully-diluted earnings per
share would have been reduced for the years ended December 31, 1997 and
1996 (the net loss, loss per share and fully-diluted loss per share for the
year ended December 31, 1995 would have been increased), on a pro forma
basis, as follows:
<TABLE>
<CAPTION>
1997 1996 1995
----------- --------- -------
$ $ $
<S> <C> <C> <C>
Net income pro forma........................................ 10,991 3,310 663
Earnings per share pro forma................................ 0.10 0.03 0.01
Fully-diluted earnings per share pro forma.................. 0.10 0.03 0.01
</TABLE>
These pro forma effects on net income in 1997 and 1996 (net loss in 1995)
are not necessarily representative of the pro forma effect on net income in
future years because it does not take into consideration expenses related
to options granted prior to January 1, 1995.
The weighted average fair value of options granted in 1997 was $21.03
($17.35 in 1996 and $8.38 in 1995).
22. SUBSEQUENT EVENT
On February 9, 1998 the Company's Board of Directors approved the filing of
a preliminary prospectus on behalf of CliniChem Development Inc.
(CliniChem). CliniChem was formed by the Company for the purpose of
continuing the research and development of a number of the Company's
therapeutic and vaccine candidates. Upon receipt of the required approvals,
the Company will contribute $150,000,000 to CliniChem as a capital
contribution and shares of CliniChem will then be distributed to the
shareholders of BioChem as a dividend-in-kind.
F-22
<PAGE> 79
BIOCHEM PHARMA INC.
SCHEDULES
DECEMBER 31, 1997, 1996 AND 1995
<TABLE>
<S> <C> <C>
Schedule VIII -- Reserves
Schedule IX -- Short-term borrowings
Schedule X -- Supplementary earnings statement information
</TABLE>
F-23
<PAGE> 80
BIOCHEM PHARMA INC.
SCHEDULE VIII -- RESERVES
<TABLE>
<CAPTION>
BALANCE CHARGED TO BALANCE
AT BEGINNING COSTS AND CHARGED TO AT END
OF YEAR EXPENSES OTHER ACCOUNTS(A) DEDUCTIONS(B) OF YEAR
------------ ---------- ----------------- ------------- --------
$ $ $ $ $
<S> <C> <C> <C> <C> <C>
AS AT DECEMBER 31, 1997
ALLOWANCE FOR DOUBTFUL
ACCOUNTS................. 3,497,000 444,000 199,000 1,505,000 2,635,000
======== ========= ========= ========= ========
As at December 31, 1996
Allowance for doubtful
accounts................. 1,861,000 2,115,000 32,000 511,000 3,497,000
======== ========= ========= ========= ========
As at December 31, 1995
Allowance for doubtful
accounts................. 2,780,182 1,178,000 158,000 2,255,182 1,861,000
======== ========= ========= ========= ========
</TABLE>
(a) Adjustments related to foreign exchange rate fluctuations of foreign
subsidiaries
(b) Uncollectible accounts written off, net of recoveries
F-24
<PAGE> 81
BIOCHEM PHARMA INC.
SCHEDULE IX -- SHORT-TERM BORROWINGS
AS AT DECEMBER 31, 1997, 1996 AND 1995
<TABLE>
<CAPTION>
BALANCE WEIGHTED MAXIMUM AVERAGE WEIGHTED
AT END AVERAGE AMOUNT DURING AMOUNT DURING AVERAGE INTEREST
OF YEAR INTEREST RATE THE YEAR THE YEAR DURING THE YEAR
--------- ------------- ------------- ------------- ----------------
$ % $ $ %
<S> <C> <C> <C> <C> <C>
LINE OF CREDIT
DECEMBER 31, 1997........ 22,967,000 8.57 27,117,985 19,091,221 7.88
========= ========= ========= ========= =======
December 31, 1996........ 12,981,000 9.10 28,811,000 20,674,000 9.24
========= ========= ========= ========= =======
December 31, 1995........ 22,184,000 10.13 25,501,000 15,295,615 9.69
========= ========= ========= ========= =======
</TABLE>
F-25
<PAGE> 82
BIOCHEM PHARMA INC.
SCHEDULE X -- SUPPLEMENTARY EARNINGS STATEMENT INFORMATION
<TABLE>
<CAPTION>
YEARS ENDED DECEMBER 31,
-----------------------------------
1997 1996 1995
--------- --------- ---------
<S> <C> <C> <C>
Maintenance and repairs............................... $3,083,512 $2,508,260 $1,780,251
========= ========= =========
Taxes
On capital -- Quebec................................ 780,744 1,469,634 542,786
Municipal and business.............................. 1,871,988 1,666,465 1,423,909
--------- --------- ---------
2,652,732 3,136,099 1,966,695
========= ========= =========
Royalties............................................. 1,688,000 820,000 2,142,000
========= ========= =========
Advertising cost...................................... 1,628,753 1,498,250 1,535,613
========= ========= =========
</TABLE>
F-26