SUPREME
COURT OF CANADA
Between:
Apotex Inc.
Appellant
and
AstraZeneca
Canada Inc., Minister of Health and
Attorney
General of Canada
Respondents
And between:
Apotex Inc.
Appellant
and
AstraZeneca
Canada Inc., Minister of Health and
Attorney
General of Canada
Respondents
‑ and ‑
Canadian
Generic Pharmaceutical Association and
Canada’s
Research‑Based Pharmaceutical Companies
Interveners
Coram:
McLachlin C.J. and Bastarache, Binnie, LeBel, Deschamps, Fish, Abella, Charron
and Rothstein JJ.
|
Reasons for
Judgment:
(paras. 1 to 43)
|
Binnie J. (McLachlin C.J. and Bastarache, LeBel,
Deschamps, Fish, Abella, Charron and Rothstein JJ. concurring)
|
______________________________
AstraZeneca Canada Inc. v. Canada (Minister of Health),
[2006] 2 S.C.R. 560, 2006 SCC 49
Apotex Inc. Appellant
v.
AstraZeneca Canada Inc., Minister of Health and
Attorney General of Canada Respondents
‑ and -
Apotex Inc. Appellant
v.
AstraZeneca Canada Inc., Minister of Health and
Attorney General of Canada Respondents
and
Canadian Generic Pharmaceutical Association and
Canada’s Research‑Based Pharmaceutical Companies Interveners
Indexed as: AstraZeneca Canada Inc. v. Canada (Minister of Health)
Neutral citation: 2006 SCC 49.
File No.: 30985.
2006: May 11; 2006: November 3.
Present: McLachlin C.J. and Bastarache, Binnie,
LeBel, Deschamps, Fish, Abella, Charron and Rothstein JJ.
on appeal from the federal court of appeal
Intellectual
property — Patents — Patented medicines — Notice
of compliance — Generic manufacturer applying in 1993 for notice
of compliance to manufacture and sell copy‑cat version of drug containing
omeprazole — Original drug sold in Canada from 1989 to
1996 — Innovator drug company continuing to list new patents associated
with drug even though it had withdrawn drug from market and had marketed no
related products — Generic manufacturer’s notice of compliance
establishing bioequivalence with 1989 version of drug — Whether
generic manufacturer was required to address new listed
patents — Whether s. 5(1) of Patented Medicines (Notice of
Compliance) Regulations refers to actual comparator drug copied by generic
manufacturer or to drug in any of its formulations — Patent Act,
R.S.C. 1985, c. P‑4, s. 55.2(4) — Patented Medicines
(Notice of Compliance) Regulations, SOR/93‑133, ss. 4(1), (5), 5(1).
In 1989, the respondent AstraZeneca, an innovator
manufacturer, obtained from the Minister of Health a notice of compliance
(“NOC”) enabling it to market its drug omeprazole for use in the treatment of
acidic stomach conditions. It was sold in Canada as Losec 20
from 1989 until 1996, when AstraZeneca decided to remove it from the
market and replace it with another formulation. AstraZeneca’s patent for
omeprazole then expired in 1999. In 2002, despite the absence of Losec 20
from the market, AstraZeneca obtained and registered with the Minister of
Health two more patents associated with Losec 20, but did not
incorporate this new technology into any of its products. In 1993, Apotex
filed an abbreviated new drug submission for a NOC for its generic version of
omeprazole, comparing its product to AstraZeneca’s 1989 version of Losec 20.
The Minister determined that Apotex was not required to address the after‑issued
patents and granted Apotex the NOC in 2004. AstraZeneca applied for
judicial review of this decision, and the motions judge upheld the Minister’s
decision. The Federal Court of Appeal overturned this judgment and quashed
Apotex’s NOC.
Held: The
appeal should be allowed.
Under the Patented Medicines (Notice of Compliance)
Regulations (“NOC Regulations”), a generic manufacturer that is not
prepared to await the expiry of what are alleged to be the relevant patents,
must challenge their validity or applicability to its proposed product
(s. 5). The challenge is to be embodied in a notice of allegation. The
innovator drug company may then apply for an order prohibiting the issuance of
the NOC based on the relevance, validity and applicability of the listed patents
(s. 7). The application for prohibition triggers a 24‑month
statutory freeze on the issuance of a NOC. In this case, the Minister was
entitled to issue the NOC to Apotex on the basis of Apotex’s abbreviated new
drug submission without subjecting it to the 24‑month statutory freeze in
respect of the after‑issued patents. The NOC Regulations are
concerned only with patents relevant to the innovator product actually copied
and not with subsequently issued and listed patents from which a generic manufacturer
could not receive a benefit. [3] [17]
AstraZeneca’s interpretation of the NOC Regulations,
which is rejected, would permit “evergreening” a product indefinitely by the
addition of new patents of marginal significance, which would trigger an
indefinite series of 24‑month statutory freezes, even though such
subsequently listed patents are not the subject of “early working” by the
generic manufacturer, and from which (as in the circumstances here) the generic
manufacturer derives no advantage. Such an interpretation not only flies in
the face of the limited regulatory purpose authorized by s. 55.2(4) of the
Patent Act , but attaches no significance to s. 4(5) of the NOC
Regulations which requires that particular patents be linked to particular
submissions. It is not to be presumed that the regulations insist on this
identification for no purpose. [23]
The scope of the protection to which AstraZeneca is
entitled is predicated on the patent list established under s. 4(1). With
respect to patents added afterwards, s. 4(5) indicates that a patentee
must link the submission to the patent list to which it relates, and to the NOC
to which the submissions are directed. This ensures that the Minister is able
to identify the precise patents relevant to the “early working” by a generic
manufacturer of its copy‑cat product. [20‑22]
Since, in this case, Apotex did not claim
bioequivalence or take advantage of the early working exception with respect
to the technology incorporated in the two after‑issued patents, the
scheme of the NOC Regulations and the statutory freeze with respect to
those patents should not apply to it. When the NOC Regulations are
considered in their context, including s. 55.2(4) of the Patent Act ,
the references in s. 5(1) to “another drug for the purpose of
demonstrating bioequivalence” and “the other drug” in respect of which patents
are listed can only mean the actual comparator drug and not a drug that never
became available on the market for comparison. [18] [23] [28] [36]
Cases Cited
Applied: Bristol‑Myers
Squibb Co. v. Canada (Attorney General), [2005]
1 S.C.R. 533, 2005 SCC 26; Bell ExpressVu Limited
Partnership v. Rex, [2002] 2 S.C.R. 559, 2002 SCC 42; overruled: Eli
Lilly Canada Inc. v. Canada (Minister of Health), [2003]
3 F.C. 140, 2003 FCA 24.
Statutes and Regulations Cited
Food and
Drug Regulations, C.R.C. 1978, c. 870,
ss. C.08.001.1, C.08.002.1(1)(a).
Food and Drugs Act, R.S.C. 1985, c. F‑27 .
Patent Act, R.S.C. 1985, c. P‑4, s. 55.2(1) , (2) , (4) .
Patented Medicines (Notice of
Compliance) Regulations, SOR/93-133, ss. 3(3),
4, 5, 6, 7, 8.
APPEAL from a judgment of the Federal Court of Appeal
(Noël, Sharlow and Malone JJ.A.), [2006] 1 F.C.R. 297,
254 D.L.R. (4th) 690, 336 N.R. 166,
40 C.P.R. (4th) 353, [2005] F.C.J. No. 889 (QL),
2005 FCA 189, reversing a decision of Kelen J. (2004),
263 F.T.R. 161, 36 C.P.R. (4th) 519, [2004] F.C.J.
No. 1545 (QL), 2004 FC 1277. Appeal allowed.
Harry B. Radomski,
Andrew R. Brodkin and Miles Hastie, for the
appellant.
Gunars A. Gaikis, Yoon Kang, Nancy P. Pei and
Colin B. Ingram, for the respondent AstraZeneca Canada Inc.
Peter M. Southey and Frederick B. Woyiwada, for the
respondents the Minister of Health and the Attorney General of Canada.
Edward Hore
and Kevin Zive, for the intervener the Canadian Generic
Pharmaceutical Association.
Patrick S. Smith and Henry S. Brown, Q.C., for the
intervener Canada’s Research‑Based Pharmaceutical Companies.
The judgment of the Court was delivered by
1
Binnie J. — On January 27,
2004, the respondent Minister issued to the appellant Apotex Inc. a notice of
compliance (“NOC”) permitting Apotex to manufacture and sell a copy-cat version
of a drug containing omeprazole. The drug was originally developed and
marketed as Losec 20 by the respondent AstraZeneca Canada Inc. The
patent on omeprazole itself, which is used to treat stomach conditions related
to hyperacidity, expired in 1999. AstraZeneca began to market Losec 20
in Canada in 1989 but withdrew it in September 1996 because it had developed
what it considered to be a superior drug using omeprazole magnesium. Apotex
wants approval to market the older Losec 20 product.
2
Nevertheless, AstraZeneca seeks to quash the NOC issued to Apotex on the
basis of two patents which it (or a related company) obtained and registered
with the Minister after Losec 20 was withdrawn from the market
(hereafter referred to as the 037 and 470 patents). The basis of AstraZeneca’s
objection at this stage is not patent infringement but the alleged failure of
Apotex to comply with the much litigated Patented Medicines (Notice of
Compliance) Regulations, SOR/93-133 (“NOC Regulations”), which are
reproduced in the Appendix. The NOC Regulations provide an innovator
drug company like AstraZeneca with procedures to freeze for the purpose of
assuring patent compliance the access of copy-cat patented medicines to market
“in addition to” whatever remedies a patent owner has under the ordinary law of
patents.
3
The response of Apotex is that the later patents have nothing to do with
the version of Losec 20 it copied, which did not (and could not) have
incorporated the 037 or 470 technology. The NOC Apotex received on January 27,
2004 does not approve the use by Apotex of that technology. Apotex copied the
1989 product and contends that in that respect all NOC regulatory requirements
have been satisfied. Apotex argues that even if it had wanted to copy the 037
and 470 technology, it could not have done so “[to] demonstrat[e]
bioequivalence” within the meaning of the NOC Regulations because
AstraZeneca never produced a product incorporating the technology taught by the
two subsequently issued and listed patents. Apotex could not copy a product
that did not exist. Kelen J. accepted the argument of Apotex that the NOC
Regulations were only concerned with patents relevant to the innovator
product actually copied, and not with subsequently issued and listed patents
from which, under the federal new drug approval process, a generic manufacturer
could receive no benefit ((2004), 263 F.T.R. 161, 2004 FC 1277). He therefore
dismissed AstraZeneca’s application to quash the Apotex NOC. The Federal Court
of Appeal reversed, Sharlow J.A. dissenting ([2006] 1 F.C.R. 297, 2005 FCA
189). In my view, Kelen J. and Sharlow J.A. reached the correct conclusion. I
would allow the appeal. The procedural delays afforded AstraZeneca by the
majority decision of the Federal Court of Appeal overshoot the provisions and
purpose of the NOC Regulations. The NOC 9427-A1114-195 issued by the
Minister on January 27, 2004 is valid.
A. Brief
Chronology of Events
4
June 19, 1989 NOC
issued to AstraZeneca for Losec 20 (DIN 00846503)
April 27, 1993 Apotex files an
abbreviated new drug submission (“ANDS”) seeking approval for Apo-omeprazole
alleging bioequivalence with the then version of Losec 20
(Apotex argues
that any patent activity by AstraZeneca that post-dates the 1993 filing of its
ANDS comparing its omeprazole product to AstraZeneca’s 1989 Losec 20
product is irrelevant.)
February 9, 1996 AstraZeneca files
application for the 037 patent
September 10, 1996 AstraZeneca withdraws Losec
20 from the market, and so advises the Minister
December 16, 1997 Apotex refiles for NOC
November 10, 1998 AstraZeneca files
application for the 470 patent
January 22, 1999 AstraZeneca files a
Supplementary New Drug Submission (“SNDS”) for approval of use of Losec 20
for treatment of H. Pylori
June 4, 1999 AstraZeneca obtains
NOC permitting it to claim treatment for H. Pylori as a new approved use
of Losec 20
July 12, 2000 AstraZeneca files
SNDS for corporate change of name
October 24, 2000 Name change NOC issued
February 26, 2002 470 patent issues
March 8, 2002 470 patent added to
Register in relation to both SNDS dated January 22, 1999 and the SNDS dated
July 12, 2000
April 16, 2002 037 patent issues
February 27, 2003 037 patent added to Register in
relation to both the SNDS dated January 22, 1999 and the SNDS dated July 12,
2000
January 27, 2004 NOC issued to Apotex
for Apo-omeprazole
5
Although the July 12, 2000 SNDS seems to have been of a purely
administrative nature, the Minister permitted the patents to be listed against
it. The position of Apotex is that the listing of the 037 and the 470 patents
was and is in any event irrelevant to the Apotex application.
6
The Minister concluded, and it is no longer disputed, that throughout
the period September 10, 1996 to the present, AstraZeneca’s Losec 20 has
been off the Canadian market. To the extent that there is a demand for an
“omeprazole only” product, it is not being met by AstraZeneca.
B. AstraZeneca’s
New Patents
7
The trial judge thought it curious that despite the withdrawal of Losec
20 AstraZeneca continued to list new patents in association with omeprazole
20 mg capsules. He found that “[n]o other brand name company has attempted to
list patents in this manner in Canada, making this a novel situation” (para.
5).
8
Kelen J. then quoted an undated internal memorandum from a departmental
official to the Deputy Minister of Health:
To date, the administrative policy has been to
address all patents listed for a drug. However, this is the first time
a patent has been listed for a supplemental new drug submission introducing a
change to a drug which was clearly never marketed, and to which the generic
could not have made a comparison.
The Patent Unit is recommending that Apotex should not
be required to address the ’470 patent. [Emphasis added; para. 14.]
Kelen J.
agreed with Apotex that even if the 037 and the 470 patents were properly added
to the register, the listing of such after-acquired patents was irrelevant to
the Apotex application.
9
The 037 patent, applied for on February 9, 1996 and issued April
16, 2002 describes a new “oral pharmaceutical dosage form” of several
compounds, including omeprazole, consisting of a core material “that contains a
proton pump inhibitor” and an outer polymer coating, the two layers being
separated by a water soluble salt. The patent also describes “a new efficient
process” for the manufacture of such a dosage in one step.
10
The 470 patent, applied for on November 10, 1998 and issued
February 26, 2002 teaches that “surprisingly . . . the substance omeprazole can
exist in more than one crystal form” and describes how a new “form A” of
omeprazole can be prepared and utilized, offering such advantages as being
“more stable” than the previously used crystalline form. It follows that
AstraZeneca must have taken the position before the Commissioner of Patents
(and accepted by him) that the new “form A” of omeprazole was patentably
distinct and different from the form of omeprazole used in the 1989 version of Losec
20.
11
As stated, neither of these inventions was incorporated into
AstraZeneca’s 1989 Losec 20 product to which Apotex made reference to
establish bioequivalence. Apotex could not have, and did not attempt to,
piggy-back on any clinical and testing work done by AstraZeneca in relation to
the 037 and 470 patents listed against its subsequent NOCs issued seven years
after the original Apotex application for its NOC. As Kelen J. found,
“[a] generic drug cannot be expected to compare itself to a drug which is not
available on the Canadian market. The generic drug manufacturer could not
obtain such a drug” (para. 46).
C. Legislative
Overview
12
The NOC Regulations lie at the intersection of two regulatory
systems with sometimes conflicting objectives. First, is the law governing
approval of new drugs, which seeks to ensure the safety and efficacy of new
medications before they can be put on the market. The governing rules are set
out in the Food and Drugs Act, R.S.C. 1985, c. F-27 (“FDA ”), and
the Food and Drug Regulations, C.R.C. 1978, c. 870. The FDA process
culminates (if successful) in the issuance of a NOC to an applicant
manufacturer by the Minister of Health on the advice of his officials in the
Therapeutic Products Directorate. The FDA objective is to encourage
bringing safe and effective medicines to market to advance the nation’s
health. The achievement of this objective is tempered by a second and to some
extent overlapping regulatory system created by the Patent Act, R.S.C.
1985, c. P-4 . Under that system, in exchange for disclosure to the public of
an invention, including the invention of a medication, the innovator is given
the exclusive right to its exploitation for a period of 20 years. Until 1993,
the two regulatory systems were largely kept distinct and separate.
13
The problem perceived by Parliament in 1993 was that if a generic
manufacturer waits to begin its preparation of a copy-cat medicine for
regulatory approval until the patent expires, the FDA approval process
will likely add at least two years to the effective monopoly of the patent
owner, which is two years of monopoly longer than the Patent Act
contemplates. On the other hand, if the generic manufacturer tries to work the
patented invention prior to the expiry of the patent, even if solely to
satisfy the FDA requirements for a NOC, it will infringe the patent,
thus inviting litigation by the patent owner (and this is a very litigious
industry).
14
The solution arrived at by Parliament in Bill C-91 (1993) was to
introduce an exemption from the owner’s patent rights which permits the generic
manufacturers to work the patented invention within the 20-year period (the
“early working” exception) to the extent necessary to obtain a NOC effective at
the time the patent(s) expire (s. 55.2(1) ) and to “stockpile” generic
product towards the end of the 20-year period to await lawful market entry
(s. 55.2(2) ). (The “stockpiling” exception was repealed by S.C. 2001, c.
10, s. 2(1) (in force July 12, 2001).)
15
Recognizing that the “early working” and “stockpiling” exceptions could
be abused, Parliament balanced creation of these exceptions with implementation
of a summary procedure designed to strengthen the protection of patent owners
against generic competitors within the 20-year patent period. The
legislative solution is found in s. 55.2 of the Patent Act as
follows:
55.2 (1) It is not an infringement of a
patent for any person to make, construct, use or sell the patented invention
solely for uses reasonably related to the development and submission of
information required under any law of Canada, a province or a country other
than Canada that regulates the manufacture, construction, use or sale of any
product. [The “early working” exception.]
(2) It is not an infringement of a patent for any
person who makes, constructs, uses or sells a patented invention in accordance
with subsection (1) to make, construct or use the invention, during the
applicable period provided for by the regulations, for the manufacture and
storage of articles intended for sale after the date on which the term of the
patent expires. [The “stockpiling” exception.]
(3) The Governor in Council may make regulations
for the purposes of subsection (2), but any period provided for by the
regulations must terminate immediately preceding the date on which the term of
the patent expires.
(4) The Governor in Council may make such
regulations as the Governor in Council considers necessary for preventing the
infringement of a patent by any person who makes, constructs, uses or sells a
patented invention in accordance with subsection (1) or (2) including,
without limiting the generality of the foregoing, regulations
(a) respecting the conditions that must be fulfilled before a
notice [e.g. of compliance] . . . may be issued . . .;
(b) respecting the earliest date on which a notice [e.g. of
compliance] . . . may take effect . . .;
(c) governing the resolution of disputes between a patentee or
former patentee and any person who applies for a notice [e.g. of compliance] .
. . as to the date on which that notice . . . may be issued or take effect;
The grant of
the regulation-making power in s. 55.2(4) is thus expressly limited to
prevention of infringement by a person who takes advantage of the “early
working” exception (s. 55.2(1) ) or (until its repeal) the “stockpiling”
exception (s. 55.2(2) ).
16
The NOC Regulations were enacted pursuant to s. 55.2(4) .
Their history and general structure were discussed by this Court in Bristol-Myers
Squibb Co. v. Canada (Attorney General), [2005] 1 S.C.R. 533, 2005 SCC 26
(the “Biolyse” decision). Serendipidously, our judgment was released
the day following the decision of the Federal Court of Appeal in this case.
For present purposes, the important aspect of the Biolyse decision is
the emphasis it placed on the need to interpret the NOC Regulations with
careful regard to the limited purposes set out in the aforesaid s. 55.2(4)
of the Patent Act .
17
The general scheme of the NOC Regulations is to create a Patent
Registry within the Department of Health in which an innovator drug company
like AstraZeneca may have patents listed relevant to its various drug
submissions for regulatory approval (s. 4). A generic manufacturer that is not
prepared to await the expiry of what are alleged to be the relevant patents
must challenge their validity or applicability to its proposed product
(s. 5). The challenge is to be embodied in a notice of allegation, which
will generally trigger an application in the Federal Court by the patent owner
to prohibit the issuance of a NOC based on (in its view) the relevance,
validity and applicability of the listed patents (s. 7). The unusual
feature of the NOC Regulations is that mere initiation by the patent
owner of its application for prohibition freezes ministerial action for 24
months unless the prohibition proceedings are earlier disposed of, which seems
to be rare (s. 7(1)(e)). As pointed out in the majority judgment
in Biolyse (at para. 24):
[U]nder this procedure, the court hearing the prohibition application
has no discretion to lift the stay even if it thinks the innovator’s case for
interim relief is weak. Nor does the court have a discretion to leave the
contending parties to their remedies under the Patent Act . The
“[generic manufacturer]”’s application for a NOC simply goes into deep-freeze
until the statutory procedures have played themselves out. For these reasons,
Iacobucci J. described the regime as “draconian” in Merck Frosst Canada Inc.
v. Canada (Minister of National Health and Welfare), [1998] 2 S.C.R. 193,
at para. 33.
18
If, as Apotex says, it did not have the advantage of an “early working”
of the after-listed 037 and 470 patents, because they came too late and were
not incorporated in any product available to Apotex to copy, it is difficult to
see in principle why in respect of those patents Apotex should be
subject to the NOC Regulations regime, with a consequent further delay
of two years, and perhaps longer. The Apotex submission has already been
pending since April 27, 1993.
D. The New
Drug Approval Process
19
The Food and Drug Regulations and departmental policies require
drug manufacturers to submit different types of new drug submission (“NDS”) for
different purposes. The two principal forms of submission are the NDS, filed
by an innovative drug manufacturer for a new drug product, and the ANDS, filed by
a generic manufacturer that claims its product is the “pharmaceutical
equivalent” of a previously approved “Canadian reference product”
(s. C.08.002.1(1)(a)). A SNDS may be submitted for substantive or
for purely administrative reasons. Unlike the situation in Biolyse, the
intention of the applicant Apotex from the outset was to produce a generic
(i.e. copy-cat) version of the AstraZeneca product marketed as Losec 20
in 1989. In this case, Apotex makes no pretence of originality.
E. Scope
of Regulatory Protection
20
The scope of the protection to which AstraZeneca is entitled as a person
who has filed a NDS is predicated on the patent list established under
s. 4(1). As stated in Biolyse, at para. 58: “The patent list
becomes the minefield that the generic ‘copy-cat’ manufacturer must navigate to
obtain a NOC.” The list of relevant patents is to be filed by the “first
person” (i.e. the innovator pharmaceutical company) at the time of its NDS
(s. 4(3)), or updated within 30 days of issuance of a new patent(s) that
had been applied for prior to filing for a submission but not issued until
afterwards (s. 4(4)). The 037 and 470 patents fall into this
“after-issued” category. (I note in passing that the 30-day limit seems not to
have been observed in the case of the 037 and 470 patents, but nothing turns on
that here.) Section 4 reads in relevant part as follows:
Patent
List
4. (1) A person who files or has filed a
submission for, or has been issued, a notice of compliance in respect of a drug
that contains a medicine may submit to the Minister a patent list certified in
accordance with subsection (7) in respect of the drug.
(2) A patent list submitted in respect of a drug must
(a) indicate the dosage form, strength and route of
administration of the drug;
(b) set out any Canadian patent that is owned by the person .
. . that contains a claim for the medicine itself or a claim for the use of the
medicine and that the person wishes to have included on the register;
(c) contain a statement that, in respect of each patent, the
person applying for a notice of compliance is the owner . . .;
(d) set out the date on which the term limited for the
duration of each patent will expire pursuant to section 44 or 45 of the Patent
Act ; and
(e) set out the address in Canada for service on the person of
any notice of an allegation . . . .
(3) Subject to subsection (4), a person who
submits a patent list must do so at the time the person files a submission for
a notice of compliance.
(4) A first person may, after the date of
filing of a submission for a notice of compliance and within 30 days after the
issuance of a patent that was issued on the basis of an application that
has a filing date that precedes the date of filing of the submission, submit
a patent list, or an amendment to an existing patent list, that includes
the information referred to in subsection (2).
(5) When a first person submits a patent list or
an amendment to an existing patent list in accordance with subsection (4), the
first person must identify the submission to which the patent list or the
amendment relates, including the date on which the submission was filed.
(6) A person who submits a patent list must keep
the list up to date but may not add a patent to an existing patent list
except in accordance with subsection (4).
(7) A person who submits a patent list or an
amendment to an existing patent list under subsection (1) or (4) must certify
that
(a) the information submitted is
accurate; and
(b) the patents set out on the patent list or in the amendment
are eligible for inclusion on the register and are relevant to the dosage form,
strength and route of administration of the drug in respect of which the
submission for a notice of compliance has been filed.
21
I emphasize the words in s. 4(5) that in the case of patents added
afterwards, “the first person must identify the submission to which the
patent list or the amendment relates, including the date on which
the submission was filed”. In addition, s. 3(3) provides that
“[n]o information submitted pursuant to section 4 shall be included on the
register until after the issuance of the notice of compliance in respect
of which the information was submitted.” These provisions, it seems to me,
provide an important key to understanding the scheme. Entry of the “Patent
list” does not destroy the linkage between the patent and the submission(s) to
which it relates, nor to the NOC to which the submission(s) are directed.
Specific patents are associated with one or more NDS, ANDS or SNDS, which in
turn (if approved) give rise to specific NOCs, which in turn approve a specific
manufacturer’s product, which a generic manufacturer may seek to copy. There
is no linkage between the 037 and 470 patents and the submissions that lead to
the Losec 20 product copied by Apotex. Those after-acquired patents
were listed in relation to a SNDS dated January 22, 1999 by AstraZeneca for a
new medical use for Losec 20 (treatment of H. Pylori), a use for
which the Apotex product is not approved, and to an administrative SNDS
submitted by AstraZeneca dated July 12, 2000, which submission has nothing at
all to do with the technology incorporated in Losec 20.
22
Thus understood, the s. 4(1) patent list in relation to a medication
that goes through various stages of development may become over time a list of
lists, or lists within a list. Section 4(5) ensures the Minister’s ability to
identify the precise patents relevant to the “early working” by a generic
manufacturer of its copy-cat product. This identification is important having
regard to the limited purposes for which the NOC Regulations are
authorized by s. 55.2(4) of the Patent Act .
23
AstraZeneca relies on Eli Lilly Canada Inc. v. Canada (Minister of
Health), [2003] 3 F.C. 140, 2003 FCA 24, for the proposition that a patent
list is submitted in respect of a drug and not in respect of any particular
submission. This is also the view taken by the majority judgment of the
Federal Court of Appeal in this case. On this view a “first person” could
carry on “evergreening” its product indefinitely by the addition of new patents
of marginal significance which would trigger an indefinite series of 24-month
statutory freezes even though such subsequently listed patents are not the subject
of “early working” by the generic manufacturer, and from which (as in the
circumstances here) the generic manufacturer derives no advantage. As this
case further illustrates, AstraZeneca even managed to piggy-back the 037 and
470 patents onto an administrative SNDS. An interpretation that would freeze
the generic product out of the market vacated by AstraZeneca in 1996 for a
further two years or more in these circumstances flies in the face of the
limited purpose authorized by s. 55.2(4) of the Patent Act . It is
not to be presumed that s. 4(5) of the NOC Regulations insisted on
linking particular patents to particular submissions for no purpose.
F. Obligation
of the Generic Applicant for a Notice of Compliance
24
When Apotex decided to seek approval to manufacture and market a
copy-cat version of Losec 20 in 1993, it saved itself a lot of time and
expense by showing that its proposed product was “bioequivalent” to the
AstraZeneca Losec 20 product, for which AstraZeneca had done the
research and clinical work to permit it to be “marketed in Canada pursuant to a
notice of compliance”. If the Apotex product is bioequivalent, Parliament
reasoned, the research and clinical work that shows AstraZeneca’s Losec 20
to be safe and effective equally shows the Apotex copy-cat product to be safe
and effective.
1. Standard
of Review
25
The outcome of this appeal turns on conflicting interpretations of
the NOC
Regulations.
On a question of legal interpretation, the Minister’s opinion is not entitled
to deference. The Federal Court of Appeal properly found that the standard of
review on the point in issue is correctness.
2. Principles
of Statutory Interpretation
26
It is now trite law that the words of an Act and regulations are to be
read in their entire context and in their grammatical and ordinary sense
harmoniously with the scheme of the Act, the object of the Act and the
intention of Parliament. Further, the scope of a regulation such as the
provisions of the NOC Regulations is constrained by its enabling
legislation, in this case s. 55.2(4) of Patent Act (Biolyse, at
para. 38).
3. The
Grammatical and Ordinary Sense of the Words
27
The generic manufacturer’s obligations are set out in s. 5(1) of the NOC
Regulations:
5. (1) Where a person files or has filed a
submission for a notice of compliance in respect of a drug and compares that
drug with, or makes reference to, another drug for the purpose of demonstrating
bioequivalence on the basis of pharmaceutical and, where applicable,
bioavailability characteristics and that other drug has been marketed in
Canada pursuant to a notice of compliance issued to a first person and in
respect of which a patent list has been submitted, the person shall,
in the submission, with respect to each patent on the register in respect of
the other drug,
(a) state that the person accepts that the notice of
compliance will not issue until the patent expires; or
(b) allege that
(i) the statement made by the first person pursuant to paragraph
4(2)(c) is false,
(ii) the patent has expired,
(iii) the patent is not valid, or
(iv) no claim for the medicine itself and no claim for the use of the
medicine would be infringed by the making, constructing, using or selling by
that person of the drug for which the submission for the notice of compliance
is filed.
28
I accept the linguistic point made by Noël J.A. in the Federal Court of
Appeal that the words “in respect of which” in s. 5(1) refer to “the other
drug”, i.e. the Canadian reference product, and not to a particular patent
list or amended patent list. However, it seems to me that the “other drug” is
the drug to which the generic manufacturer makes reference “for the purpose of
demonstrating bioequivalence”. If that “other drug” evolves over time by means
of patentably distinct inventions, the safety and efficacy of a new product
containing those patentably distinct inventions must be established to the
satisfaction of the Minister of Health (not the Commissioner of Patents). Thus
in Biolyse the Minister was not prepared to accept as bioequivalent a
drug made with the medicine paclitaxel sourced from the yew species taxus
canadensis in substitution for paclitaxel sourced from a different
species of yew. In matters of drug approval, bioequivalence requires proof,
not conjecture. If Apotex claims bioequivalence with Losec 20 it is
important to be precise about what generation of Losec 20 is the
comparator drug.
29
As stated, however, the majority judgment of the Federal Court of Appeal
proceeded on the basis that “the drug” was Losec 20 and that Apotex was
required to address all patents listed against Losec 20 in the Patent
Register, including the 037 and 470 patents. On this view, presumably, Apotex
would have to address new patents as fast as AstraZeneca could have them added
to the Losec 20 patent list, regardless of their relevance to the issue
of “early working” and “bioequivalence”. Sharlow J.A. adopted a narrower view,
excluding from consideration the 037 and 470 patents. Considering the entire
context, there is a measure of textual ambiguity as to what “another drug” and
“the other drug” refers to, and this ambiguity seems to have given rise to the
disagreement between Noël J.A. and Sharlow J.A. in the court below.
30
Ambiguity does not have to manifest itself in the text of s. 5(1).
Rather, “one must consider the ‘entire context’ of a provision before
one can determine if it is reasonably capable of multiple interpretations” (Bell
ExpressVu Limited Partnership v. Rex, [2002] 2 S.C.R. 559, 2002
SCC 42, at para. 29 (emphasis added)).
31
As to the 037 and 470 patents, the question is whether the reference in
s. 5(1) to “another drug for the purpose of demonstrating bioequivalence” and
“the other drug” against which patents are listed is a reference to Losec 20
in any of its formulations, including formulations never brought to
market (which is the AstraZeneca position); or does it mean, more narrowly, the
Losec 20 drug based on the June 19, 1989 NOC which Apotex copied (as
Apotex contends).
G. The
Regulatory Context
32
At the time of the Apotex ANDS in 1993, its Canadian reference product
was the version of Losec 20 brought to market in Canada by AstraZeneca
pursuant to the June 19, 1989 NOC. Section C.08.001.1 of the Food and Drug
Regulations defines “Canadian reference product” as
(a) a drug in respect of which a notice of compliance is
issued pursuant to section C.08.004 and which is marketed in Canada by
the innovator of the drug,
(b) a drug, acceptable to the Minister, that can be
used for the purpose of demonstrating bioequivalence on the basis of
pharmaceutical and, where applicable, bioavailability characteristics, where a
drug in respect of which a notice of compliance has been issued pursuant to
section C.08.004 cannot be used for that purpose because it is no longer
marketed in Canada, or
(c) a drug, acceptable to the Minister, that can be used for
the purpose of demonstrating bioequivalence on the basis of pharmaceutical and,
where applicable, bioavailability characteristics, in comparison to a drug
referred to in paragraph (a);
33
It is significant that this series of definitions draws distinctions
between a drug which is marketed in Canada (para. (a)) and a drug
“acceptable to the Minister that . . . cannot be used for that purpose” [i.e.
as a reference drug] because it is no longer marketed in Canada (para. (b)).
Under (b), unlike (a), the Minister is given a discretion based
on nothing but the fact that the product to which reference is made has been
withdrawn from the market. As a practical matter, there was no AstraZeneca
omeprazole product on the market after 1996 which Apotex could copy.
However, Apotex had obtained samples prior to 1996 sufficient to demonstrate
bioequivalence to the earlier technology incorporated in Losec 20. As stated,
that product did not incorporate the 037 and 470 patent inventions.
34
I agree with Noël and Malone JJ.A. that “[t]he fact that a first person
does not presently occupy the market has no bearing on the question whether a
second person’s proposed drug will infringe” (para. 54). However, as Noël J.A.
also conceded, “it is the actual drug, from which samples can be taken
and used for comparative purposes, that is relevant to the application of
subsection 5(1) of the NOC Regulations” (para. 46 (emphasis added)).
35
In my opinion, the rules governing acceptable “comparator” drugs give a
further important clue to the legislative intention. If, as para. (b)
says, a drug cannot be used as a comparator unless acceptable to the Minister
“because it is no longer marketed in Canada”, it seems obvious that a drug
cannot be used as a comparator if it has never been marketed in Canada.
That is the significance of the fact that AstraZeneca has never had a
product on the market based on AstraZeneca’s later submissions in relation to
which the 037 and 470 patents were listed.
36
Viewed in this light, it seems to me inescapable that the expression
“another drug” in s. 5(1) refers to the actual comparator drug — not a drug
that never became available for comparison — and that the words “with respect
to each patent on the register in respect of the other drug” carries the
same meaning.
37
The whole obligation incurred by the generic manufacturer under the NOC
Regulations is based on its “early working” of patents embodied in “another
drug for the purpose of demonstrating bioequivalence”. The only drug that fits
the description is the version of Losec 20 approved in the June 19, 1989
NOC.
H. The
Broader Statutory Purpose
38
I repeat that Parliament’s stated purpose in authorizing the NOC
Regulations was to permit the “early working” of the patented invention
(s. 55.2(4) ). As Apotex did not make use of the patented inventions taught by
the 037 and 470 patents, Apotex is not on this occasion within the mischief
aimed at by the NOC Regulations.
39
By imposing the 24-month delay called for by the NOC Regulations,
the decision of the Federal Court of Appeal undermines achievement of the
balance struck by Parliament between the objectives of the FDA and
regulations thereunder (making safe and effective drugs available to the
public) and the Patent Act and its regulations (preventing abuse of the
“early working” exception to patent infringement). Given the evident (and
entirely understandable) commercial strategy of the innovative drug companies
to evergreen their products by adding bells and whistles to a pioneering
product even after the original patent for that pioneering product has expired,
the decision of the Federal Court of Appeal would reward evergreening even if
the generic manufacturer (and thus the public) does not thereby derive any
benefit from the subsequently listed patents. In my view, s. 5(1) of the NOC
Regulations requires a patent-specific analysis, i.e. the generic
manufacturer is only required to address the cluster of patents listed against
submissions relevant to the NOC that gave rise to the comparator drug, in this
case the 1989 version of Losec 20.
40
If AstraZeneca had brought to market a Losec 20 product pursuant
to the later NOCs and if Apotex had made reference to that modified product for
the purpose of demonstrating bioequivalence, Apotex would have been required to
file a notice of allegation with respect to the 037 and 470 patents.
41
However, it is clear that AstraZeneca did not market any product
pursuant to the subsequent NOCs and that the preconditions to any obligations
of Apotex under s. 5(1) were therefore not triggered.
I. The
Apotex Product Cannot Claim the Advantages of the 037 and 470 Patents
42
Apotex acknowledges that its NOC dated January 27, 2004 does not permit
Apotex to produce a product formulated or manufactured in accordance with the
037 and 470 patents, nor to claim that the Apotex product is indicated for the
treatment of H. Pylori. This opinion deals only with the obligations of
Apotex under the NOC Regulations. AstraZeneca seemed to suggest at
various points during the oral hearing that Apotex is indeed infringing
AstraZeneca patents. If this be so (and there is no evidence before us either
way), then of course AstraZeneca retains all its remedies under the Patent
Act , including, in appropriate circumstances, an interlocutory injunction.
The only patent-related consequence of the present decision is to deny
AstraZeneca the benefit of a 24-month freeze without any proof of patent
infringement.
J. Conclusion
43
I would allow the appeal. The order of the Federal Court of Appeal is
set aside and the order of the Federal Court, Trial Division is restored.
Apotex is entitled to its costs in this Court and in the courts below. The
Minister is entitled to his costs in this Court and in the Federal Court of
Appeal.
APPENDIX
Patent Act,
R.S.C. 1985, c. P‑4
Infringement
.
. .
55.2 (1) [Exception] It is not an
infringement of a patent for any person to make, construct, use or sell the
patented invention solely for uses reasonably related to the development and
submission of information required under any law of Canada, a province or a
country other than Canada that regulates the manufacture, construction, use or
sale of any product.
(2) [Repealed, S.C. 2001, c. 10, s. 2(1) ]
(3) [Repealed, S.C. 2001, c. 10, s. 2(1) ]
(4) [Regulations] The Governor in Council may
make such regulations as the Governor in Council considers necessary for
preventing the infringement of a patent by any person who makes, constructs,
uses or sells a patented invention in accordance with subsection (1),
including, without limiting the generality of the foregoing, regulations
(a) respecting the conditions that must be fulfilled before
a notice, certificate, permit or other document concerning any product to which
a patent may relate may be issued to a patentee or other person under any Act
of Parliament that regulates the manufacture, construction, use or sale of that
product, in addition to any conditions provided for by or under that Act;
(b) respecting the earliest date on which a notice,
certificate, permit or other document referred to in paragraph (a) that
is issued or to be issued to a person other than the patentee may take effect
and respecting the manner in which that date is to be determined;
(c) governing the resolution of disputes between a patentee
or former patentee and any person who applies for a notice, certificate, permit
or other document referred to in paragraph (a) as to the date on which
that notice, certificate, permit or other document may be issued or take
effect;
(d) conferring rights of action in any court of competent
jurisdiction with respect to any disputes referred to in paragraph (c)
and respecting the remedies that may be sought in the court, the procedure of
the court in the matter and the decisions and orders it may make; and
(e) generally governing the issue of a notice, certificate,
permit or other document referred to in paragraph (a) in circumstances
where the issue of that notice, certificate, permit or other document might
result directly or indirectly in the infringement of a patent.
(5) [Inconsistency or conflict] In the event of
any inconsistency or conflict between
(a) this section or any regulations made under this section,
and
(b) any Act of Parliament or any regulations made
thereunder,
this section or the regulations made under this section shall prevail
to the extent of the inconsistency or conflict.
(6) [For greater certainty] For greater
certainty, subsection (1) does not affect any exception to the exclusive
property or privilege granted by a patent that exists at law in respect of acts
done privately and on a non‑commercial scale or for a non‑commercial
purpose or in respect of any use, manufacture, construction or sale of the
patented invention solely for the purpose of experiments that relate to the
subject‑matter of the patent.
Patented
Medicines (Notice of Compliance) Regulations, SOR/93‑133
Patent
List
4. (1) A person who files or has filed a
submission for, or has been issued, a notice of compliance in respect of a drug
that contains a medicine may submit to the Minister a patent list certified in
accordance with subsection (7) in respect of the drug.
(2) A patent list submitted in respect of a
drug must
(a) indicate the dosage form, strength and route of
administration of the drug;
(b) set out any Canadian patent that is owned by the person,
or in respect of which the person has an exclusive licence or has obtained the
consent of the owner of the patent for the inclusion of the patent on the
patent list, that contains a claim for the medicine itself or a claim for the
use of the medicine and that the person wishes to have included on the
register;
(c) contain a statement that, in respect of each patent,
the person applying for a notice of compliance is the owner, has an exclusive
licence or has obtained the consent of the owner of the patent for the
inclusion of the patent on the patent list;
(d) set out the date on which the term limited for the
duration of each patent will expire pursuant to section 44 or 45 of the Patent
Act ; and
(e) set out the address in Canada for service on the person
of any notice of an allegation referred to in paragraph 5(3)(b) or (c),
or the name and address in Canada of another person on whom service may be
made, with the same effect as if service had been made on the person.
(3) Subject to subsection (4), a person who
submits a patent list must do so at the time the person files a submission for
a notice of compliance.
(4) A first person may, after the date of
filing of a submission for a notice of compliance and within 30 days after the
issuance of a patent that was issued on the basis of an application that has a
filing date that precedes the date of filing of the submission, submit a patent
list, or an amendment to an existing patent list, that includes the information
referred to in subsection (2).
(5) When a first person submits a patent list
or an amendment to an existing patent list in accordance with subsection (4),
the first person must identify the submission to which the patent list or the
amendment relates, including the date on which the submission was filed.
(6) A person who submits a patent list must
keep the list up to date but may not add a patent to an existing patent list
except in accordance with subsection (4).
(7) A person who submits a patent list or an
amendment to an existing patent list under subsection (1) or (4) must certify
that
(a) the information submitted is accurate; and
(b) the patents set out on the patent list or in the
amendment are eligible for inclusion on the register and are relevant to the
dosage form, strength and route of administration of the drug in respect of
which the submission for a notice of compliance has been filed.
5. (1) Where a person files or has filed a
submission for a notice of compliance in respect of a drug and compares that
drug with, or makes reference to, another drug for the purpose of demonstrating
bioequivalence on the basis of pharmaceutical and, where applicable,
bioavailability characteristics and that other drug has been marketed in Canada
pursuant to a notice of compliance issued to a first person and in respect of
which a patent list has been submitted, the person shall, in the submission,
with respect to each patent on the register in respect of the other drug,
(a) state that the person accepts that the notice of
compliance will not issue until the patent expires; or
(b) allege that
(i) the statement made by the first person pursuant to paragraph
4(2)(c) is false,
(ii) the patent has expired,
(iii) the patent is not valid, or
(iv) no claim for the medicine itself and no claim for the use of
the medicine would be infringed by the making, constructing, using or selling
by that person of the drug for which the submission for the notice of
compliance is filed.
.
. .
(2) Where, after a second person files a
submission for a notice of compliance but before the notice of compliance is
issued, a patent list or an amendment to a patent list is submitted in respect
of a patent pursuant to subsection 4(4), the second person shall amend the submission
to include, in respect of that patent, the statement or allegation that is
required by subsection (1) or (1.1), as the case may be.
(3) Where a person makes an allegation pursuant
to paragraph (1)(b) or (1.1)(b) or subsection (2), the person shall
(a) provide a detailed statement of the legal and factual
basis for the allegation;
(b) if the allegation is made under any of subparagraphs
(1)(b)(i) to (iii) or (1.1)(b)(i) to (iii), serve a notice of the
allegation on the first person;
(c) if the allegation is made under subparagraph (1)(b)(iv)
or (1.1)(b)(iv),
(i) serve on the first person a notice of the allegation relating to
the submission filed under subsection (1) or (1.1) at the time that the person
files the submission or at any time thereafter, and
(ii) include in the notice of allegation a description of the dosage
form, strength and route of administration of the drug in respect of which the
submission has been filed; and
(d) serve proof of service of the information referred to in
paragraph (b) or (c) on the Minister.
Right
of Action
6. (1) A first person may, within 45 days
after being served with a notice of an allegation pursuant to paragraph 5(3)(b)
or (c), apply to a court for an order prohibiting the Minister from
issuing a notice of compliance until after the expiration of a patent that is
the subject of the allegation.
(2) The court shall make an order pursuant to
subsection (1) in respect of a patent that is the subject of one or more
allegations if it finds that none of those allegations is justified.
(3) The first person shall, within the 45 days
referred to in subsection (1), serve the Minister with proof that an
application referred to in that subsection has been made.
.
. .
(5) In a proceeding in respect of an
application under subsection (1), the court may, on the motion of a second
person, dismiss the application
(a) if the court is satisfied that the patents at issue are
not eligible for inclusion on the register or are irrelevant to the dosage
form, strength and route of administration of the drug for which the second
person has filed a submission for a notice of compliance; or
(b) on the ground that the application is redundant,
scandalous, frivolous or vexatious or is otherwise an abuse of process.
.
. .
(9) In a proceeding in respect of an
application under subsection (1), a court may make any order in respect of
costs, including on a solicitor‑and‑client basis, in accordance
with the rules of the court.
(10) In addition to any other matter that the
court may take into account in making an order as to costs, it may consider the
following factors:
(a) the diligence with which the parties have pursued the
application;
(b) the inclusion on the certified patent list of a patent
that should not have been included under section 4; and
(c) the failure of the first person to keep the patent list
up to date in accordance with subsection 4(6).
Notice
of Compliance
7. (1) The Minister shall not issue a notice
of compliance to a second person before the latest of
(a) [Repealed, SOR/98‑166, s. 6(1)]
(b) the day on which the second person complies with section
5,
(c) subject to subsection (3), the expiration of any patent
on the register that is not the subject of an allegation,
(d) subject to subsection (3), the expiration of 45 days
after the receipt of proof of service of a notice of any allegation pursuant to
paragraph 5(3)(b) or (c) in respect of any patent on the
register,
(e) subject to subsections (2), (3) and (4), the expiration
of 24 months after the receipt of proof of the making of any application under
subsection 6(1), and
(f) the expiration of any patent that is the subject of an
order pursuant to subsection 6(1).
(2) Paragraph (1)(e) does not apply if
at any time, in respect of each patent that is the subject of an application
pursuant to subsection 6(1),
(a) the patent has expired; or
(b) the court has declared that the patent is not valid or
that no claim for the medicine itself and no claim for the use of the medicine
would be infringed.
.
. .
(4) Paragraph (1)(e) ceases to apply in
respect of an application under subsection 6(1) if the application is withdrawn
or discontinued by the first person or is dismissed by the court hearing the
application.
(5) If the court has not yet made an order
under subsection 6(1) in respect of an application, the court may
(a) shorten the time limit referred to in paragraph (1)(e)
on consent of the first and second persons or if the court finds that the first
person has failed, at any time during the proceeding, to reasonably cooperate
in expediting the application; or
(b) extend the time limit referred to in paragraph (1)(e)
on consent of the first and second persons or, if the court finds that the
second person has failed, at any time during the proceeding, to reasonably
cooperate in expediting the application.
8. (1) If an application made under
subsection 6(1) is withdrawn or discontinued by the first person or is
dismissed by the court hearing the application or if an order preventing the
Minister from issuing a notice of compliance, made pursuant to that subsection,
is reversed on appeal, the 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.
(2) A second person may, by action against a
first person, apply to the court for an order requiring the first person to
compensate the second person for the loss referred to in subsection (1).
.
. .
(4) The court may make such order for relief by
way of damages or profits as the circumstances require in respect of any loss
referred to in subsection (1).
(5) In assessing the amount of compensation the
court shall take into account all matters that it considers relevant to the
assessment of the amount, including any conduct of the first or second person
which contributed to delay the disposition of the application under subsection
6(1).
Appeal allowed with costs.
Solicitors for the appellant: Goodmans, Toronto.
Solicitors for the respondent AstraZeneca Canada
Inc.: Smart & Biggar, Toronto.
Solicitor for the respondents the Minister of Health and the
Attorney General of Canada: Attorney General of Canada, Ottawa.
Solicitors for the intervener the Canadian Generic Pharmaceutical
Association: Hazzard & Hore, Toronto.
Solicitors for the intervener Canada’s Research‑Based
Pharmaceutical Companies: Gowling Lafleur Henderson, Ottawa.
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