Date:
20121024
Docket:
T-1144-05
Citation:
2012 FC 1235
Toronto, Ontario, October 24, 2012
PRESENT: The Honourable Mr. Justice Hughes
BETWEEN:
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APOTEX INC.
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Plaintiff
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and
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MERCK CANADA INC. and MERCK
FROSST CANADA & CO.
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Defendants
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PUBLIC REASONS
FOR JUDGMENT AND JUDGMENT
[1]
This
is a continuation of an action commenced by the Plaintiff Apotex in 2005 for
compensation for any loss suffered by it as against the Defendants,
collectively Merck, under the provisions of section 8 of the Patented
Medicines (Notice of Compliance) Regulations, SOR/93-133, as amended (NOC
Regulations). The purpose of this present part of that action is to seek to
quantify that loss. For the reasons that follow I have made findings as to the
matters in controversy and ask that the accounting experts for each of the
parties, on the basis of these findings, and including the matters agreed upon,
collaborate to produce a final calculation as to the amount of compensation. I
have asked for submissions as to costs. Following receipt of the foregoing,
final Judgment will be issued.
INDEXING
[2]
For
convenience, the matters considered in these Reasons can be found at the
following paragraphs:
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LITIGATION
HISTORY
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Paras
3 - 8
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THE
ISSUES
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Paras
9 - 11
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THE
EVIDENCE
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Paras 12 - 34
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THE
“BUT FOR” WORLD, WHO BEARS THE BURDEN
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Paras 35 - 38
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WHAT
IS THE RELEVANT PERIOD
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Paras 39
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OVERALL
SIZE OF THE ALENDRONATE MARKET
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Paras 40 - 41
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GENERIC
SHARE OF THE OVERALL ALENDRONATE MARKET
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Para 42
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APOTEX’S
SHARE OF THE GENERIC MARKET
- Capacity
- Motivation
- Formlulary
Listing
- Ontario
- Saskatchewan
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Paras 43 –
Paras 45 – 47
Paras 48 – 49
Paras 50 - 69
Paras 59 – 64
Paras 65 - 69
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FORMULARY
LISTINGS FOR THE NOVOPHARM AND COBALT ALENDRONATE PRODUCTS
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Paras 70 - 73
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AT
WHAT PRICE WOULD APOTEX OF SOLD ITS PRODUCT
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Paras 74 - 80
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DOUBLE
RAMP-UP
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Paras 81 - 87
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DEDUCTIONS
- Agreed
Deductions
- Rebates
- Free
Goods
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Paras 88 – 104
Paras 88 – 91
Paras 92 - 101
Paras 102 - 104
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INTEREST
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Paras 105 - 106
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CONCLUSION
AND COSTS
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Paras
107 - 108
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LITIGATION
HISTORY
[3]
I
will repeat what I wrote in my earlier decision in this action cited as 2008 FC
1185 at paragraphs 3 to 7:
FACTUAL BACKGROUND
3 Counsel for the parties are to be commended
for co-operating in providing an agreement as to facts and documents (Exhibit
1). The Plaintiff, Apotex Inc., is what is known colloquially as a generic drug
company which manufactures and markets primarily generic versions of
pharmaceuticals in Canada. In the PMNOC Regulations, Apotex is referred to as a
"second party". The two Merck Canadian companies Merck Frosst Canada
Ltd. and Merck Frosst Canada & Co. (collectively referred to in these
reasons as Merck) are the Canadian branch of a multinational organization which
manufactures and markets are what are commonly referred to as "brand
name" or "originator" or "innovator" pharmaceuticals
and are what is referred to as "first person" under the PMNOC
Regulations. Merck & Co. Inc., a United States company, was named as a
party defendant in this action but shortly before trial, an Order was issued,
on consent, discontinuing this action against that entity.
4 The pharmaceutical of interest in this action
is a drug commonly known as alendronate which is used primarily in the treatment
of osteoporosis. Merck has an interest in a patent, Canadian Patent 2,294,595
('595) which, among other things, includes claims directed to a particular
dosage regimen for the use of that known drug, alendronate, in the treatment of
osteoporosis, a known use. Merck listed the '595 patent with the Minister of
Health under the provisions of the PMNOC Regulations which meant that any
generic seeking approval to sell a generic version of alendronate in Canada for
the patented dosage regimen for the treatment of osteoporosis and wanting to
take advantage of simply referencing approvals already given to Merck for that
drug could file an Abbreviated New Drug Submission (ANDS). In so doing a
generic is required to send a notice to Merck alleging, among other things,
that the '595 patent would not be infringed or was invalid, thereby permitting
Merck to commence an application in this Court to prohibit the generic from
marketing its generic version of alendronate in Canada in the dosage regimen
claimed in the '595 patent.
5 Merck received an NOC approving for sale its
version of alendronate in Canada on February 4, 2002. Apotex filed an ANDS for
alendronate on February 7, 2003 and sent a Notice of Allegation to Merck on
April 14, 2003 alleging that the '595 patent was invalid for a number of
reasons. On May 29, 2003, Merck & Co. Inc. and Merck Frosst Canada &
Co. commenced proceedings in this Court, T-884-03, to prohibit the Minister of
Health from issuing a Notice of Compliance to Apotex which otherwise would permit
Apotex to sell a generic version of the alendronate drug in Canada. On February
3, 2004 the Minister send a letter to Apotex advising it that its application
was approved but would be held in abeyance subject to the Court proceedings. On
May 26, 2005, Mosley J. of this Court gave Reasons and an Order in T-884-03,
dismissing Merck's application, finding that Apotex's allegations as to
invalidity, on some but not all grounds, were justified. These Reasons are
cited as 2005 FC 755. No appeal was taken. On May 27, 2005, the Minister issued
a Notice of Compliance to Apotex permitting it to sell its generic version of
alendronate, Apo-alendronate, in Canada.
6 On July 5, 2005, Apotex instituted this action
T-1144-05 claiming recovery against Merck under the provisions of section 8 of
PMNOC Regulations for the period from February 3, 2004 to May 27, 2005.
7 By Orders of this Court dated January 24, 2006
and August 14, 2008, the quantification of any amounts found to be properly
recoverable in this action is a matter to be determined at a subsequent trial.
The two preliminary issues previously referred to are the subject of the
present trial.
[4]
I
delivered the following Judgment after that trial:
JUDGMENT
For the Reasons
provided herein:
THE COURT ADJUDGES that:
1. Section 8 of the Patented Medicines
(Notice of Compliance) Regulations SOR/93-133 as amended (SOR/98-166) effective
until 2006 is:
a. within the competence of the Federal
Court to hear and determine an action brought thereunder;
b. enabled by the Patent Act, R.S.C. 1985,
c. P-4 as amended S.C. 1993, c. 2, s. 4; and
c. intra vires the constitutional authority
of the federal Parliament of Canada
2. In this action brought under the
provisions of said section 8:
a. Apotex Inc. is not entitled to elect an
account or the disgorgement of the profits of the Respondent, Merck Frosst
Canada Ltd. or Merck Frosst Canada & Co.;
b. Apotex Inc. is entitled to claim damages
or its lost profits for the period from February 3, 2004 to May 26, 2005; and
c. Apotex Inc. is entitled to claim damages
for lost sales and lost permanent market share as claimed in paragraphs 1
(a)(ii) of its Further Amended Statement of Claim dated October 6, 2008 for a
period beyond May 26, 2005 provided it is shown in evidence that such loss was
not rectified and could not have been rectified before that date;
3. The quantification of the damages or lost
profits referred to in paragraph 2 above shall be the subject of the further
trial as set out in the Order of this Court dated August 14, 2008.
Any party is entitled to seek case management by the
Prothonotary assigned to this action for directions as to the procedure to be
followed in respect of said trial;
4. No party is entitled to costs of this
present portion of the trial of this action.
[5]
Merck
appealed from my Judgment and the matter was heard by the Federal Court of
Appeal; which Court delivered Reasons for Judgment, cited as 2009 FCA 187.
Judgment was delivered by that Court as follows on June 4, 2009:
JUDGMENT
[1] The appeal is allowed in part, paragraph 2
(c) of the judgment rendered by the Federal Court Judge is set aside, and
giving the judgment which ought to have been given, it is held that Apotex’s
claim for damages for lost sales and lost permanent market share must be
confined to such losses which can be shown to have been incurred during the
section 8 period. Costs computed at the mid-level of Column I of Tariff B are
awarded in favour of the appellant.
[2] Apotex’s cross-appeal is dismissed with
costs computed at the mid-level of Column III of Tariff B.
[6]
Thus,
the present trial came before me commencing on September 17, 2012. The
parameters of the task before me are contained in paragraphs 2(b) and 2(c) of
my Judgment as modified by the Federal Court of Appeal and may be restated as
follows:
2(b) Apotex Inc. is entitled to claim damages
or lost profits for the period from February 3, 2004 to May 26, 2005 (the
section 8 period); and
2(c) Apotex Inc.’s claim for damages for lost
sales and lost permanent market share must be confined to such losses which can
be shown to have incurred during the section 8 period.
[7]
As
to liability, the parties have entered into an Undertaking whereby each of the
Defendants Merck Frosst Canada & Co. and Merck Frosst Canada Ltd. have
agreed that any order or judgment for monetary relief against either of them in
this action may be enforced by Apotex against either of them, subject to their
right to appeal or seek a stay.
[8]
It
must also be noted that during trial I was advised that about a year and a half
ago the Defendant previously called Merck Frosst Canada Ltd. changed its name
to Merck Canada Inc. I made an Order changing the style of cause to reflect
this change.
THE ISSUES
[9]
Having
regard to my Judgment, as modified by the Court of Appeal as set out above, my
task is to arrive at a calculation of the “loss suffered by Apotex” during the
period from February 3, 2004 to May 26, 2005, based on a hypothetical situation
that Apotex had not been impeded from entering the Canadian marketplace with
its 70 mg Apo-alendronate tablets by any NOC proceedings taken by Merck.
[10]
I
am obliged to my colleague Justice Snider, who, in two recent decisions, Apotex
Inc v Sanofi-Aventis, 2012 FC 553, and Sanofi-Aventis Canada Inc v Teva
Canada Limited, 2012 FC 552, has provided a clear and useful roadmap as to
how to approach such a calculation. I propose to follow, by and large, that
roadmap by addressing the following issues:
a. The
“But For” World, who bears the burden
b. What
is the relevant period?
c. What
is the overall size of the alendronate market in that period?
d. What
would have been the size of the generic share of the overall alendronate market
in that period?
e. What
would have been Apotex’s share of that generic share in that period?
o When
would Apotex have been alone in that market?
o When,
if at all, would Cobalt have entered that market?
o When,
if at all, would Novopharm have entered that market?
f. At
what price would Apotex have sold in that market in that period?
o When
the sole generic?
o When in
competition with other generic(s)?
o Compensation
for double ramp-up
g. What
deductions, if any, should be made from the selling price?
o
agreed
deductions
o
rebates
o
free
goods
§ How is
pre-judgment interest to be calculated?
[11]
I
will first review the evidence.
THE
EVIDENCE
[12]
At
the trial before me in September 2012, the Plaintiff Apotex provided evidence
from two expert witnesses and five witnesses as to fact. Portions of the
transcript and exhibits from Apotex’s discovery of Merck were entered into
evidence, as well.
[13]
Apotex
called as expert witnesses the following two persons. Merck agreed that they
could be called as experts and the parties jointly tendered in evidence their
agreement as to their expert qualifications, which I repeat as follows:
a. Mr.
Howard Rosen: A Senior Managing Director of FTI Consulting Inc.
having offices in several places around the world. He is located in Toronto, Ontario. The parties have agreed as to his qualifications as follows:
A Chartered
Accountant, Chartered Business Valuator and Certified Fraud Examiner with
expertise in investigative and forensic accounting, business valuation and loss
quantification in commercial and intellectual property disputes.
b. Ms.
Rosemary Bacovsky: President, Integra Consulting Ltd. of
Calgary, Alberta. The parties have agreed as to her qualifications as
follows:
A pharmaceutical
industry consultant and pharmacist with expertise in formulary listings, market
access, reimbursement policies and pricing regimes of the Canadian
pharmaceutical marketplace.
[14]
The
Plaintiff Apotex called the following five persons as factual witnesses:
a. Ms.
Marlie Yoshiki: Client services, Global Operations of IMS Brogan,
an organization that collects and distributes to members of the pharmaceutical
community, data; including data as to the sale of pharmaceutical products in Canada.
b. Mr.
Darren Hall: Vice President, Supply Operations of Apotex
Pharmaceuticals, a company related to the Plaintiff. He testified as to the
manufacture and capacity to manufacture alendronate tablets by his company for
Apotex.
c. Dr.
Bernard Sherman: Chairman of the Board of the Plaintiff Apotex. He
is responsible for the overall operations of Apotex and gave evidence as to
those operations, including the manufacture and sale of the alendronate product
at issue.
d. Mr.
David Kohler: Vice President, National Sales of the Plaintiff
Apotex. He gave evidence as to the sales of Apotex products in Canada, including the alendronate product at issue.
e. Mr.
Gordon Fahner: Vice President of Business Operations and Finance
of the Plaintiff Apotex. He gave evidence as to the manufacture and sales of
Apotex products, including the Apotex product at issue. He testified as to
rebates given to Apotex’s customers.
[15]
The
Defendant Merck provided evidence from two expert witnesses and seven witnesses
as to fact. Portions of the transcript and exhibits of Merck’s discovery of
Apotex were entered into evidence, as well.
[16]
Merck
called as expert witnesses the following two persons. Apotex agreed that they
could be called as experts, and the parties tendered into evidence their expert
qualifications, which I repeat below:
a. Mr.
W. Neil Palmer: President and Principal Consultant of PDCI Market
Access Inc. of Ottawa, Ontario. The parties have agreed to his qualifications
as follows:
Neil Palmer is a
pharmaceutical industry consultant with expertise in formulary listing, market
access, reimbursement policies and pricing regimes related to the Canadian
pharmaceutical marketplace.
b. Mr.
W. Ross Hamilton: A partner in the firm of Cohen Hamilton Steger of
Toronto, Ontario. The parties have agreed to his qualifications as follows:
Chartered
Accountant with a specialist designation in investigative and forensic
accounting and expertise in business valuation and damages quantification in
commercial and intellectual property disputes.
[17]
The
Defendants Merck called the following seven persons as factual witnesses:
a. Mr.
Gordon Fahner This is the Apotex executive who was a witness for
Apotex. He was recalled by Merck under subpoena.
b. Mr.
Jeff Spencer: Vice President, Women’s Health and Diversified
Brands of Merck Canada Inc. He testified as to Merck’s marketing and litigation
strategy.
c. Mr.
David Boughner Director, Strategic Initiatives of Teva Canada
Limited (formerly Novopharm). He testified as to Novopharm’s marketing
strategies.
d. Mr.
Chris Ichiyen Director, Financial Management of Cobalt
Pharmaceuticals Company. He testified as to Cobalt’s marketing strategy.
e. Mr.
Brent Fraser: Director, Drug Processing Services, Ontario Public Drug Program. He testified as to how drugs were put on to the Ontario drug formulary.
f. Ms. Kimberley Van Wart:
Consultant, Mississauga, Ontario. She was previously the President of Cobalt Canada. She testified as to Cobalt marketing and legal strategies in the 2004-2005 period.
g. Ms.
Virginia Cirocco: Consultant, Mississauga, Ontario. She was an
Executive Vice President of Shoppers Drug. She testified as to the purchasing
practices of that organization in the 2004-2005 period.
[18]
In
reply, the Plaintiff Apotex recalled:
a.
Mr.
Gordon Fahner: He testified as to the percentage of Apotex sales
to Shoppers Drug in the 2004-2005 period.
[19]
I
have found all of the expert witnesses to be credible. Where they differed,
they did so in respect of methodology and assumptions made. Where I have
preferred the evidence of one of them over the other, I have not done so on the
basis of credibility, or in any sense on the basis of superior credentials. I
will endeavour to state, in respect of certain of their conclusions or opinions
that I prefer, to say why I have done so.
[20]
With
respect to the factual witnesses, I find that all but one of them is credible.
I have comments as to that person and two others.
[21]
Two
factual witnesses who I find to be credible nonetheless cause me concern.
Ms.Yoshiki and Ms. Van Wart. Some background is necessary to explain my
concern. This matter was case managed. In May of this year I issued a direction
that Counsel were to exchange lists of witnesses including will-says for the
factual witnesses. There was to be no surprise at trial. The trial of this
matter was originally scheduled to be heard in June of this year. A few days
before the trial was to begin, Counsel for Merck notified Counsel for Apotex
that Merck was changing its position with respect to an important factual
issue; namely, the date that Merck would be alleging that a second generic,
Cobalt, entered the Canadian marketplace. After a pre-trial hearing with
Counsel, I adjourned the trial, on terms, to permit Apotex to explore the
factual basis that Merck had for the change of position and to provide new
instructions to its expert witnesses (and the same would apply to Merck). With
respect to Cobalt, Merck’s Counsel provided certain information to Apotex’s
Counsel as to the factual basis for Merck’s assertions as to the entry date of
Cobalt into the Canadian market. That basis was the evidence to be given by Mr.
Ichiyen, and certain documents were provided. Apotex conducted a discovery of
Merck a few days before this trial began in September, and Merck’s Counsel gave
assurances that this was all there was in respect of this matter.
[22]
Mr.
Ichiyen appeared as a witness for Merck at the trial before me. He was examined
and cross-examined. Suffice it to say that his evidence did not turn out as
Merck might have expected. He said that Cobalt would not enter the marketplace
as long as there was a patent around. He was Cobalt’s auditor, but not a Cobalt
executive or employee at the relevant time. I do not find anything in his
evidence that would be sufficient to support Merck’s assertion as to an early
entry date by Cobalt into the Canadian market.
[23]
As
the evidence shows, one of Merck’s Counsel, minutes after Mr. Ichiyen had given
his evidence at the trial; obtained Ms. Van Wart’s email address from Ms.
Cirocco, another of Merck’s witnesses who had not yet been called and
contacted Ms. Van Wart to set up a meeting with her. It must be made very clear
that Ms. Van Wart’s name was not on Merck’s witness list; nor was it disclosed
at any time to Apotex, whether on discovery or otherwise, before the evening
prior to the morning of trial when Ms. Van Wart gave her evidence. Apotex
strongly objected to her appearing as a witness. I allowed her to appear,
indicating that I would reserve as to admissibility of her evidence and, in any
event, review the evidence with a very large measure of salt.
[24]
As
it turned out, Ms. Van Wart’s testimony was largely directed to an attempt to
contradict Mr. Ichiyen’s evidence and to provide a picture much more favourable
to Merck. Ms. Van Wart’s evidence was based on her recollection as to what
might have happened some eight years ago assisted by discussions that she had a
few hours previous with persons not called as witnesses and a review of
documents not tendered in evidence. It became clear during cross-examination
that the Canadian Cobalt company’s decisions such as whether and when to enter
the Canadian marketplace, particularly when a patent might be involved, were
made by those higher up the corporate ladder. The Canadian Cobalt company was a
subsidiary of a European corporate structure. Ms. Van Wart had limited input
into these decisions. I will admit her evidence, but will prefer that of Mr.
Ichiyen. Ms. Van Wart’s evidence is insufficient to persuade me as to Merck’s
position that Cobalt would have entered the Canadian market in or about
November 2004, or at any time prior to the entry of Novopharm.
[25]
I
rebuked Merck’s Counsel at trial. The direction as to disclosure of witness
names and will says was ignored. A delay of several months in the date set for
the hearing of the trial was provided but seemingly did not assist in the
preparation of the case. Days before this trial began Merck’s Counsel, on
discovery, gave assurances that there would be nothing more presented at trial.
[26]
I
must add that my remarks in no way should be taken to reflect upon the
character of Ms. Van Wart. She retired from Cobalt some time ago, and has a
consulting business. She was contacted the night before she appeared. Her
memory was refreshed by speaking to persons who did not appear as witnesses,
and in reviewing documents not produced at trial. A contact was arranged
through Ms. Cirocco, but nonetheless came out of the blue as far as Ms. Van
Wart was concerned. She seemed to be perplexed and uncertain as well she might
be, as to what was going on.
[27]
I
also have concerns about the evidence of Ms Yoshiki. Her name was not on
Apotex’s witness list, nor was a will-say provided. In this case however Merck
did not object to her being called as a witness. She did not contradict the
evidence of another witness. She provided information as to data was collected
by an organization known as IMS Brogan, in particular Canadian Drug Store
Hospital Audit known as CDH. The accounting experts for each of the parties
referred to this data. Unlike Ms. Van Wart her evidence was not an endeavour to
impeach a party’s own witness. I accept her evidence and find it credible.
[28]
The
third factual witness, about whom I have concerns, is Ms. Cirocco. She
graduated from university as a pharmacist. She joined Shoppers Drug Mart in 1995
and retired from a position as Senior Vice President of Pharmacy and Corporate
Affairs in 2009 to do what she described as volunteer community work and
consulting. Although she was apparently subpoenaed, she was in fact retained by
Merck’s solicitors as a consultant. For instance, she was the person who
quickly obtained Ms. Van Wart’s email address.
[29]
Ms.
Cirocco testified principally as to the rebate programme instituted by Shoppers
Drug Mart, whereby Shoppers would more or less insist wherever possible that
generic drug suppliers such as Apotex provide by way of a rebate, a percentage
of the money paid by Shoppers to purchase drugs from the drug supplier. Her
evidence in this regard went well beyond her will say as provided by
Merck’s Counsel to Apotex’s Counsel, particularly in a critical area as to the
size of the rebate. Her evidence in this regard was unsupported by any document
or other evidence.
[30]
The
evidence shows that Apotex’s Counsel, when her name was disclosed to them by
Merck’s Counsel in June, attempted to contact Ms. Cirocco with a view to
discussing her possible evidence in the case. This is quite proper; there is no
property in a witness. Ms. Cirocco played a game of cat and mouse, through
emails, with Apotex’s Counsel. She insisted that they disclose a list of
questions they might ask. They did so, by email. She did not communicate with
them any further and never met with them. That is her prerogative; however, it
indicates a lack of candour and a willingness to play games.
[31]
Further,
it appears that Ms. Cirocco was disciplined for professional misconduct in 2004
by the Ontario College of Pharmacists. She frankly admitted to this when asked
in cross-examination. Merck’s Counsel went through an extremely lengthy
examination in chief as to Ms. Cirocco’s background and activities in the
pharmaceutical field, and never touched on this aspect. He did so in reply but
only because the matter had been raised in cross-examination.
[32]
It
appears that, according to Ms. Cirocco, Shoppers was accepting rebates as high
as sixty percent (60%) in about the relevant period. The Ontario government had
passed legislation in 2006/7 intended to curb rebates at twenty percent (20%).
It appears from Ms. Cirocco’s evidence that her company had what she described
as “private business” in “various places” that apparently continued to receive
those larger rebates.
[33]
In
all, I am quite sceptical as to Ms. Cirocco’s evidence. It deals with the
rather murky business of rebates. She provided no candid illumination in this
area. She offered that Shoppers was getting rebates of up to sixty percent
(60%) This statement, if true, is important. It was not disclosed by Merck in
a pre-trial will say or otherwise. It is unsupported by any other evidence.
This number was never put by Merck’s Counsel in cross-examination of any Apotex
witness, including Mr. Fahner, who appeared again as a witness in reply after
Ms. Cirroco had given her evidence.
[34]
I
will not accept Ms. Cirocco’s evidence on any point unless it is clearly
supported by other credible evidence.
THE
“BUT FOR” WORLD, WHO BEARS THE BURDEN
[35]
The
Court is required to consider what would likely have been the case had Apotex
not been prevented from entering the Canadian marketplace with its generic 70
mg Apo-alendronate tablets. It was prevented from doing so because Merck had
instituted and prosecuted through to a judgment unfavourable to it, proceedings
under the NOC Regulations. Therefore, the Court is to determine, as best
it can, a hypothetical question: What would have been the case “but for” those
proceedings?
[36]
In
entering the “but for” world, the Court is to be mindful as to who bears what
burden. Both parties have cited and relied on what I wrote at paragraph 35 of
my decision in Apotex Inc v AstraZeneca Canada Inc, 2012 FC 559;
therefore, I repeat it:
35 In brief, it may be said that the party who
has led sufficient evidence to put an issue "in play", must, to
succeed on that issue, put in sufficient evidence so that on the balance of probabilities,
the relevant facts are accepted by the Court as having been proved. Thus Apotex
must put in play and subseqtently prove on the balance of probabilities the
facts that it needs to establish its case for compensation. AstraZeneca must
put in play and subsequently prove those facts that it asserts disqualifies
Apotex or reduces or negates Apotex's claim for compensation.
[37]
Also,
both parties have cited and relied upon the decision of the Supreme Court of
Canada in Athey v Leonati, [1996] 3 S.C.R. 458, at paragraphs 26 and 27,
which I repeat:
26 The respondents argued that the trial judge's
assessment of probabilities in causation was similar to the assessment of
probabilities routinely undertaken by courts in adjusting damages to reflect
contingencies. This argument overlooks the fundamental distinction between the
way in which courts deal with alleged past events and the way in which courts
deal with potential future or hypothetical events.
27 Hypothetical events (such as how the
plaintiff's life would have proceeded without the tortious injury) or future
events need not be proven on a balance of probabilities. Instead, they are
simply given weight according to their relative likelihood: Mallett v.
McMonagle, [1970] A.C. 166 (H.L.); Malec v. J. C. Hutton Proprietary Ltd.
(1990), 169 C.L.R. 638 (Aust. H.C.); Janiak v. Ippolito, [1985] 1 S.C.R. 146.
For example, if there is a 30 percent chance that the plaintiff's injuries will
worsen, then the damage award may be increased by 30 percent of the anticipated
extra damages to reflect that risk. A future or hypothetical possibility will
be taken into consideration as long as it is a real and substantial possibility
and not mere speculation: Schrump v. Koot (1977), 18 O.R. (2d) 337 (C.A.); Graham v. Rourke (1990), 74 D.L.R. (4th) 1 (Ont. C.A.).
[38]
I
emphasize the last sentence of that decision; the hypothetical possibility must
be real and substantial not mere speculation. Put another way, the possibility
must be realistic and not simply hopeful.
WHAT IS THE
RELEVANT PERIOD
[39]
This
period has already been determined by this Court and affirmed by the Federal
Court of Appeal. It is from February 3, 2004 to May 26, 2005. The parties have
agreed that the accountants should pro-rate the compensation over precisely
those dates.
OVERALL
SIZE OF THE ALENDRONATE MARKET
[40]
The
parties are agreed that the size of the total market for 70 mg alendronate
tablets during the relevant period is to be the quantity as sold by Merck, the
only authorized person in the real world who sold that product in that period.
[41]
I
should add that others, including Apotex, Novopharm and Cobalt, were selling
alendronate tablets in other strengths, 5 mg and 10 mg tablets, during at least
a portion of that period. To some extent, the experts have used sales of these
tablets as models or proxies for their opinions. The difference between these
tablets and the 70 mg tablets appears to be that the 70mg tablets are intended
for “once a week” administration.
GENERIC
SHARE OF THE OVERALL ALENDRONATE MARKET
[42]
The
parties have agreed that the share of the alendronate market that would have
been occupied by the generics in the period in question; that is, the share in
the “but for” world, is the same as the share occupied by the generics in the
subsequent “real world” period.
APOTEX’S SHARE
OF THE GENERIC MARKET
[43]
To
answer this question, two matters must be addressed. First, when would Apotex
have entered the market in the “but for” world. Second, when would one or other
of the two generics, Cobalt and Novopharm, have entered that market in the
relevant period, if at all.
[44]
The
question as to when a generic would have entered the marketplace must be
answered in several parts. First one has to establish when the generic would
have received its Notice of Compliance (NOC). Another part is whether the
generic had the capacity to manufacture or acquire the product in the relevant
time. Another part is whether the generic was motivated or dissuaded from
entering the marketplace during the relevant period. The final part is when, if
at all, the product would have been accepted by the relevant branch of the
provincial or territorial governments for listing in a formulary; which listing
would permit the product to be sold in that province in significant quantities.
1. Capacity
[45]
I
find on the evidence, particularly of Mr. Hall, that Apotex had the ability to
manufacture 70 mg alendronate tablets in a quantity sufficient to fill the
market in the relevant time period. This is supported by the fact that as soon
as Apotex did receive its NOC in the “real world”, sufficient quantities
appeared on the market very quickly. This matter was not seriously contested by
Merck.
[46]
I
find in considering the evidence of Mr. Ichiyen and Ms. Van Wart, that I do not
have enough evidence to persuade me that Cobalt had sufficient resources
available to it in the “but for’ period to make or obtain the product. Neither
of them had first-hand knowledge that would support such a conclusion.
[47]
As
to Novopharm, I find on the evidence of Mr. Boughner that he did have first-hand
knowledge of the relevant facts. He testified that Novopharm had the ability to
acquire from a related company abroad, sufficient quantities of alendronate
product to supply the market in the relevant time period.
2. Motivation
[48]
I
find that both Apotex and Novopharm would have entered the market during the
“but for” time period had each of them received an NOC. Both Dr. Sherman and
Mr. Boughner testified as to this. No serious challenge was raised in respect
of this testimony.
[49]
The
matter is different with respect to Cobalt. Mr. Ichiyen testified that Cobalt
would not have launched a product while a patent was in place. Ms. Van Wart’s
testimony related only to a situation where no patent was in place. I find
that, in the relevant period, since Merck still had a patent in place, Cobalt
would not likely have been motivated to launch a product.
3. Formulary
Listing
[50]
It
is common ground that a pharmaceutical product such as tablets containing an
active ingredient such as alendronate cannot be sold commercially in Canada until the distributor has received from the federal Minister of Health a Notice of
Compliance (NOC). It is also common ground that, even though a distributor has
received an NOC, the product generally cannot be sold in any reasonable
commercial quantities in any province of Canada until it has been listed on
what is called a formulary, by the relevant provincial Ministry. Thus, when
considering when a product could have been sold in Canada, an important date is
the date that the product would have been listed on the relevant provincial
formulary.
[51]
It
is common ground that, in general, the first generic version of a drug listed
on a provincial formulary during the period in question here, 2004 and 2005,
would have been sold at a price established at seventy percent (70%) of the
price established for the previously listed branded product. In argument
Apotex’s Counsel urged that the price would have been greater. I will address
this matter later. It is further agreed that when one or more generics
subsequently enter the marketplace, the price of all generics will drop to
sixty-three percent (63%) of the brand listed price. Therefore, it is important
in this case to determine the period for which Apotex’s 70 mg alendronate product
would have been the exclusive generic, and the period for which it was no
longer the exclusive generic.
[52]
In
discussing price in this context, I am not considering the issue of rebates
which I will discuss elsewhere.
[53]
Each
of the parties provided expert evidence as to the dates, in the relevant
period, when Apotex would, in their opinion, have been listed on the provincial
formularies and when the products of competitor generics, Novopharm and Cobalt,
would have been so listed.
[54]
These
experts, Ms. Bacovsky for Apotex, and Mr. Palmer for Merck; are agreed as to
twenty-three of those dates, and disagree as to seven. I set out Table 1 of Mr.
Palmer’s Supplementary Report of September 10, 2012 at paragraph 33, which
lists all of the dates and highlights those in disagreement.
[55]
Ms.
Bacovsky set out the dates which were in disagreement at Table 1 of her
Responding Expert Report dated September 16, 2012, paragraph 3, as follows:
[56]
The
accounting experts, Mr. Rosen for Apotex, and Mr. Hamilton for Merck, have used
these listing dates in their calculations. Thus, it is necessary to resolve the
disagreements.
[57]
Fortunately,
the parties have agreed that while several of these dates are in disagreement,
the disagreement makes no material difference to the final calculation of a
quantum. Further, the parties have agreed that “but for” sales in Canada’s territories may be added in to the quantum.
[58]
In
the result, the “but for’ entry date for Apotex’s product remains in dispute in
respect of two provinces only; Ontario and Saskatchewan.
a. Ontario
[59]
Ms.
Bacovsky’s opinion is that Apotex’s product would have been listed on the Ontario formulary on April 6, 2004. Mr. Palmer’s opinion is that it would be listed on July
20, 2004. Much of the bases for the differences in these opinions lies in their
respective views as to the Ontario “fast track” programme in place at about the
relevant period and whether the Apotex product, had it received its NOC in
early February 2004, would have been placed on that fast track.
[60]
Merck
called the evidence of Mr. Fraser, who was a senior official with the relevant Ontario ministry at the time. I accept his evidence as credible and authoritative as to
what transpired in the Ontario Drug Benefit Program (ODB), the relevant
department at the time.
[61]
Mr.
Fraser stated that, in general, the ODB had a continuous programme for the
review of drugs sought to be listed on the formulary. Those that had received
an NOC as approved generic equivalents of drugs already approved on the
formulary received faster treatment. Once approved by ODB, the matter was
passed up for approval by cabinet. Delays could occur if cabinet was not
meeting within the next while or if the matter could not be reached on the
cabinet agenda. His department established internal cut-off dates, not
generally known to the public, as to when material respecting various drugs
would be bundled together to be forwarded for cabinet approval. In the period
in question a cut-off date of December 31, 2003 was established so that any new
drugs submitted for approval as of that date would be bundled and forwarded for
cabinet approval in April 2004. He testified that any submission received after
December 31, 2003, such as February 2004, would not have been eligible for
inclusion in the April 2004 bundle previously sent to cabinet.
[62]
Ms.
Bacovsky’s opinion leading to an approval date of April 6, 2004 was based on
her reading of a recital of evidence given in Reasons for Judgment in a
decision given by Justice O’Driscoll of the Ontario Superior Court of Justice
in Apotex Inc v Minister of Health, Court File 157/04, et al, April 27,
2004, involving the drug citalopram. In that case, a submission for listing on
the formulary made by another generic in December 2003 was included in the
April 2004 bundle, but Apotex’s submission made in January 2004 was not. This
is consistent with Mr. Fraser’s evidence that a submission filed after the end
of December 2003, namely in February 2004, would not have been included in the
bundle sent to cabinet for approval in April. It would have been put in a later
bundle.
[63]
When
asked in cross-examination whether Mr. Fraser’s evidence (which had not yet
been given) that December 31, 2003 was a hard cut-off date would have changed
her opinion, Ms. Backovsky paused and said only that Mr. Fraser was not senior
enough in the decision making process. I find that he was senior enough and
that his factual evidence is to be preferred to Ms. Bacovsky’s opinion
evidence.
[64]
Mr.
Palmer’s opinion is based on the assumption, borne out by Mr. Fraser’s
evidence, was that July 20, 2004 was the more likely date for listing of the
Apotex product on the Ontario formulary. I agree with that opinion and so find
that the relevant date for the listing of the Apotex 70 mg. tablets on the Ontario formulary in the but-for world is July 20, 2004.
b. Saskatchewan
[65]
It
is Ms. Bacovsky’s opinion that Apotex’s product would have been listed on the Saskatchewan formulary on March 1, 2004. Mr. Palmer’s opinion if that the listing would
have taken place April 1, 2004. Apparently, there is no middle ground; it is
one date or the other.
[66]
Ms.
Bacovsky used ciprofloxacin as the criterion for the speed of listing a product
in Saskatchewan. Here, her opinion was that listing could be achieved in less
than a month.
[67]
Mr.
Palmer’s opinion was that a drug submitted for listing in February 2004 would
more likely be processed and listed in the month of April, not March. He stated
that ciprofloxacin was a special case where listings were expedited because of
a perceived fear of an anthrax outbreak. The time period for listing, in his
opinion, is consistent with listings of other drugs such as ramapril.
[68]
I
accept Mr. Palmer’s approach. It is more consistent with a realistic estimate
as to a listing date than with the more hopeful approach of Ms. Bacovsky.
[69]
The
listing date for the Apotex product in Saskatchewan in the but for world would
have been April 1, 2004.
FORMULARY
LISTINGS FOR THE NOVOPHARM AND COBALT ALENDRONATE PRODUCTS
[70]
I
have already found that the evidence is insufficient to support Merck’s
assertion that Cobalt would have entered the marketplace in the relevant
period. The evidence does not establish that Cobalt could make or obtain the
product in that period or that it would have been motivated to release the
product in that period. In any event, the only province for which the experts
were apart as to listing dates for the Cobalt product is British Columbia, and
it is agreed that for purposes of calculations, the difference is not relevant.
[71]
As
to Novopharm, there is a minor difference between the experts as to the listing
dates in British Columbia, but that, as previously discussed, is irrelevant.
[72]
There
is also a difference between the experts as to Novopharm’s listing date on the Ontario formulary in the “but for” world. In this case, Mr. Palmer’s date, February 24,
2005, is more favourable to Apotex than Ms. Bacovsky’s date of January 25,
2005.
[73]
In
argument, Merck accepted Mr. Palmer’s date and I so find that the Novopharm
listing date in the “but for” world in the Ontario formulary would have been
February 24, 2005.
AT
WHAT PRICE WOULD APOTEX HAVE SOLD ITS PRODUCT
[74]
There
are two scenarios to consider when endeavouring to establish the price that
Apotex would have sold its 70 mg alendronate tablets in the “but for” world. They
are the period when it was the only generic, and the period when another
generic would have entered the market. In this case, that other generic would
have been Novopharm. As I have found, there is insufficient evidence to
establish that Cobalt would have entered the market at any time within in the
relevant time period.
[75]
Apotex’s
expert, Ms. Bacovsky, stated that the price would generally be set at 70% of
the brand (Merck) when a generic such as Apotex was the sole generic in the
marketplace, and 63% of the brand when other generics entered a particular
provincial formulary. Apotex’s expert, Mr. Rosen, accepted those figures to be
consistent with his understanding of the real world, and provided his opinions
based on those percentages.
[76]
Merck’s
expert, Mr. Palmer, accepted those figures, as well. Merck’s expert, Mr.
Hamilton, provided various scenarios where those figures were used.
[77]
It
seems that it has been comfortably established that the 70% figure for exclusivity,
and 63% for shared market, would be the basis for establishing a price.
[78]
In
closing argument, Apotex’s Counsel scoured through various pieces of testimony
and argued that there was, to use their words, a “realistic chance” that Apotex
would have sought and secured a price greater than the 70% level during its
period of exclusivity.
[79]
While,
undoubtedly, Apotex would have, in negotiating with its customers, sought as
high a price as it dared; there may have been a chance that it could have
obtained a price just below that of the brand; say, 95%. However, I am not
persuaded that this is the most realistic expectation in the “but for” world.
[80]
I
find that the most realistic price that Apotex would obtain for its product in
the “but for” world is 70% of the brand price during exclusivity, and 63% of that
price when it was not exclusive.
DOUBLE RAMP-UP
[81]
When
an organization introduces a new drug product into the marketplace, there is an
initial period during which the product has to be made or acquired, orders
received from customers, and the product is to be shipped to customers. This is
referred to in evidence as “ramp-up”. In the real world, when Apotex did
release its 70 mg alendronate tablets, it did incur a “ramp-up” before it
reached a more or less steady state as to sales levels. The accounting experts
differ as to what this “ramp-up” loss - that is, the lower level of sales
before reaching a steady state - was in the real world. Mr. Hamilton’s opinion
is that Apotex suffered minimal losses due to ramp-up in the real world. Mr.
Rosen’s opinion is that they were larger.
[82]
Both
Mr. Hamilton and Mr. Rosen agree that in the “but for” world, Apotex would also
have incurred a ramp-up in the period when its product was introduced. Further,
and very importantly, they agree that, were it not for the view taken by the
Federal Court of Appeal in its earlier decision in this case, 2008 FCA 189 at
paragraphs 97 to 102, it would be proper accounting practice to avoid a “double
ramp-up”. In other words, the loss encountered in the “real world” ramp-up
should be added to the compensation for loss in the “but for” world.
[83]
The
jurisprudence on this issue bears repeating. When the argument was first raised
before me in the earlier trial of this action, it was done so not in the
context of ramp-up, but in the context of permanent loss of market share. For
instance, if Apotex had entered the market in the “but for” period, it may have
achieved, say, 60% of the market, but since it was delayed, it only achieved
50% in the “real world”; thus it suffered a continuing loss of 10% market share
in the period after the “but for” period. I wrote at paragraphs 117 to 121 in
2008 FC 1185:
FUTURE LOSSES
117 Merck characterizes a claim made by Apotex
in respect of certain damages as a claim for "future losses". While
perhaps not entirely accurate as catchwords, it is convenient to refer to that
claim as such.
118 Apotex's claim is set out in paragraph 1.
(a)(ii) of its Further Amended Statement of Claim as follows:
1. The Plaintiff, Apotex Inc. ("Apotex"),
claims:
(a) damages suffered by Apotex in respect of the
drug alendronate by reason of the commencement of a proceeding by the
Defendants pursuant to the Patented Medicines (Notice of Compliance)
Regulations (the "Patent Regulations"), in respect of:
...
(ii) lost sales and permanent market share due to
the fact that launch by Apotex of its alendronate product was unjustly delayed
with the result that two other generic manufacturers, Novopharm Limited
("Novopharm") and Cobalt Pharmaceuticals Inc. ("Cobalt"),
launched their alendronate products essentially simultaneously, thus denying
Apotex the opportunity to establish as permanent market share advantage in
advance of any generic competitor.
119 Excerpts from the discovery of Apotex were
put in evidence at trial (Exhibit 4) in which there was the following exchange
between counsel (Tab 1, pages 21 & 22), Markwell for Merck and Crowfoot for
Apotex:
Mr. Markwell: Sorry, to clarify your last statement.
The damages that flow from those losses at law, what do you mean by that?
Mr. Crowfoot: Well, the damages that flow from that
period because they were kept off the market during that period. The damages
may incorporate things like lost market share which is a present value
calculation.
Mr. Markwell: So it's not correct, then that your
loss is restricted to the 16-month period, that it could be for the longer
period of time?
Mr. Crowfoot: No, the losses in respect of the
16-month period being off the market. The calculation of that loss may involve
the present value calculation of a lesser market share than Apotex otherwise
would have had.
Mr. Markwell: During those 16 months or beyond those
16 months?
Mr. Crowfoot: The loss of market share occurs once
they enter the market, and they only have an X percent market share instead of
a Y percent market share. That loss is incurred as of the date that they
entered the market because they cannot acquire the market share they should
have. So the losses still occurred within the period, but calculating it may
involve looking forward.
Mr. Markwell: So what would be the time frame for
those future losses?
Mr. Crowfoot: The loss of market share would be
perpetual, but it's the present value calculation that are the further out you
get, the less financial impact it has. It's all a matter of expert evidence. I
don't know how long it would be.
Mr. Markwell: So it's Apotex's position that there
may, in fact, be a perpetual loss that would be calculated as of the date of
the Notice of Compliance taking into account factors that will be subject of
expert evidence?
Mr. Crowfoot: Yes.
120 As I understand Apotex's claim, it is saying
that during the period from February 3, 2004 to May 26, 2005, the marketplace
for this particular product became distorted because two other generics entered
the marketplace in that period. Apotex claims that, were it not for Merck's NOC
application against Apotex, Apotex could have been first in the marketplace or
at least entered the marketplace at about the same time that the other generics
did and that Apotex's market share would, thereby, have been larger that it now
is. Apotex argues that such lesser market share is a matter that permanently
endures and is a matter of permanent loss. The loss, says Apotex, may be
quantified by experts at the later trial.
121 I analogize the situation to one of an
injury that a person may have suffered by the tortious activity of another
person. For instance, a person may be injured in the leg so that, for the rest
of that person's life, that person suffers a leg disability. The leg may heal,
the person perhaps ought to have sought, but did not, medical attention or
remedial therapy. These are matters of quantification and not a matter of
injury itself.
[84]
The
Court of Appeal in 2009 FCA 187 reversed me on this point, writing at
paragraphs 97 to 102:
97 No one takes issue with the Federal Court
Judge's characterization of the claim made by Apotex in its Further Amended
Statement of Claim. The issue is therefore whether the claim as construed by
the Federal Court Judge comes within the words of subsection 8(1). This again
gives rise to a pure question of statutory interpretation which stands to be
reviewed on a standard of correctness.
98 As has already been noted, section 8 in its
original form was somewhat obscure (see para. 45 above). The RIAS which
accompanied the 1998 amendment to section 8 indicates that the change was
brought in order to provide a clearer indication as to the circumstances in
which damages can be awarded. In this respect, the amended version of section 8
makes it clear that:
[T]he first person "is liable to the second
person for any loss suffered during the period
(a) beginning on the date, as certified by the
Minister, on which a notice of compliance would have been issued in the absence
of these Regulations, unless the Court is satisfied on the evidence that
another date is more appropriate; and
(b) ending on the date of the withdrawal, the
discontinuance, the dismissal or the reversal.
[...] la première personne est responsable envers la
seconde personne de toute perte subie au cours de la période :
a) débutant à la date, attestée par le ministre, à
laquelle un avis de conformité aurait été délivré en l'absence du présent règlement,
sauf si le tribunal estime d'après la preuve qu'une autre date est plus
appropriée;
b) se terminant à la date du retrait, du désistement
ou du rejet de la demande ou de l'annulation de l'ordonnance.
[My emphasis]
99 According to the analysis of the Federal
Court Judge, the losses claimed by Apotex were caused during the period since
that is when Apotex was prevented from occupying the market and obtaining the
market share which, based on its claim, it would otherwise have had. No one
takes issue with this reasoning. The question is whether the decrease in sales
which occurs in future years as a result of this decreased market share comes
within section 8. The Federal Court Judge, by allowing the claim for losses
"beyond May 26, 2005" to proceed, answered this question in the
affirmative.
100 When regard is had to the broad grant of
authority conferred by subsection 55.2(4) of the Patent Act, it seems clear
that the measure of the compensation which can be awarded under the PM(NOC)
Regulations is a matter within the discretion of the Governor-in-Council. It is
also clear that in keeping with the purpose of the PM(NOC) Regulations and the
balance which the Patent Act seeks to achieve, a range of compensation was open
to the Governor-in-Council in the exercise of this discretion.
101 In this case, we have the advantage of
knowing that in 1998 the Governor-in-Council focused on this very issue, and
chose to limit the measure of the losses which can be compensated by way of
damages to those suffered during the period. No issue of principle flows from
this. The Governor-in-Council could have extended the measure of the losses to
include those caused during the period, regardless of when they are suffered.
However, it did not do that.
102 The Governor-in-Council's clearly expressed
intent must be given effect to. This excludes compensation for losses occurring
in future years since such losses cannot be said to have been suffered during
the period. It follows, for instance, that Apotex's entitlement to damages for
lost sales resulting from the alleged decrease in its market share must be
confined to sales that can be shown to have been lost within the period. In
order to be compensated, the losses must be shown to have been incurred during
the period. I therefore conclude that the appeal should be allowed on this
limited point.
[85]
It
is to be noted that in paragraph 101, the Court of Appeal rests its findings on
the use of the word “suffered” in section 8 of the NOC Regulations, and
contrasts “suffered” with “caused”. Yet, in paragraph 102, that Court uses
neither word; it uses the word “incurred”. Justice Snider in her decision
released in May of this year, Apotex Inc v Salofi-Aventis, 2012 FC 553,
supra, declined to award compensation for double ramp-up, based on her view of
the Federal Court of Appeal decision, supra. She wrote at paragraphs 265 to
270:
265 Apotex claims that it should be entitled to
recover an amount that it refers to as a second "ramp-up" or
"ramp-up damages". Sanofi submits that Apotex is not entitled to any
such recovery.
266 In general terms, as I understand it, the
term "ramp-up" refers to the period of time that it takes a drug
manufacturer after initial approval of its drug to reach its final level of
sales. It takes some time to negotiate agreements with pharmacies and
distributors, to get formulary listings and to physically get product to drug
stores. In the hypothetical world, Apotex would have experienced a ramp-up
period for which it does not seek compensation. However, Apotex does seek
compensation in respect of its "real world" or "duplicate"
ramp-up which it argues was only incurred because of Sanofi's actions.
267 Mr. Rostant described this "ramp
up" during the "Subsequent Loss Period" (i.e. after December 12,
2006) as follows (Exhibit 26 at 33):
When Apotex launched Apo-Ramipril in December 2006,
there was a "ramp up" period before it earned profits on a fully
functional basis ("Ramp Up Period"). After receiving its NOC, Apotex
commenced the marketing and sale of Apo-Ramipril, including obtaining formulary
listings. Had Apotex commenced sale of Apo-Ramipril at the start of the Initial
Loss Period, it would have only experienced the "ramp up" at that
earlier date, such that, in the period in December 2006 and following, it would
have made its sales on a fully functional basis.
... [t]he lost profit associated with the ramp up
period in the Subsequent Loss Period is the difference between what Apotex
would have sold had it ramped up in the Initial Loss Period and what it sold in
the Subsequent Loss Period when it ramped up.
268 According to the calculations of Mr.
Rostant, the lost profits suffered by Apotex during the subsequent ramp-up were
$9,205,121. Mr. Hamilton calculated this amount as $7,211,327 (Exhibit 119,
Schedule 9).
269 Although the value of the second or
duplicate ramp-up period is obviously a loss to Apotex, it is a loss occurring
after the Relevant Period. The scope of a claim under s. 8 of the PM (NOC)
Regulations was addressed by the Court of Appeal in Alendronate (FCA), above. In
that case, Apotex had pleaded that, under s. 8 of the Regulations, it was
entitled to damages in respect of "lost sales and permanent market
share" (see Alendronate (FC), above at para 118). Most relevant to the
question before me, the Court of Appeal held that s. 8 does not include damages
for "future losses", such as decreased market share due to delayed
entry into the generic market. It is worthwhile repeating the determinative
portion of the decision, at paragraphs 99 to 102:
[99] According to the analysis of the Federal Court
Judge, the losses claimed by Apotex were caused during the period since that is
when Apotex was prevented from occupying the market and obtaining the market
share which, based on its claim, it would otherwise have had. No one takes
issue with this reasoning. The question is whether the decrease in sales which
occurs in future years as a result of this decreased market share comes within
section 8. The Federal Court Judge, by allowing the claim for losses beyond
"May 26, 2005" to proceed, answered this question in the affirmative.
[100] When regard is had to the broad grant of
authority conferred by subsection 55.2(4) of the Patent Act, it seems clear
that the measure of the compensation which can be awarded under the PM(NOC)
Regulations is a matter within the discretion of the Governor-in-Council. It is
also clear that in keeping with the purpose of the PM(NOC) Regulations and the
balance which the Patent Act seeks to achieve, a range of compensation was open
to the Governor-in-Council in the exercise of this discretion.
[101] In this case, we have the advantage of knowing
that in 1998 the Governor-in-Council focused on this very issue, and chose to
limit the measure of the losses which can be compensated by way of damages to
those suffered during the period. No issue of principle flows from this. The
Governor-in-Council could have extended the measure of the losses to include
those caused during the period, regardless of when they are suffered. However,
it did not do that.
[102] The Governor-in-Council's clearly expressed
intent must be given effect to. This excludes compensation for losses occurring
in future years since such losses cannot be said to have been suffered during
the period. It follows, for instance, that Apotex's entitlement to damages for
lost sales resulting from the alleged decrease in its market share must be
confined to sales that can be shown to have been lost within the period. In
order to be compensated, the losses must be shown to have been incurred during
the period. I therefore conclude that the appeal should be allowed on this
limited point.
[Emphasis in original]
270 Apotex argues that the decision of the Court
of Appeal in Alendronate (FCA) did not extend to a claim for subsequent
ramp-up. I do not agree. The holding of the Court of Appeal is directly
applicable to this type of loss. Apotex is claiming for a loss that may have
been caused during the Relevant Period but that was not incurred during that
time. The claimed loss - however named - falls squarely within the exceptions
set out in Alendronate (FCA) and, unfortunately, is not recoverable.
[86]
I
am not satisfied, particularly given the common view of the accounting experts
that, normally, compensation would be made to prevent a double ramp-up loss,
that the Court of Appeal had this situation in mind.
[87]
However,
in the interests of comity and in the expectation of an inevitable appeal
regardless how I might decide, I will adopt the view of Justice Snider. I will
not allow compensation for double ramp-up.
DEDUCTIONS
a. Agreed
Deductions
[88]
It
is understood that certain deductions must be made from the price that Apotex
otherwise would have received for the quantities of product it would have sold
in the “but for” world. The parties have agreed to some of them, in particular:
§ Prompt payment
discount
§ Sales returns
§ Cost of sales
§ Sales
Commissions
§ Freight and
distribution
[89]
The
parties have arrived at the basis for accounting for these factors, and they
require no further discussion in these Reasons.
[90]
The
parties have not agreed as to two categories of deductions:
§ Rebates
§ Free goods
[91]
I
will, therefore, discuss these matters.
b. Rebates
[92]
Rebates,
sometimes referred to as trade allowances or incentives, are amounts that are
paid by the seller, such as a generic drug company, to its purchaser; generally
after the goods have been invoiced by the seller to the purchaser. The
purchaser would send an invoice to the seller, generally based on a percentage
of the price of the goods sold. The purchaser would receive a cheque in the
amount invoiced.
[93]
While
various explanations may be given for this practice, one must be blunt. It is a
kick back. The Ontario government, for one, endeavoured in 2006 and later, to
regulate this practice and limit the amount to twenty percent (20%).
[94]
The
practice seems to be a murky one. There seems to be no established figure for
the rebates; nor does one particular rebate necessarily, but not inevitably,
apply to one particular product and another to another. The rebates seem to be
applied collectively to a range of products and vary over time. Much seems to
depend on the negotiating strength of the supplier, such as Apotex, and the
purchaser, such as a pharmacy chain or purchasing group. Product exclusivity
gives the supplier a stronger hand; non-exclusivity gives the purchaser a
stronger hand. Even if there is exclusivity, a supplier may give a rebate in
order to build goodwill or in expectation of favourable treatment in other
areas. A purchaser who does not get a favourable rebate may seek to exact
retribution elsewhere, or later. There is no science or exactitude that can be
applied.
[95]
In
the present situation, several proxies were established. For instance, what
were the rebates offered for the 5 mg and 10 mg alendronate tablets? What were
the “real world” rebates once Apotex entered the market with its 70 mg tablets?
What rebates were given for other drugs, both exclusive and non-exclusive in
the “but for” period? In argument, the parties urged that rebates ranging from
almost zero (Apotex) to sixty percent (60%) (Merck) were applicable. Here and
there in the evidence one can find support for using rebates of five percent
(5%) or forty percent (40%) and many other figures.
[96]
There
is no one correct figure. Undoubtedly, Apotex, in its period of exclusivity,
would like to have given little or no rebate. However, other factors, such as
customer goodwill or fear of retribution elsewhere, may have resulted in a
rebate being given.
[97]
Having
considered all the evidence, I am satisfied that the most reasonable conclusion
as to the level of rebate that Apotex would have given in its period of
exclusivity is that level arrived at by Mr. Rosen in Schedule 16 of his Report
of August 7, 2012. That figure is ______
It is arrived at using several other drugs as proxies. I appreciate that there
may have been other drugs as well that could have been used as proxies, but
those selected by him are reasonable.
[98]
Mr.
Hamilton uses Mr. Rosen’s figure in some of his calculations, as well. He also
uses 40% and 60%, but clearly stated in cross-examination that he did so only
because he was instructed by Merck’s Counsel to do so. He had no independent
basis for selecting these figures.
[99]
Turning
to the period when Apotex was no longer the exclusive generic, the evidence shows
that in the “real world”, Apotex gave rebates of _________________
including free goods. Mr. Rosen’s Schedule 16, aforesaid, using proxy drugs,
estimated the rebate during the non-exclusive period at _____________________
[100] Thus,
I am faced with a choice; “real world” at _____________________or
proxy drugs in the “but for” world at _______________________________
In the exclusive period, I did choose Mr. Rosen’s proxy model. It would seem
that, in order to be consistent, I should do so again. I will not. I will
choose the “real world” figure as being better established as being the most
appropriate. Mr. Rosen’s figure for the exclusivity period was the best
evidence I had for that period. The “real world” figure for the non-exclusive
period is the best evidence I have for that period.
[101] Thus,
I conclude that the allowance for rebates in the period of Apotex exclusivity
should be set at ____________________ of
the selling price and at __________________
of the selling price in the non-exclusive period.
c. Free
Goods
[102]
Mr.
Rosen and Mr. Hamilton disagreed as to what, if any, deduction should be made
for the provision of free goods. The figures of ______and
______ as stated above, include a
provision for free goods.
[103] The
difference between these experts boils down to whether the data as provided by
Ms. Yoshiki’s organization (IMS CDH) did or did not include free goods. Her
evidence was that it did not include free goods. For that reason, Mr. Rosen’s
approach is the correct one.
[104] The
percentages set out previously, ______
and ____take into account free goods. No
further deduction will be taken for free goods.
INTEREST
[105] Apotex
claims interest on the sums of money found to be payable to it by Merck in this
action. Apotex’s accounting expert, Mr. Rosen, calculated interest based on a
simple interest rate of 2.8%. Merck’s accounting expert, Mr. Hamilton,
calculated interest based on the average annual Bank of Canada short-term
lending rate.
[106] I was
advised by Counsel that the parties had agreed as to the manner in which
pre-trial interest is to be calculated. Exhibit P-65 sets out that manner.
Pre-trial interest is to be calculated according to what is set out there. That
interest shall run to the date of these Reasons
CONCLUSION
AND COSTS
[107]
I
have endeavoured to set out in these Reasons those matters that have been
agreed upon by the parties, and to resolve those matters that have remained at
issue. The accounting experts for the parties are to collaborate and provide a
final figure as to compensation, together with a brief report setting out the
calculations made to support the result. While I trust that no matter has been
overlooked in these Reasons, and that no matter will still be the subject of
disagreement, I may be spoken to as soon as possible if that is not the case. I
expect to receive the final figure and report as to calculations within fifteen
(15) days.
[108] The
parties have asked that I reserve as to the matter of costs. They should keep
in mind my earlier Order adjourning the trial date, which addressed some aspects
as to costs. There may be other Orders, as well, which made certain
dispositions as to costs. The parties are to make brief (5 pages or less)
submissions as to costs within ten (10) days following the submission of the
report of the accounting experts aforesaid.
JUDGMENT
FOR
THE REASONS PROVIDED:
THIS
COURT’S JUDGMENT is that:
1.
The
accounting experts for the parties shall collaborate and produce within fifteen
(15) days an agreed upon amount of compensation for Apotex having regard to
those matters agreed upon and the findings made in these Reasons. They shall
submit a brief Report setting out the basis for their figure. If any matter
remains in dispute it shall be identified and I will set out a process for
resolving it.
2.
The
parties shall make submissions as to costs (no more than five pages) within ten
(10) days after the submission from the experts as above.
3.
Final
judgement is reserved until after receipt of the two foregoing matters.
“Roger T. Hughes”
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