Docket: A-146-14
Citation:
2015 FCA 166
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CORAM:
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NADON J.A.
DAWSON J.A.
BOIVIN J.A.
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BETWEEN:
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ELI LILLY
CANADA INC.
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Appellant
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And
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ATTORNEY
GENERAL OF CANADA and MINISTER OF HEALTH
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Respondents
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REASONS
FOR JUDGMENT
NADON J.A.
[1]
This is an appeal from a judgment of Madam
Justice Bédard (the Judge) of the Federal Court dated February 17, 2014 (2014
FC 152; the Federal Court Decision) wherein she dismissed Eli Lilly Canada
Inc.’s (the Appellant’s) application for judicial review of a decision made by
the Minister of Health (the Minister) on May 30, 2011 in which the Minister
refused to list the Appellant’s Canadian patent No. 2,379,329 (the ‘329 Patent
or the Patent) on the patent register (the Register) maintained under the Patented
Medicines (Notice of Compliance) Regulations S.O.R./93-133, as am. by S.O.R./98-166,
S.O.R./99-379, S.O.R./2006-242 (the Regulations) against the Appellant’s drug
product Trifexis identified as New Drug Submission No. 141 509 (NDS 141 509).
[2]
The main issue in this appeal is whether the
Minister was wrong in refusing to list the ‘329 Patent against the Appellant’s
approved Trifexis drug product on the Register. In my view, the Minister was
wrong to refuse to list the ‘329 Patent on the Register and consequently the
Judge below ought to have intervened.
I.
Factual Background
[3]
The relevant facts are not complicated and can
be summarized as follows.
[4]
Trifexis is the Appellant’s drug product. On
September 16, 2010, the Appellant filed a new drug submission, NDS 141 509,
with the Minister for this drug product which is intended for veterinary use,
specifically the prevention of heartworm disease, the prevention and treatment
of flea infestations and the treatment and control of adult hookworm, adult
roundworm and adult whipworm infections in dogs and puppies.
[5]
On November 1, 2011, the Minister issued a Notice
of Compliance (NOC) in respect of NDS 141 509. More particularly, the Minister
approved NDS 141 509 for a precise formulation containing two medicinal
ingredients, namely spinosad and milbemycin oxime.
[6]
The ‘329 Patent entitled “Oral Treatment of Companion Animals with Ectoparasiticidal
Spinosyns” was filed with the Patent Office on August 2, 2000 and issued
on October 20, 2009. Its invention pertains to oral formulations of
agricultural insecticides known as spinosyns that are to be administered to
companion animals, such as household dogs and cats for control of parasite
infections such as fleas and other parasites that can cause heartworm disease.
[7]
The ‘329 Patent, which contains seven claims,
indicates that the formulation of the invention may include, in combination
with the spinosyn compound, other compounds with antiparasite activity, such as
“milbemycins”. None of the claims expressly
refer to milbemycin oxime. They do, however, expressly refer to spinosad.
[8]
The relevant part of the disclosure, for the
purpose of this appeal, is found at page 8 of the ‘329 Patent and provides as
follows:
The formulations of this invention may
further include, in combination with the spinosyn component, one or more other
compounds that have activity against the specific ectoparasite or endoparasite
to be controlled, such as, for example, synthetic
pyrethroids, natural pyrethins, organophosphates, organochlorines, carbamates,
foramidines, avermectins, milbemycins, insect growth regulators
(including chitin synthesis inhibitors, juvenile hormone analogs, and juvenile
hormones), nitromethylenes, pyridines and pyrazoles.
….
The term “oral formulation” means that the
spinosyn component or components, either alone or in combination with one or
more of the other types of compounds listed supra, is formulated into a
product or formulation suitable for administering to the animal by mouth.
[Emphasis added]
[9]
As to the claims, claims 1 and 5 are relevant
and they read as follows:
1. A single-dose
oral formulation for controlling an ectoparasite infestation on a dog or cat
comprising an ectoparasiticidal amount of spinosad, or a physiologically
acceptable N-demethyl derivative or salt thereof, and a physiologically
acceptable carrier in a dosage form selected from tablet, capsule or liquid
suitable for administration once every at least 7 days at a dose of 10 to 100
mg of spinosad per kg of body weight.
…
5. A single-dose oral formulation for
controlling an ectoparasite infestation on a dog or cat comprising an
ectoparasiticidal amount of spinosad, or a physiologically acceptable
N-demethyl derivative or salt thereof, and a physiologically acceptable carrier
in a chewable treat oral dosage form suitable for administration once every at
least 7 days at a dose of 10 to 100 mg of spinosad per kg of body weight.
[10]
On September 16, 2010, the Appellant filed
patent lists with the Office of Patented Medicines and Liaison (OPML) at Health
Canada to list the ‘329 Patent in respect of NDS 141 509.
[11]
By letter dated November 8, 2010, the Minister
advised the Appellant that the ‘329 Patent was not eligible for listing in
respect of NDS 141 509 on the grounds that it did not contain a claim for the
two compounds found in its drug product. More particularly, the Minister
indicated that the ‘329 Patent did not claim the medicinal ingredients spinosad
and milbemycin oxime, that it did not claim the formulation containing the two
medicinal ingredients and that it did not claim the use of the two medicinal
ingredients, as required by subsection 4(2) of the Regulations. In other words,
the Minister made it clear to the Appellant that the ‘329 Patent did not
contain a claim for the formulation containing both spinosad and milbemycin
oxime, but rather that it contained claims for a formulation containing
spinosad alone. The Minister’s letter concluded by advising the Appellant that
it could provide written representations in response within the next 30 days.
[12]
The Appellant responded to the Minister’s letter
on March 31, 2011. On May 30, 2011, the Minister advised the Appellant that, after
consideration of its written representations, the OPML maintained its view that
the ‘329 Patent was not eligible for listing on the Register in respect of NDS
141 509 (the Minister’s Decision).
[13]
In the Minister’s opinion, although milbemycins
are mentioned in the ‘329 Patent as compounds which can be combined with
spinosad, the Patent does not meet the requirements of paragraph 4(2)(b)
of the Regulations which require that the patent make a claim to the formulation
containing the medicinal ingredients found in the NOC-approved drug. The
Minister’s view is expressed as follows (Minister’s Decision, p. 3):
While we agree that the ‘329 patent contains
claims for a formulation containing the medicinal ingredient spinosad, there
are no claims in the ‘329 patent specifying milbemycin oxime as the second
medicinal ingredient present in the formulation of the invention. The mere
mention of milbemycins in the disclosure as one of many groups of compounds
that may be combined with spinosad in the formulation of the invention is not
sufficient to constitute a claim for the formulation containing the medicinal
ingredients(s), as required by section 2 and paragraph 4(2)(b) of the PM(NOC)
Regulations. Specifically, the passage at page 8 of the disclosure of the
‘329 patent, to which you refer in your representations, states the following:
The
formulation of this invention may further include, in combination with the spinosyn
component, one or more other compounds that have activity against the specific
ectoparasite or endoparasite to be controlled, such as, for example, synthetic
pyrethroids, natural pyrethins, organophosphates, organochlorines, carbamates,
foramidines, avermectins, milbemycins, insect growth regulators (including
chitin synthesis inhibitors, juvenile hormone analogs, and juvenile hormones),
nitromethylenes, pyridines and pyrazoles.
Milbemycins are characterized as a family of
macrolide antibiotics with insecticidal and acaricidal activity and include not
only milbemycin oxime but milbemectin, nemadectin and moxidectin as well. This
characterization is consistent with that of your expert, Dr. Manon Paradis who
acknowledges at paragraph 24 of her affidavit that:
24.
Macrocyclic lactones are broad spectrum potent antiparasitic agents derived
from soil organisms and include two closely related chemical groups:
avermectins (e.g., ivermectin, abamectin, eprinomectin, doramectin and
selamectin) and milbemycins (e.g., milbemycin oxime and moxidectin). […]
Therefore, even
if the OPML accepts your position that the PM(NOC) Regulations do not
require that all of the medicinal ingredients present in the approved drug be
specified in the claim for the formulation, a close examination of the
above-noted passage of the disclosure reveals that the specific medicinal ingredient
milbemycin oxime, which is not explicitly mentioned in the claims, is also
not explicitly mentioned in the disclosure. Rather, as indicated above,
milbemycins are mentioned as one of many groups of compounds that may be
combined with spinosad in the formulation of the invention.
[Emphases in original]
[14]
As a result of the Minister’s Decision, the Appellant
brought an application for judicial review under section 18.1 of the Federal
Courts Act, R.S.C. 1985 c. F-7. On February 17, 2014, the Judge dismissed
the Appellant’s application with costs.
[15]
Before turning to the Federal Court Decision, a
few words concerning the administrative framework pursuant to which drug
products such as Trifexis are approved for marketing in Canada will be useful
in the present case.
II.
Administrative Framework
[16]
To advertise or sell a new drug in Canada,
manufacturers require the issuance of a NOC from the Minister. In order to
obtain a NOC, they must file a drug submission for their product which
satisfies the Minister that it is safe and effective.
[17]
New drug submissions, which are usually filed by
innovator companies pursuant to section C.08.002 of the Food and Drug
Regulations, C.R.C., c. 870 (the FDR), typically contain considerable
clinical trial data and detailed studies which form the basis upon which their
product will be approved for sale in Canada.
[18]
No NOC can be issued by the Minister if
prohibited by the Regulations. Prohibition to issue NOCs begins with the filing
of a patent list by innovators in which they describe the patents which they
seek to list on the Register against their drug products. The Minister,
pursuant to subsection 3(2) of the Regulations, is bound to maintain the Register.
Hence, through her officials in the OPML, the Minister may add patents to the Register
which meet the prescribed requirements and may refuse to add, or may delete,
those patents that do not meet the prescribed requirements.
[19]
In order to qualify under the Regulations, a
patent must meet the requirements of subsection 4(2):
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4. (2) A patent on a patent list in relation to a new drug
submission is eligible to be added to the register if the patent contains
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4. (2) Est admissible à l’adjonction au
registre tout brevet, inscrit sur une liste de brevets, qui se rattache à la
présentation de drogue nouvelle, s’il contient, selon le cas :
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(a) a claim for the medicinal ingredient and the medicinal
ingredient has been approved through the issuance of a notice of compliance
in respect of the submission;
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a) une
revendication de l’ingrédient médicinal, l’ingrédient ayant été approuvé par
la délivrance d’un avis de conformité à l’égard de la présentation;
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(b) a claim for the formulation that contains the medicinal
ingredient and the formulation has been approved through the issuance of a
notice of compliance in respect of the submission;
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b) une
revendication de la formulation contenant l’ingrédient médicinal, la
formulation ayant été approuvée par la délivrance d’un avis de conformité à
l’égard de la présentation;
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(c) a claim for the dosage form and the dosage form has
been approved through the issuance of a notice of compliance in respect of
the submission; or
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c) une
revendication de la forme posologique, la forme posologique ayant été
approuvée par la délivrance d’un avis de conformité à l’égard de la présentation;
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(d) a claim for the use of the medicinal ingredient, and
the use has been approved through the issuance of a notice of compliance in
respect of the submission.
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d) une
revendication de l’utilisation de l’ingrédient médicinal, l’utilisation ayant
été approuvée par la délivrance d’un avis de conformité à l’égard de la
présentation.
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[20]
Of particular relevance to this appeal is
paragraph 4(2)(b) of the Regulations, i.e. “claim
for the formulation.” This phrase is defined in section 2 of the Regulations:
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“claim for the formulation”
“claim for the
formulation” means a claim for a substance that is a mixture of medicinal and
non-medicinal ingredients in a drug and that is administered to a patient in
a particular dosage form; (revendication de la formulation)
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« revendication de la formulation »
« revendication
de la formulation » Revendication à l’égard d’une substance qui est un
mélange des ingrédients médicinaux et non médicinaux d’une drogue et qui est
administrée à un patient sous une forme posologique donnée. (claim for the
formulation)
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[21]
At issue in this appeal is whether the ‘329 Patent
claims a formulation that contains the two medicinal ingredients found in Trifexis
for which the Minister has issued a NOC.
III.
Federal Court Decision
[22]
I now turn to the Federal Court Decision. After
setting out the factual background, the Minister’s decision and the regulatory
framework, the Judge turned to the issues and the standard of review.
[23]
She first indicated that the Minister was bound
to apply the three-step test enunciated by Hughes J. in Abbott Laboratories
Ltd. v. Canada (Attorney General), 2008 FC 700, 67 C.P.R. (4th) 51 (Abbott
FC) to determine the eligibility of a patent for listing on the Register
(the Abbott test). The Abbott test has been accepted by this Court
in a number of decisions: Abbott Laboratories Ltd. v. Canada (Attorney
General), 2008 FCA 354, [2009] 3 F.C.R. 547 at paragraphs 29 – 33 (Abbott
FCA); G.D. Searle & Co. v. Canada (Minister of Health), 2009 FCA
35, 386 N.R. 262 at paragraphs 33 - 35 (Searle); Purdue Pharma v. Canada
(Attorney General), 2011 FCA 132, 417 N.R. 223 at paragraphs 111 - 113
(Purdue); and Gilead Sciences Canada Inc. v. Canada (Minister of
Health), 2012 FCA 254, 435 N.R. 188 at paragraphs 11 – 12 (Gilead FCA).
[24]
In the context of this case, the Judge
formulated the Abbott test as follows (Federal Court Decision, para. 16):
In this case,
paragraph 4(2)(b) of the Regulations which relates to a claim for a
formulation is involved. The Minister was required to answer the following questions:
(1) What
formulation does the patent claim?
(2) What is the formulation of the NOC issued for the drug in
question?
(3) Is the formulation claimed by the patent that which was
authorized in the NOC?
[25]
The Judge then turned to the applicable standards
of review. In her view, based on this Court’s decisions in Abbott FCA, Searle,
Purdue and Gilead FCA, the first step had to be determined on a
standard of correctness. The second prong was in turn reviewable on a
reasonableness standard. Lastly, the third step involved two questions
reviewable on different standards, correctness with regard to the Minister’s
interpretation of paragraph 4(2)(b) of the Regulations and
reasonableness with respect to the Minister’s application of paragraph 4(2)(b)
to the facts before her.
[26]
Both sides agreed that there was no issue with
respect to the second prong of the Abbott test. Therefore, the Judge set
out the three issues raised by the Appellant’s application as follows:
I.
Was the Minister correct in construing the ‘329
Patent?
II.
Was the Minister correct in interpreting the
requirements of paragraph 4(2)(b) of the Regulations?
III.
Was the Minister’s refusal to list the ‘329
Patent on the Register reasonable?
[27]
The Judge then reviewed the parties’ submissions
and evidence. She carefully set out the Appellant’s expert evidence, namely the
affidavits of Dr. Manon Paradis, a veterinarian and professor at the Department
of Clinical Sciences, Faculty of Veterinarian Medicine at the University of
Montreal and of Mr. Michel Sofia, a patent agent with Bereskin and Parr LLP,
with over 23 years of experience in intellectual property.
[28]
She then proceeded to determine the questions
before her. Firstly, she dealt with the question of whether the Minister had
correctly construed the ‘329 Patent. She observed that the Minister had found
that the ‘329 Patent did not contain a formulation containing both spinosad and
milbemycin oxime.
[29]
She then reviewed the principles of patent
construction from the Supreme Court of Canada’s decisions in Free World
Trust v. Électro Santé Inc., 2000 SCC 66, [2000] 2 S.C.R. 1024 (Free
World) and Whirlpool Corp. v. Camco Inc., 2000 SCC 67, [2000] 2
S.C.R. 1067 (Whirlpool), namely that patents are to be construed through
the eyes of persons skilled in the art willing to understand the invention and
that claims construction must be undertaken in a purposive manner.
[30]
The Judge then referred to this Court’s decision
in Purdue for the principle that construction of a patent for the
purpose of determining its eligibility under the Regulations is to follow the
principles set out in Free World and Whirlpool.
[31]
The Judge then posed the key question, as she
saw it (Federal Court Decision, para. 62):
In this case, the question to be asked is
whether a person skilled in the art would have understood that the formulations
encompassed in the ‘329 Patent claims, in light of the definition provided for
the term “oral formulation”, could include a formulation containing the
specific medicinal ingredients spinosad and milbemycin oxime.
[32]
In answer to this question, she held that the
claims of the ‘329 Patent included not only spinosad as the active ingredient,
but other active ingredients such as milbemycin oxime. In arriving at this
conclusion, the Judge relied mainly on the evidence of both Dr. Paradis and Mr. Sofia
(Federal Court Decision, para. 69).
[33]
The Judge therefore found that the Minister had
erred in her construction of the patent. However, she added that this finding was
not conclusive of the ‘329 Patent’s eligibility to be listed on the Register “since the matching exercise under paragraph 4(2)(b) of the
regulations has yet to be done” (Federal Court Decision, para. 71).
[34]
The Judge then turned to the third prong of the Abbott
test, i.e. whether the Minister had correctly interpreted the requirements
of paragraph 4(2)(b) of the Regulations and applied them to the relevant
facts.
[35]
She began by agreeing with the Minister that, to
be eligible for listing under paragraph 4(2)(b) of the Regulations,
the formulation claimed by the ‘329 Patent had to include the two medical
ingredients found in Trifexis. In the Judge’s opinion, this view was in
accordance with the principles set out in Abbott FCA, Searle, Purdue
and Gilead. In her opinion, these cases established that subsection 4(2)
of the Regulations, as amended in 2006, had introduced a “product specificity requirement” and that a “perfect match” between the compounds claimed in the
patent and those found in the NOC-approved drug was required. In support of that
view, the Judge again referred to Purdue, Searle and Gilead
FCA quoting those passages from these decisions which she believed
supported her perspective (Federal Court Decision, paras. 72-78).
[36]
This led her to find that the Minister had
correctly interpreted paragraph 4(2)(b) of the Regulations (Federal
Court Decision, para. 78). Thus she examined whether the Minister’s decision to
exclude the ‘329 Patent was reasonable.
[37]
She began her inquiry by observing that the
Minister had excluded the ‘329 Patent because of her view that its claims did
not match the authorized formulation in Trifexis in that the ‘329 Patent’s claims
did not include a formulation containing spinosad and milbemycin oxime (Federal
Court Decision, para. 79).
[38]
The Judge then reiterated that her construction
of the ‘329 Patent was broader than that of the Minister and that “the claims are directed not only to a formulation including
spinosad alone as the active ingredient, but also to formulations that include
other active ingredients such as, but not restricted to, milbemycin oxime”
(Federal Court Decision, para. 80).
[39]
She then made the following, in my view somewhat
equivocal, statement (Federal Court Decision, para. 81):
The question now is whether the fact that
the claims can be read as covering a formulation that could, but that does not
necessarily, comprise the specific ingredient, milbemycin oxime, is sufficient
to meet the strict matching requirement with Trifexis’ NOC which clearly
comprise this specific ingredient.
I say that this statement is equivocal because
it appears to contradict the clear finding made by the Judge at paragraph 69 of
the Federal Court Decision that the ‘329 Patent claimed a formulation
containing both spinosad and milbemycin oxime. I shall return to this point
later in these reasons.
[40]
In the Judge’s view, this case offered a similar
situation to that at issue in Gilead FCA. She quoted paragraph 46 of the
Federal Court’s decision in that case (Gilead Sciences Canada Inc. v. Canada
(Minister of Health), 2012 FC 2, 403 F.T.R. 86 (Gilead FC)) and then
opined as follows (Federal Court Decision, paras. 83-86):
The applicant distinguishes the facts in Gilead
from those in this case. He asserts that the medicinal ingredient that was not
specifically mentioned in the patent claims in Gilead (the patent
referred to the general class of non-nucleoside transcriptase inhibitors
(NNRTIs) to which the specified medicinal ingredient mentioned in the approved
drug belongs), but was specified in the NDS, was invented and disclosed only
after Gilead’s invention and as such, a person of ordinary skill in the
art could not have known of its existence at the relevant time. This
distinction is a valid one as it is clear in this case that, at the relevant
time, milbemycin oxime existed and was part of the family of milbemycins.
However, the Federal Court of Appeal
endorsed the Federal Court’s reasoning pertaining to the product specificity
requirement. It is worth noting that Justice Mosley’s finding was that it was
insufficient for a patent to meet the product specificity requirement by
referring to a class of compound rather than to a specific medicinal
ingredient. He found that the claim was not specific enough to match the
medicinal ingredients in Complera. That conclusion was based on the principle
above, not on the fact that the third medicinal ingredient could not have been
claimed in the patent because it had not been discovered at the date of the
patent’s publication.
I feel bound by this reasoning and,
therefore, I conclude that it should equally apply to the case at bar. Referring
to the general family of milbemycins in the definition of oral formulation is
not specific enough to conclude that the claims match the formulation contained
in Trifexis. In my respectful view, this conclusion is not altered by the
possibility that the ‘329 Patent could extend to a formulation containing
milbemycin oxime.
For all of these reasons, I conclude that
the Minister’s decision to refuse to list the ‘329 Patent on the patent
register was reasonable despite the fact that the Minister erred in her
construction of the patent claims.
[41]
Thus, the Judge was satisfied that she was bound
to follow our decision in Gilead FCA. In her view, reference in the ‘329
Patent to milbemycins was not sufficiently specific so as to allow her to find
that its claims matched the formulation found in Trifexis.
[42]
As a result, she concluded that the Minister’s
decision to refuse to list the ‘329 Patent on the Register was reasonable
notwithstanding the fact that the Minister had erred in construing the claims
of the ‘329 Patent.
IV.
Issues
[43]
In my view, there are two issues to be
determined by us in this appeal. First, whether the Judge erred with respect to
her construction of the ‘329 Patent’s claims and her consequent overturning of
the Minister’s determination on that issue and second, whether the Judge erred
in respect of the third prong of the Abbott test for patent listing
eligibility, i.e. whether the formulation claimed in the ‘329 Patent is the
formulation found in the Appellant’s drug submission for Trifexis.
V.
Analysis
[44]
There is no dispute between the parties with
regard to the applicable standards of review. However, a few words in regard
thereto will be useful.
A.
Standard of Review
[45]
It is trite law that on an appeal from a
decision determining an application for judicial review, this Court must
determine whether the Judge selected and applied the correct standard of review
(Telfer v. Canada Revenue Agency, 2009 FCA 23, 386 N.R. 212 at
paragraph 19; Agraira v. Canada (Public Safety and Emergency Preparedness),
2013 SCC 36, [2013] 2 S.C.R. 559 at paragraphs 45 – 47). If the Judge erred
in either selecting or applying the correct standard of review, then it is for
this Court to examine the Minister’s decision in light of the correct standard.
[46]
The parties are in agreement that the first
prong of the Abbott test for patent listing eligibility was to be
decided by the Judge on a standard of correctness. On the second prong, I note
that our Court has taken different positions on the applicable standard of
review (compare Purdue, para. 13 which indicates reasonableness with Gilead
FCA, para. 11 which indicates correctness applies). However, given that there
is no dispute between the parties with respect to the second prong, I need not
resolve this question in this decision.
[47]
The third prong of the Abbott test, i.e.
whether the formulation claimed in the ‘329 Patent is the formulation found in Trifexis
in respect of which a NOC has been issued by the Minister, is subject to two
standards. Firstly, the interpretation of paragraph 4(2)(b) of the Regulations
must be reviewed on a standard of correctness. Secondly, the determination of
whether the formulation claimed in the ‘329 Patent is the formulation which has
been approved by the Minister through the issuance of a NOC stands to be
decided on a standard of reasonableness as it requires the application of
paragraph 4(2)(b) of the Regulations to the specific facts of the case (Abbott
FCA, paras. 26 – 34).
[48]
In my view, the Judge erred in respect of the
third prong. More particularly, she misunderstood the requirements of paragraph
4(2)(b) of the Regulations which led her to misapply the Regulations to
the specific facts before her.
B.
Legislative Test
[49]
Paragraph 4(2)(b) of the Regulations
provides that a patent is eligible for listing on the Register if it claims a
formulation of medicinal ingredients which has been approved by the Minister by
reason of the issuance of a NOC.
[50]
The purpose of the Abbott test is to set
out the questions which the Court must resolve in order to determine if the
requirements of subsection 4(2) have been met. The Judge clearly understood the
relevant test as it appears at paragraph 16 of the Federal Court Decision
(quoted at paragraph 24 of these reasons).
C.
First Prong of the Abbott Test
[51]
As noted above, at the first step of the test, the
Judge determined what formulation the ‘329 Patent claimed. In other words, did the
formulation claimed in the Patent contain both spinosad and milbemycin oxime? As
I have already indicated, the Judge disagreed with the Minister’s finding that
the formulation claimed in the ‘329 Patent claimed spinosad only. Her rationale
for disagreeing with the Minister is as follows.
[52]
First, she correctly instructed herself with
regard to the governing principles of claim construction, i.e. that a patent is
to be construed through the eyes of the person skilled in the art having a mind
willing to understand the invention, that the construction of the patent’s
claims must be approached in a purposive manner and that the patent had to be
construed in light of both the disclosure and of the claims (as per Free
World and Whirlpool).
[53]
She clearly understood that she could count on
the assistance of the expert witnesses who had given evidence before her in
order to arrive at the proper construction of the ‘329 Patent. However, she
noted that it was her responsibility, not that of the experts, to reach a
conclusion with regard to what was properly claimed by the Patent (Bell
Helicopter Textron Canada Limitée v. Eurocopter, société par actions
simplifiée, 2013 FCA 219, 449 N.R. 111. The Judge also understood that claim
construction in the context of eligibility assessment under subsection 4(2) of
the Regulations is subject to the principles enunciated in Free World and
Whirlpool (Purdue, para. 17).
[54]
She then turned to the expert evidence before
her so as to determine how the person skilled in the art would understand the
formulations claimed by the ‘329 Patent. More particularly, the crucial
question was whether a person skilled in the art would understand the
formulation to contain both spinosad and milbemycin oxime. In answer to this
question, she noted that milbemycin oxime was a member of the family of
milbemycins, coming to that view primarily on the basis of Dr. Paradis’ opinion.
The Judge also noted that Mr. Jubran, the Minister’s representative, had
conceded that point during his testimony and that the Minister’s Decision was
also reflective of that view.
[55]
The Judge then turned to the real question at
issue which she formulated as follows (Federal Court Decision, para. 63):
What is in contention is whether a
definition in the descriptive portion of the patent of “oral formulation” would
be understood by a person skilled in the art to include a formulation
comprising both spinosad and milbemycin oxime.
[56]
To answer that question the Judge turned to Dr.
Paradis’ affidavit and more particularly to paragraph 44 thereof where Dr.
Paradis opined that although only spinosad was specifically referred to in the
‘329 Patent, there was also clear reference to milbemycin oxime in the claims
because the Patent defined “oral formulation” as
including milbemycin oxime and also because the term “comprising”,
found in the claims, meant that the inventors contemplated that spinosad would
be formulated with one or more active ingredients.
[57]
The Judge clearly understood that Dr. Paradis’
opinion was based on her view that the words milbemycin oxime and milbemycins
were, in context, interchangeable when reading the ‘329 Patent. Dr. Paradis’
evidence led the Judge to say that the parties were in agreement that milbemycin
oxime was a compound that was included in the class of compounds described as
milbemycins and that a person skilled in the art would have had that
understanding at the time of the publication of the ‘329 Patent (Federal Court
Decision, para. 68).
[58]
As a result, the Judge held that the ‘329 Patent
claimed a formulation which included both spinosad and milbemycin oxime. The
Judge therefore found that the Minister had been “too
restrictive” in her interpretation of the ‘329 Patent and had thus erred
(Federal Court Decision, para. 71).
[59]
Before this Court, the Minister disagrees with
the Judge’s conclusions on this issue. While the Minister acknowledges that
claims construction is a question of law for the Judge to decide and that the
Judge could rely on expert evidence for assistance with regard to technical
terms and the scientific background to a patent, she argues that the Judge was
not required to rely on the expert evidence to construe the claims of the ‘329
Patent (citing Pfizer Canada Inc. v. Canada (Health), 2007 FC
446, [2008] 1 F.C.R. 672, para. 35).
[60]
In the Minister’s view, two factors show that
her view of the Patent was correct. First, the fact that none of the ‘329
Patent’s claims specify milbemycin oxime as a second medicinal ingredient
present in the formulation of the invention. Second, the insufficiency of the mere
mention of milbemycins in the disclosure as one of the many groups of compounds
that may be combined with spinosad to constitute a claim for the formulation
containing the medicinal ingredients of Trifexis.
[61]
The Minister then explains why her construction
of the ‘329 Patent is correct. Specifically, she notes that her construction
was conducted prior to and separate from the exercise required by the third
prong of the Abbott test. She adds that she was under no obligation to
call expert evidence to support her construction.
[62]
The Minister then argues that the Judge erred in
finding that the person skilled in the art would understand that reference to
milbemycins would include milbemycin oxime. In support of that proposition, the
Minister says that the class of milbemycins is not a medicinal ingredient, but
rather a group of compounds, any of which could possibly be combined with
spinosad, the medicinal ingredient specified in the Patent’s claims.
[63]
Thus, according to the Minister, it follows that
a person skilled in the art would not conclude that a reference to milbemycins
was a reference to milbemycin oxime “if the only clue
to the choice of milbemycin oxime for the formulation was the reference to the
entire class of milbemycins” (Minister’s Memorandum of Fact and Law, para.
33).
[64]
In summary, the Minister says that no guesswork
is allowed in pharmaceutical science. Consequently, when the ‘329 Patent is
properly construed, the only possible conclusion is that the only medicinal
ingredient claimed in the formulation claimed by the ‘329 Patent is spinosad. To
conclude that the formulation also contains milbemycin oxime necessarily
requires a stretch of the imagination for any person skilled in the art.
[65]
I cannot agree with the Minister that the Judge
either erred in law or made a palpable and overriding error in her construction
of the ‘329 Patent’s claims. The Judge’s construction of the ‘329 Patent was based
on her reading and understanding of the Patent in the light of the expert
evidence adduced before her and more particularly the evidence of Dr. Paradis.
[66]
The Minister does not directly challenge the
evidence of Dr. Paradis nor criticize the Judge for relying on it with regard to
the question of whether the person skilled in the art would conclude that
reference to milbemycins was also a reference to milbemycin oxime. While there
is no doubt that the Minister did not have to present expert evidence to
support her construction of the Patent, she did have to demonstrate that the
Judge erred in construing the Patent in the manner that she did. In effect, by
not challenging Dr. Paradis’ evidence or the Judge’s reliance upon it, the
Minister has not made any serious attempt to demonstrate that the Judge so-erred.
[67]
I therefore conclude that there is no basis for
us to interfere with the Judge’s analysis of the first step of the Abbott test.
D.
Second Prong of the Abbott Test
[68]
As I have already indicated, there is no issue
between the parties regarding the second step of the Abbott test as both
sides agree that NDS 141 509 sought the approval of an oral dosage form of two
specified active ingredients, spinosad and milbemycin oxime.
E.
Third Prong of the Abbott Test
[69]
The third prong of the Abbott test
required the Judge to determine whether the formulation claimed by the Patent
was that which was authorized by the Minister when she issued a NOC for Trifexis.
[70]
Having concluded that the ‘329 Patent claimed a
formulation of both spinosad and milbemycin oxime, one would have expected the
Judge to conclude that the ‘329 Patent was eligible for listing on the Register.
After all, the Patent, as construed by the Judge, claims, in the words of
paragraph 4(2)(b) of the Regulations, “the
formulation that contains the medicinal ingredient and the formulation has been
approved through the issuance of a notice of compliance in respect of the submission”.
However, as noted above, the Judge did not arrive at this conclusion. Rather,
she concluded that the ‘329 Patent was ineligible for listing on the Register.
The question, therefore, is what led her to this conclusion. To answer this
question requires a deeper examination of the Judge’s consideration of the
third prong of the Abbott test.
[71]
The Judge began her examination of the third
prong by stating the view, which no one disputes, that the claimed formulation
in the ‘329 Patent must include the two medicinal ingredients found in
Trifexis. This view finds support in all of the leading cases on the question and
is in accordance with paragraph 4(2)(b) of the Regulations.
[72]
After a discussion of the 2006 amendments to the
Regulations which, in effect, require a match between the formulation claimed
by the ‘329 Patent and the NOC-authorized drug product, the Judge said that she
was bound by this Court’s interpretation of subsection 4(2) of the Regulations
and more particularly by our decision in Gilead FCA.
[73]
The Judge then reviewed, in turn, Purdue,
Gilead FCA and Searle and concluded that the Minister had
correctly interpreted paragraph 4(2)(b) of the Regulations. In my view, if
the Minister’s construction of the ‘329 Patent was correct, then there can be
no doubt that her interpretation of paragraph 4(2)(b) of the Regulations
would have also been correct. The Minister concluded that the formulation
claimed by the ‘329 Patent did not contain milbemycin oxime, and therefore correctly
concluded that there was no match between the claims of the ‘329 Patent and the
NOC-approved drug. The Minister’s conclusion and logic, based upon her
construction of the ‘329 Patent, are unimpeachable.
[74]
However, the real issue in this appeal arises from
the fact that the Judge overturned the Minister’s construction of the ‘329
Patent, but nonetheless concluded that the Minister correctly refused to list
the ‘329 Patent on the Register.
[75]
First of all, there is no difficulty in
understanding what paragraph 4(2)(b) of the Regulations requires. Indeed,
the Judge herself seems to have understood what this paragraph requires when
she formulated the Abbott test insofar as it applied to the case before
her.
[76]
The Abbott test simply requires the Judge
to determine whether the formulation claimed by the patent at issue is the one
in respect of which the Minister has issued a NOC. Having understood, at least
initially, the meaning of paragraph 4(2)(b), the Judge then appears to
have resiled from that understanding of the provision when she dealt with the
third prong of the test. In my respectful view, this happened because she
misunderstood our decisions on the issue and more particularly our decision in Gilead
FCA.
[77]
In Gilead, both before the Federal Court
and this Court, the issue was whether the appellant’s ‘475 Patent was eligible
for listing against its NOC-approved drug product Complera. On the basis of the
Abbott test, Mosley J. of the Federal Court had to determine if the
Minister correctly refused to list the ‘475 Patent on the Register. In the
Minister’s view, the ‘475 Patent did not contain a claim for the three
medicinal ingredients found in Complera, namely tenofovir disoproxil fumarate
(“tenofovir”), emtricitabine, and rilpivirine. Thus, the Minister concluded
there was no match between what the ‘475 Patent claimed and Complera and
refused to list it on the Register (Gilead FC, paras. 7-9).
[78]
Before Mosley J., there was no dispute between
the parties with regard to the second prong of the test, i.e. that Complera
contained three medicinal ingredients, tenofovir, emtricitabine and
rilpivirine. The parties also agreed that rilpivirine was within a class of
agents known as non-nucleoside reverse transcriptase inhibitors (NNRTIs) and
that this class was referenced in the ‘475 Patent (Gilead FC, para. 10).
[79]
With regard to the first prong of the Abbott test,
Mosley J. held that the ‘475 Patent did not claim rilpivirine. More
particularly, he said that (Gilead FC, para. 26):
I construe the relevant claims of the ‘475
Patent as combinations and formulations of two medicinal ingredients plus a
third one of the NNRTI class that could possibly include but is not
specifically rilpivirine.
[Emphasis added]
[80]
Further, Mosley J. also stated (Gilead FC,
para. 46):
There is nothing in the ‘475 Patent that
points specifically to rilpivirine as the third ingredient in the class of
NNRTIs. As the evidence of Dr. Miller on behalf of the applicant states,
several other NNRTI’s had been studied for their efficacy in treating HIV prior
to the grant of the patent. References to an NNRTI in the patent are not to a
specific medicinal ingredient but rather to the class of compounds, one or more
of which may have been found to be suitable to be included in a formulation
with tenofovir and emtricitabine. The claims that specify such a formulation
are not specific to the drug in the Complera NDS.
[81]
Having concluded that the ‘475 Patent did not
claim rilpivirine as a medicinal ingredient, Mosley J. proceeded to the third
prong of the test and determined that the ‘475 Patent did not meet the strict
product specificity required by paragraph 4(2)(b) of the Regulations. He
went on to say that the ‘475 Patent “did not meet the
specifics of the NDS” (Gilead FC, para. 49). Hence, the Judge
concluded that the Minister’s decision to refuse to list the ‘475 Patent on the
Register was reasonable.
[82]
This Court dismissed the appeal for different reasons
than those of Mosley J. in Gilead FC. More particularly, our Court was
of the view that the claims of the ‘475 Patent pertained to a new combination
of medicinal ingredients and hence that its eligibility for listing had to be
determined on the basis of paragraph 4(2)(a), rather than 4(2)(b),
of the Regulations (Gilead FCA, para. 3).
[83]
After reviewing the relevant facts and the
applicable standard of review, Trudel J.A. turned to the construction of the
‘475 Patent. More particularly, she reproduced paragraph 26 of Gilead FC where
Mosley J.’s construction of the ‘475 Patent appears (Gilead FCA, para.
19). She then indicated that the parties did not take issue with this construction
of the ‘475 Patent’s claims and that, as a result, the only question in dispute
concerned the Minister and Mosley J.’s interpretation of paragraphs 4(2)(a)
and (b) of the Regulations and their application to the relevant facts (Gilead
FCA, para. 20).
[84]
After a brief explanation of the regulatory
framework, Trudel J.A. turned to the meaning of paragraphs 4(2)(a) and (b)
of the Regulations and concluded that the ‘475 Patent fell under paragraph
4(2)(a) and not 4(2)(b). My colleague then dealt with the product
specificity requirement of the Regulations (beginning at Gilead FCA,
para. 33). She first indicated that the parties were agreed that the Regulations
made product specificity between the claims of the patent at issue and the NOC-approved
drug a requirement for the listing of a patent on the Register. She then
reviewed our decision in Purdue and adopted Layden-Stevenson J.A.’s
comment reproduced below (Purdue, para. 44):
In my view, the requirement for this level
of specificity is consistent with the text, the object and the purpose of the
Regulations. It is also consistent with the interpretation of the other classes
of claims in section 4 of the Regulations as determined by the jurisprudence of
this Court.
[85]
This led Trudel J.A. to say that there was no
basis to adopt different legislative requirements for the various paragraphs of
subsection 4(2). She further added that the product specificity requirement of
the Regulations “sets a high threshold of consistency”
and that the three medicinal ingredients, “i.e.
tenofovir, emtricitabine and rilpivirine must be set out in the patent claims
and the NOC for the patent to be eligible on the register” (Gilead
FCA, paras. 39-40).
[86]
My colleague further said that “the wording of section 4 is consistent across the four
subsections and requires a high degree of specificity between the wording of
the claim and the NOC” adding that “[i]t would
be necessary to read an interpretation into paragraph 4(2)(a) to allow
the paragraph to support claims which contain only some of the medicinal
ingredients” (Gilead FCA, para. 45). In her view, such an
interpretation flew in the face of the ordinary meaning of the words found in
the subsection, the purpose and object of the Regulations and the government’s
position that product specificity was a key consideration in interpreting
subsection 4(2).
[87]
Trudel J.A. then noted Mosley J.’s conclusion
that the ‘475 Patent’s claims did not meet the requirement for product
specificity of the Regulations in that its claims “do
not make specific reference to the medicinal ingredient rilpirivine (sic), but
only the broad class of compounds” (Gilead FCA, para. 49).
[88]
In my view, this examination of the facts and
holdings in Gilead FC and Gilead FCA distinguishes these
decisions from the present appeal. It is clear from Gilead FCA that Trudel
J.A. accepted Mosley J.’s construction of the ‘475 Patent to the effect that it
did not claim rilpivirine. In other words, contrary to the matter before
us in this appeal, the patent at issue in Gilead FC and Gilead FCA did
not claim the three medicinal ingredients found in the NOC-approved drug
product Complera. In the present appeal, the Judge specifically found that the formulation
claimed by the ‘329 Patent was the formulation found in Trifexis, i.e. a
formulation which contained both spinosad and milbemycin oxime.
[89]
Consequently, when one answers the questions posed
by the Abbott test in this case, the answers are:
- What
formulation does the Patent claim?
The Patent claims a formulation containing
spinosad and milbemycin oxime.
- What is the
formulation of the NOC issued for the drug in question?
A formulation containing spinosad and
milbemycin oxime.
- Is the
formulation claimed by the Patent that which was authorized by the NOC?
Yes it is.
[90]
The Judge concluded that the formulation claimed
by the Patent was not the one which the NOC authorized. As I indicated earlier,
the Judge concluded as she did because she misinterpreted our decision in Gilead
FCA. More particularly, the Judge appears to have understood Gilead FCA
to require her to find the words milbemycin oxime in the ‘329 Patent’s claims
and that, failing the appearance of those words, the ‘329 Patent did not claim
the formulation which had been approved by the issuance of the NOC and could
not be listed.
[91]
In expressing her view of the matter, the Judge
emphasized the fact that in Gilead FCA, this Court endorsed Mosley J.’s
reasoning pertaining to the product specificity requirement. In particular, she
drew attention to Mosley J.’s conclusion that a patent could not meet the
product specificity requirement if it referred to a class of compounds rather
than to a specific medicinal ingredient and that the ‘475 Patent failed this
requirement because it claimed the class of NNRTIs rather than rilpivirine
specifically (see Federal Court Decision, para. 82).
[92]
Again, it is important to point out that Mosley
J. actually found in Gilead FC that the third medicinal ingredient,
rilpivirine, was not claimed by the ‘475 Patent. Consequently, in my opinion,
based upon that premise, Mosley J. was correct to find that there was no match
between the ‘475 Patent’s claims and the NOC-approved drug.
[93]
I acknowledge that certain statements in Gilead
FCA arguably led the Judge astray in this regard. For example, Trudel J.A. stated
that the medicinal ingredients found in Complera “must
be set out in the patent claims and the NOC for the patent to be eligible on
the register” and that subsection 4(2) “requires
a high degree of specificity between the wording of the claim and the NOC”
(Gilead FCA, paras. 40 and 45). However, in my respectful opinion, these
statements cannot be understood to have changed the requirements of the Abbott
test. On the contrary, our Court has consistently and repeatedly affirmed
the Abbott test.
[94]
In other words, I do not understand our decision
in Gilead FCA as an abandonment of the Abbott test or the
principles of claim construction enunciated by the Supreme Court in Free
World and Whirlpool. Thus, contrary to what the Judge understood
from Gilead FCA, the question at the third step of the Abbott test
is not whether the words milbemycin oxime appear in the claims of the ‘329
Patent, but whether the claims of the ‘329 Patent claim milbemycin oxime as a
medicinal ingredient in the formulation set out in the Patent.
[95]
The concept of product specificity must be
understood in the context of the 2006 amendments to the Regulations. On this
point, it is worth reproducing paragraph 43 of Gilead FCA in full where Trudel
J.A. elaborated upon the notion of product specificity:
The 2006 revisions also clearly introduced
the requirement for product specificity. A plain reading of the version in
force prior to the 2006 revisions establishes that if the patent claims were
shown to be “relevant to” the approved drug, the submitted patents were
generally accepted for listing. In contrast, the revised version introduces a
requirement for more detailed information on the product against which the
patent is to be listed, including the medicinal ingredient, the brand name, the
dosage form, the strength, the route of administration and the use as set out
in the NDS. In addition, the categories set out in section 4 are now more
detailed and precisely defined. These changes, combined with the greater
emphasis on meeting eligibility criteria and being subject to the Minister’s
determination as noted above, lead to a clear rejection of Gilead’s argument for
a wide scope of connection between the patent claims and the NOC.
[96]
Thus, in order to have a patent listed on the Register
prior to the 2006 amendments, it was only necessary to demonstrate that the
patent claims were “relevant” to the NOC-approved
drug. The concept of relevance is a very broad concept and allowed the listing
of many patents which, following the 2006 amendments, would no longer be accepted.
Thus, the concept of product specificity, brought in by the 2006 amendments,
can only be understood by reference to what it sought to replace, i.e. the
concept of relevance. Innovators could still
list patents against their drug products but such patents would have to claim,
under paragraph 4(2)(b) of the Regulations, the very formulation
authorized by the Minister in the NOC issued for the drug product.
[97]
On my understanding of the Regulations prior to
the 2006 amendments, the ‘475 Patent at issue in Gilead FC and Gilead
FCA would have, in all likelihood, been accepted for listing on the Register
by the Minister because it would have been demonstrated that the patent at
issue was “relevant” to Complera even though the
third medicinal ingredient rilpivirine was not claimed by the ‘475 Patent.
However, under the amended Regulations, relevancy is no longer sufficient to
allow the listing of a patent. In effect, it must now be shown that the patent
which the innovator seeks to list on the Register contains, as per paragraph
4(2)(b), a formulation of certain medicinal ingredients which the
Minister has approved through the issuance of a NOC. In other words, the patent
must claim specifically the formulation which the Minister has approved through
the issuance of a NOC.
[98]
Thus, in the circumstances of this case, it is
clear that the third prong of the Abbott test has been met. In short, the
‘329 Patent claims a formulation of two medicinal ingredients, spinosad and
milbemycin oxime. The Minister has approved of this formulation through the
issuance of a NOC for Trifexis.
VI.
Conclusion
[99]
For these reasons, I would therefore allow the
appeal with costs, I would set aside the Federal Court Decision dated February 17,
2014, and rendering the judgement which ought to have been made, I would allow
the Appellant’s judicial review application with costs and return the matter to
the Minister for reconsideration in the light of these reasons.
“M Nadon”
“I agree.
Richard Boivin J.A.”
DAWSON
J.A. (Concurring Reasons)
[100] I agree with Justice Nadon that this appeal should be allowed with
costs. For the reasons given by him, I agree that the Judge construed the 329
patent to claim not only spinosad as the active ingredient but also
formulations that contain other active ingredients, including a formulation
that contains both spinosad and milbemycin oxime. For the reasons given by Justice Nadon,
I also agree that the Judge erred in respect of the third prong of the test
articulated in Abbott Laboratories Ltd. v. Canada (Attorney General),
2008 FCA 354, [2009] 3 F.C.R. 547. The single point of divergence I have with
my colleague’s reasons is that I am unable to distinguish the decision of our
Court in Gilead Sciences Canada Inc. v. Canada (Minister of Health),
2012 FCA 254, 435 N.R. 188. As I am unable to distinguish Gilead, and as
I agree with my colleague’s analysis on the merits of this appeal, I
respectfully conclude that Gilead was wrongly decided. I reach this
conclusion on the following basis.
[101] The patent in issue in Gilead (475 patent) claimed
combinations and formulations of two or more anti-viral agents. The Federal
Court construed the relevant claims of the patent as combinations and
formulations of two medicinal ingredients (including tenofovir and
emtricitabine) plus a third anti-viral agent from the class of non-nucleoside
reverse transcriptase inhibitors (NNRTIs). The parties agreed that the drug in
issue, Complera, contained three medicinal ingredients: tenofovir,
emtricitabine and rilpivirine. They also agreed that rilpivirine was a member
of the class of NNRTIs. The issue was whether the 475 patent could be listed
because it did not specifically name rilpivirine as a medicinal ingredient.
[102] The Federal Court and this Court concluded that the 475 patent could
not be listed because it did not explicitly name rilpivirine as a medicinal
ingredient and so there was no match between the subject matter of the patent
and the formulation approved in the notice of compliance.
[103] However, given the construction of the 475 patent by the Federal
Court, and given the agreement of the parties that Complera contained
tenofovir, emtricitabine and rilpivirine, and that rilpivirine was a member of
the class of NNRTIs, without doubt the 475 patent claimed the combination and
formulation of tenofovir, emtricitabine and rilpivirine; any manufacture or
sale of that formulation would infringe the 475 patent. Notwithstanding that
the 475 patent claimed this formulation and the notice of compliance approved
tablets formulated with tenofovir, emtricitabine and rilpivirine as medicinal
ingredients, the 475 patent was found to be ineligible for listing.
[104] This result is not consistent with the result in the present appeal
where the 329 patent is found to be eligible for listing because it claims the
formulation approved in the notice of compliance issued in respect of Trifexis.
[105] In my view, the result in the present appeal is correct because it
accords with the text, context and purpose of paragraphs 4(2)(a) and (b)
of the Patented Medicines (Notice of Compliance) Regulations, SOR/93-133
(Regulations).
[106] Paragraphs 4(2)(a) and (b) (set out at paragraph 19 of
my colleague’s reasons) provide that a patent is eligible for listing if it
contains “a claim for the medicinal ingredient”
or “a claim for the formulation”
(emphasis added) and the medicinal ingredient or formulation has been approved
through the issuance of a notice of compliance. A textual reading of the
provisions therefore requires inquiry into what the patent in issue claims.
[107] Patent claims are analogized to “fences”
and “boundaries” (Free World Trust v. Electro
Santé Inc., 2000 SCC 66, [2000] 2 S.C.R. 1024, at paragraph 14. In this
context, the inquiry required by paragraphs 4(2)(a) and (b) of
the Regulations into the claims of the patent supports the interpretation that
it is not necessary to require a patent to specifically name every medicinal
ingredient approved through the issuance of a notice of compliance. If the
patent claims the approved medical ingredient there will be a sufficient nexus
between the patent and the subject of the notice of compliance to allow the
patent to be listed.
[108] The purpose of the Regulations is to regulate the early working
exception under the Patent Act, R.S.C. 1985, c. P-4 and to balance
patent protection with the early entry of generic drugs. This purpose is not
served by denying listing to a patent when the patent claims an innovative and
useful medicinal ingredient or formulation and that same medicinal ingredient
or formulation has been approved for use through the issuance of a notice of
compliance.
“Eleanor R. Dawson”
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