Date: 20070111
Docket: T-1847-03
Citation: 2006 FC 1558
BETWEEN:
ABBOTT LABORATORIES and ABBOTT
LABORATORIES LIMITED
Applicants
and
THE MINISTER OF HEALTH
and APOTEX INC.
Respondents
PUBLIC REASONS FOR ORDER
(Confidential Reasons Issued December 29,
2006)
HENEGHAN,
J.
I. Introduction
[1]
Abbott
Laboratories and Abbott Laboratories Limited (the “Applicants” or “Abbott”)
bring this application pursuant to the Patented Medicines (Notice of
Compliance) Regulations, SOR/193-133 (the “NOC Regulations) for an order
prohibiting the Minister of Health from issuing a Notice of Compliance (“NOC”)
pursuant to section C.08.004 of the Food and Drug Regulations, C.R.C.,
c. 870 until the expiry of the following Canadian letters patent:
2,261,732 (the “ ’732 Patent”);
2,258,606 ( the “ ’606 Patent”);
2,386,527 (the “ ’527 Patent”);
2,386,534 (the “ ’534 Patent”);
2,277,274 (the “ ’274 Patent”);
2,387,361 (the “ ’361 Patent”); and
2,387, 356 (the “ ’356 Patent”)
(collectively the “Abbott Patents”).
[2]
This
application arose in response to the Notice of Allegation (“NOA”), dated August
21, 2003, served by Apotex Inc. (the “Respondent” or “Apotex”). Apotex alleges
that the Abbott Patents are invalid on several grounds including anticipation,
obviousness, lack of utility, lack of sound prediction and further, that its
generic version of clarithromycin will not infringe the Abbott Patents that are
valid.
[3]
On
October 7, 2003, the Applicants commenced this proceeding by filing an
application, pursuant to the NOC Regulations and stated in their Notice of
Application that the allegations were not justified.
II. The Parties
[4]
The
Applicant Abbott Laboratories Limited is a Canadian company that distributes
and sells, inter alia, BIAXIN® BID (“BIAXIN”), an antibiotic. The
Applicant Abbott Laboratories, a company incorporated under the laws of the United
States of America, is the parent of Abbott Laboratories Limited. It is the
owner of the patents at issue in this proceeding. The Applicants are engaged in
the development and manufacture of innovative pharmaceutical products.
[5]
Apotex
is a Canadian corporation that manufactures generic products. It has applied
for an NOC to allow it to market its version of clarithromycin, to be sold in
tablets of 250 mg and 500 mg.
III. Clarithromycin
[6]
Clarithromycin,
or 6-0-methylerythromycin, is an antibiotic. It fights infections in the human
body and is described in the Abbott Patents as being useful for treating
respiratory tract infections. It is the active ingredient in the Applicants’ BIAXIN
product, which is sold in dosages of 250 and 500 mg.
[7]
The
clarithromycin molecule can take a number of crystalline forms, depending on
the manner of manufacture. There are at least seven pure forms and innumerable
combinations may be made of these forms and other substances.
[8]
Clarithromycin
was first disclosed on December 9, 1981 in European Patent Application No. 0
041 355 A1. It was first marketed in Canada in July 1992.
[9]
The
Applicants did not invent clarithromycin itself but they invented some of the crystalline
forms of the drug. Initially, it was thought that clarithromycin had only one
crystal form but it was later discovered that it was polymorphic, that is having
more than one crystalline form. Abbott claims to have discovered these new
forms which are the basis for the patents here in issue.
[10]
The
Abbott Patents cover clarithromycin compounds, processes and methods for their manufacture,
and the use of the claimed compounds as an antibiotic. Specifically, the claims
cover the crystalline forms called Form 0, Form I and Form II, and the use of
Form 0 to make Form II.
[11]
The
conversion of one clarithromycin form to another involves the heating of the
substance at high temperatures. Abbott takes the position that heating at high
temperatures was not common knowledge and constitutes the inventive step.
Apotex says that heating at high temperatures was known to persons skilled in
the art and did not amount to an invention.
[12]
Apotex’s
intended generic form of clarithromycin uses Form 0 to produce Form II. Apotex
proposes to sell its version in 250 and 500 mg dosage forms, using methods of
manufacture that it says are disclosed in the prior art.
IV. The Patents
[13]
The
Applicants hold seven Canadian patents related to clarithromycin, as listed
above and the NOA was served against those Patents. However, the Applicants
addressed only four patents in their memorandum of fact and law, that is the
’274, ’732, ’606 and ’361.
[14]
At
the commencement of the hearing on September 11, 2000, counsel for the
Applicants advised that an agreement had been reached with the Respondent that,
for the purpose of the present proceeding and only this proceeding, the
Applicants will not obtain a prohibition order in relation to the ’274 Patent
as a result of the decision of the Federal Court of Appeal in Abbott
Laboratories v. Canada (Minister of Health) (2006), 350 N.R. 242
(“Ratiopharm”), application for leave to appeal to the Supreme Court of Canada filed
August 17, 2006. At the close of the hearing of this application counsel
submitted a copy of this agreement respecting the ’274 Patent. This agreement
provides as follows:
Both parties have agreed to proceed with
this hearing on the basis that neither party will make arguments in respect of
the ’274 Patent.
Abbott has acknowledged that, because of
the facts of this particular case, the Court of Appeal’s judgment in the
ratiopharm case in respect of the ’274 Patent is binding and as such, Apotex’s
allegation of anticipation in respect of the ’274 Patent must be held to be
justified in this Court.
The parties have agreed that the above
mentioned agreement is without prejudice to either party advancing any position
that it wishes at the Court of Appeal, should an appeal be pursued.
[15]
In
light of this agreement between the parties, it is not necessary for me to
address the ’274 Patent. I acknowledge that Abbott has not abandoned its
arguments in respect of the ’274 Patent but the consideration of those
arguments will occur elsewhere, if at all. The matter proceeded only in
relation to the ’732 Patent, the ’606 Patent and the ’361 Patent.
A. Canadian Patent No. 2,261,732 (The “
’732 Patent”)
[16]
The
’732 Patent is entitled “Preparation of Crystal Form II of Clarithromycin”. The
invention in this patent is described as “a process for the direct isolation of
6-0-methylerythromycin A crystal Form II”. Claims 1 through 15 set out methods
and processes by which Form II may be formed; the resulting preparations of
Form II are covered in claims 16 to 21.
[17]
The
’732 Patent was filed in the Canadian Patent Office on July 28, 1997, with
priority dates of July 29, 1996 and July 25, 1987. This patent claimed priority
from U.S. Patent application numbers 08/681,695 and 08/900,271 respectively.
The ’732 Patent was granted on July 24, 2001.
B. Canadian Patent No. 2,258,606 (The “
’606 Patent”)
[18]
The
’606 Patent is entitled “Crystal Form II of Clarithromycin”. It relates to an
invention for “6-0-methylerythromycin A crystal Forms I and II, a process for
their preparation, pharmaceutical compositions comprising these compounds and
methods of use as a therapeutic agent”. Claims 1 through 4 cover Forms I and
II, having differing values in the powder x-ray diffraction patterns.
[19]
The
’606 Patent application was filed in the Canadian Patent Office on July 25,
1997, with a priority date of July 29, 1996 with respect to U.S. patent
application 08/681,723. This patent was granted on May 27, 2003.
[20]
The
claims of the ’606 Patent relevant to this application are as follows:
• Claims
one (1) and two (2) relate to two forms of 6-0-methylerythromycin A Form II,
which are characterized by peaks in the powder x-ray diffraction pattern having
particular 2θ values.
• Claims
three (3) and four (4) relate to two forms of 6-0-methylerythromycin A Form II,
which are substantially free of 6-0-methylerythromycin A Form I, and are
characterized by peaks in the powder x-ray diffraction pattern having
particular 2θ values.
C. Canadian Patent No. 2,387,361 (The “
’361 Patent”)
[21]
The
’361 Patent is entitled “Crystal Form 0 and Form II of Clarithromycin and Uses
Thereof”. Patent protection is claimed over “the novel compound
6-0-methylerythromycin A crystal form 0 solvate, a process for its preparation,
pharmaceutical compositions comprising this compound and a method of use as a
therapeutic agent”. Forms and compositions of the drug appear in claims 15 to
23 and 42 to 50. Uses are covered in claims 8 to 14, 24 to 41, and 51 to 68,
while the processes appear in claims 1 to 7.
[22]
An
application was submitted to the Canadian Patent Office on December 19, 1997.
Priority was claimed to January 17, 1997 in accordance with U.S. patent application
number 08/785,623. The 361 Patent was granted on May 27, 2003.
[23]
The
claims of the ’361 Patent relevant to this application are as follows:
• Claim
one (1) relates to a process for preparing 6-0-methylerythromycin A Form II
which involves the heating of 6-0-methylerythromycin A Form 0 solvate under
vacuum at a temperature between approximately seventy and one hundred and ten
degrees Celsius.
• Claim
thirty-one (31) relates to the use of 6-0-methylerythromycin A Form 0
ethanolate in the preparation of 6-0-methylerythromycin A Form II for use as an
antibiotic.
• Claim
sixty-two (62) relates to the use of 6-0-methylerythromycin A Form 0
ethanolate, substantially free of 6-0-methylerythromycin A Form I, in the
preparation of 6-0-methylerythromycin A Form II, substantially free of
6-0-methylerythromycin A Form I and 6-0-methylerythromycin A Form 0 ethanolate,
wherein the Form 0 ethanolate and Form II are characterized by peaks in the
powder x-ray diffraction pattern having particular 2θ values.
V. The NOA
[24]
By
letter dated August 21, 2003, Apotex served its NOA upon the Applicants,
pursuant to subsection 5(3) of the NOC Regulations, respecting its generic clarithromycin.
The NOA was lengthy, consisting of one hundred and four pages, together with
appendices. The NOA raised allegations of invalidity and the ineligibility of
certain claims for inclusion on the Patent Register. It also alleged that
Apotex would not infringe the Abbott Patents because its product will be
prepared in accordance with methods disclosed in the prior art.
[25]
In
its NOA, Apotex claims that the commercially available and viable form of
clarithromycin has always been Form II, ever since the claim date of the
relevant patents, that is July 29, 1996.
[26]
Apotex
says that its proposed tablets would be comprised only of Form II and would use
methods of manufacture that it says are disclosed in the prior art. It claims
that the Applicants’ patents would not be infringed since a valid patent cannot
be infringed if the impugned activity is old or a non-patentable version
thereof. In this regard, the Respondent relies on Gillette Safety Razor Co.
v. Anglo American Trading Co. Ltd. (1913), 30 R.P.C. 465 at 480-481 (H.L.)
(the “Gillette Defence”).
[27]
As
well as these broadly-framed allegations, the NOA addressed non-infringement of
the individual patents, with the exception of the ‘606 Patent. In each case, it
was asserted that Apotex could produce its generic version of clarithromycin
without infringing the Applicants’ patents.
[28]
Allegations
of invalidity were advanced with respect to all of the Applicants’ patents.
These allegations were based upon claims of double patenting, obviousness, lack
of invention,
anticipation, patent claims being broader
than the invention made, and the amendment of specifications to describe matter
which could not reasonably be inferred from the original claim.
[29]
Apotex
further alleged that the Applicants’ patents are not and were never eligible
for a listing on the Patent Register, in compliance with the NOC Regulations.
Paragraph 4(2)(b) of the NOC Regulations sets out the criteria for inclusion of
a patent on the Patent Register, that is a claim for the medicine itself or a
claim for the use of the medicine. Apotex alleged that none of the Abbott
Patents contain valid claims for medicines or claim for use of a medicine.
[30]
As
well, Apotex argues that the patents are ineligible for registration on the
Register since none of them have filing dates that precede the date of filing
of the original NOC submissions.
VI. The Evidence
[31]
Both
the Applicants and the Respondent filed affidavits from a number of factual and
expert witnesses. The qualifications of the experts are not contested, although
in some respects, each party challenged the value of the evidence provided.
i. Applicants’ Witnesses
[32]
Abbott
filed the affidavits of Mr. Daniel Artola, Ms. Sonia Atwell, Ms. Loretta del
Bosco, Mr. Kenneth Dillman, Dr. Michael Zaworotko, Dr. Leonard Chyall, Dr.
Allan Myerson, Dr. Stephen Bryn and Dr. Jerry Atwood.
[33]
Mr.
Artola, a lawyer with the law firm McCarthy Tétrault, counsel for the
Applicants in this matter, deposed about his efforts to obtain information
about the book entitled Analytical Profiles of Drug Substances and
Excipients published by Acadamia Press. A chapter in this book, consisting
of an article by I.I. Salem, was cited as prior art by the Respondent in its
NOA.
[34]
Ms.
Atwell is a law clerk with the law firm of McCarthy Tétrault. In her affidavit,
she set out some factual details concerning the Applicants’ medicine BIAXIN and
the receipt of the Respondent’s NOA in August 2003. Among the exhibits attached
to this affidavit are copies of the NOA and of the Notice of Application filed
by Abbott on October 7, 2003.
[35]
Ms.
del Bosco is the Director of Regulatory Affairs and Quality Assurance with
Abbott Canada. She
appended to her affidavit, as an exhibit, a copy of a paper that was presented
to a meeting of Chemical Engineers on November 5, 2002. In her affidavit, she
deposed that this paper related to experiments conducted in the ordinary course
of Abbott’s business.
[36]
Mr.
Kenneth Dillman is a laboratory technician with SCCI, Inc., an independent
laboratory that was retained by McCarthy Tétrault, counsel for the Applicants,
to perform powder x-ray diffraction (“PXRD”) analyses of solid material samples
that were provided to him and identified as SSCI#48844, sample no. 1765-01-01.
[37]
Dr.
Michael Zaworotko is Professor and Chair of the Department of Chemistry at the
University of South
Florida
in Tampa, Florida. He
considers himself to be an expert in the fields of x-ray crystallography and
crystal engineering, “including how they relate to understanding form and
polymorphism in pharmaceuticals”. Dr. Zaworotko was asked to comment upon the
thesis prepared by G.A. Stephenson, entitled “Solid-state investigations of
selected pharmaceutical compounds” that was cited by the Respondent as prior
art in relation to the ’606 Patent.
[38]
Dr.
Leonard Chyall is a scientist employed by SCCI, Inc. He is an organic chemist
with experience in crystallization technology. He received a sample from Abbott
Laboratories and created a number of samples by recrystallization of
clarithromycin from ethanol. The sample was subsequently dried under a number
of different conditions, including drying at ambient temperature, at 40° Celsius,
under vacuum and with a vacuum aspirator. He conducted a reanalysis by PXRD of
the sample that was dried at 40° Celsius for 15 hours. He offers no opinion in
his affidavit but rather reports the results of the various experiments that he
conducted at the request of the Applicants.
[39]
In
the course of cross-examination upon his affidavit, Dr. Chyall said that he had
never dried anything above the temperature of 40° Celsius. He said that using a
higher temperature “…just strikes me off the top of my head as atypical and
unnecessary”.
[40]
Dr.
Allan Myerson, the Philip Danforth Armour Professor of Engineering, is Provost
and Senior Vice President at the Illinois Institute of Technology. He holds a
doctorate in chemical engineering and has taught at the university level for
nearly thirty years. He considers himself an expert in the fields of chemical
engineering and crystallization, including industrial crystallization and
polymorphism.
[41]
Dr.
Myerson was asked to consider the allegations of the NOA in relation to all of
the Abbott Patents. He expressed the opinion that all of the allegations of
invalidity and non-infringement were not justified. In his view, none of the
prior art references taught the existence of multiple crystal forms of
clarithromycin and neither did they “teach any method for producing any particular
form of clarithromycin”.
[42]
He
further expressed the view that none of the Abbott Patents are rendered obvious
by the prior art. According to him, the sale of BIAXIN prior to July, 1996 did
not anticipate the patents as it did not disclose the crystal forms of
clarithromycin and a person skilled in the art would have been unable to
ascertain it, if such form existed.
[43]
In
addition to his broad comments, Dr. Myerson addressed the individual patents.
With respect to the ’606 Patent, he rejected the Respondent’s argument that
European Patent Application 0 041 355 and the U.S. Patent No. 4,331,803 and EU
Patent spec. No. 0 041 355 B1, Apotex Document No. 1 disclose a method for
making Form II. Since no method is disclosed, he says that the allegation of
non-infringement is not justified.
[44]
He
concluded that the prior art cited by Apotex to establish anticipation does not
disclose the information necessary to produce the forms and methods claimed in
the ’606 Patent. None of the prior art reaches the drying temperatures required
to convert Form 0 or Form I to Form II.
[45]
Dr.
Myerson concluded that the Respondent’s proposed manufacturing process for its
clarithromycin tablets falls within the claims of the ’361 Patent and
consequently, infringe that patent. As well, he expressed the opinion that this
patent is neither anticipated nor obvious. In his view, a skilled person would
not infer from the prior art that Form II could exist in any form, still less
in multiple crystal forms. A skilled person would not infer that heating Form 0
or Form I at high temperatures could cause a conversion to Form II.
[46]
Dr.
Stephen Bryn is the Charles B. Jordan Professor of Medicinal Chemistry at the School of Pharmacy
and Pharmaceutical Sciences and the Head of the Department of Industrial and
Physical Pharmacy at Purdue University in Indiana. He holds a
Doctorate in physical and organic chemistry.
[47]
Dr.
Bryn addressed the allegations in respect of all the Abbott Patents. His
assessment of the prior art led him to conclude that, as of the claim dates of
the Abbott Patents, the prior art did not show that clarithromycin was polymorphic,
that is having more than one crystal form, the existence and crystal forms of
Forms 0, I and II, or methods for their manufacture. Further, in his opinion,
Abbott did not disclose its inventions by preparing BIAXIN for commercial sale
and there is no anticipation, obviousness or double patenting.
[48]
Dr.
Bryn discussed specific pieces of prior art. He stated that the Iwasaki article
discloses a methanol solvate structure that does not match anything claimed in
the Abbott Patents.
[49]
In
cross-examination, Dr. Bryn admitted that exposing a substance to high heat
could result in melting. However, he added that such treatment could also cause
the creation of amorphous material or degradation.
[50]
Dr.
Jerry Atwood is the Professor and Chairman of the Department of Chemistry at
the University of Missouri-Columbia. He holds a Doctorate in Chemistry and has
more than thirty years teaching experience at university levels. He considers
himself to be an expert in the fields of crystal growth, crystal engineering
and polymer chemistry.
[51]
Dr.
Atwood addressed the Respondent’s allegation that the NOC Regulations do not
apply to the Abbott Patents. He said that there was no basis for the
Respondent’s claim that Forms 0 and I are intermediates since the patents, as
illustrated by the ’527 and the ’274 Patents, clearly identify them as
antibiotics, and a person skilled in the art would recognize them as such.
Notwithstanding its instability, a person skilled in the art would know that
Form 0 is an antibiotic with therapeutic utility, not merely an intermediate.
Further, in his opinion, Form I is sufficiently stable to be used as a
medicine.
[52]
Dr.
Atwood also rejected the allegations respecting the ’361 Patent. He dismissed
the allegation that Apotex’s production of clarithromycin will not infringe
because it, Apotex, will not heat Form 0 under temperatures of between 70 and
100° Celsius. He observed that a person skilled in the art would know that the
temperature for conversion would fluctuate and that this would have no material
effect on the way the conversion process proceeded. Further, he concluded that
the amendments to the ’361 Patent were properly made.
[53]
According
to Dr. Atwood, the referenced prior art contained no information about
particular crystal forms of clarithromycin and methods of manufacture, in
particular that drying and heating clarithromycin could result in form
conversion.
[54]
In
cross-examination, Dr. Atwood admitted that in 1996, a person skilled in the
art would know how to analyse a pharmaceutical tablet in order to determine the
crystal form of its active pharmaceutical ingredient. That same person would
know how to separate crystals from a solvent. He disagreed with the proposition
that, in 1996, compounds were heated up to 150° Celsius in order to assess whether
a polymorphic transition would occur. However, he did agree that one method of
assessing whether a transition would occur would be to subject the sample to
elevated heat.
ii. Apotex’s Witnesses
[55]
For
its part, Apotex filed the affidavits of John Hems, Peter Stang, Lee Timothy
Grady, Carlos Zetina Rocha, Allan W. Remy, Matthew Buck, Robert McClelland,
Nicholas Taylor, Robert Brown, Michael J. Cima, and William K. Sinden.
[56]
Mr.
John Hems is the Director of Regulatory Affairs with Apotex. He is responsible
for the preparation of the company’s drug submissions for regulatory approval. He
was asked to provide samples of 250 mg and 500 mg BIAXIN tablets, that is
clarithromycin film-coated tablets, to Dr. Michael Cima, a professor at the
Massachusetts Institute of Technology in Cambridge, Massachusetts.
[57]
Dr.
Peter J. Stang is a Professor of Chemistry at the University of Utah. He
holds a Doctorate in organic chemistry and is considered an expert in the
field. He was asked to provide an opinion upon the allegations of
non-infringement advanced by Apotex in respect of the Abbott Patents. He was
also asked to review and compare the Drug Master File (the “DMF”) of Medicorp,
the supplier of clarithromycin to Apotex, with the prior art cited by Apotex.
[58]
Dr.
Stang discussed the conversion of erythromycin A into clarithromycin, as set
out in the Medicorp DMF. In his opinion, the Medicorp process would not result
in Form II but rather in clarithromycin acetane solvate. An acetane solvate is
not Form II and consequently the Medicorp process does not infringe the ’732
Patent. It is possible to obtain Form II from a methanol solvate through
extended drying times but the ’732 Patent does not teach this.
[59]
Dr.
Stang acknowledged that the prior art, in particular, the Morimoto article is silent
on the drying step. However, he said that a person skilled in the art would
regard a drying step as implicit and inherent, and that Form 0 and Form I “were
made and are inherent in the prior art”.
[60]
Dr.
Lee Timothy Grady is the Vice President and Director Emeritus of the United
States Pharmacopeial Convention, Incorporated (“USPC”). He was asked to review
correspondence from
counsel for Apotex to comment at USPC
concerning certain lots of clarithromycin. In his affidavit, Dr. Grady provided
information about the operations of the United States Pharmacopeia (“USP”).
[61]
Dr.
Carlos Zetina Rocha holds a Doctorate in chemistry and formerly worked as a
research chemist with Apotex Pharmaceuticals Inc., previously known as
Brantford Chemicals Inc. He was employed there as a synthetic, organic chemist.
He was asked to conduct the reproduction of certain examples of the ’732 Patent
involving the crystallization and recrystallization of clarithromycin.
[62]
In
his affidavit, he provided details about the experiments that he carried out.
He did not provide any opinion. In cross-examination, Dr. Zetina stated that,
typically, when drying a substance to remove a solvent , a lower temperature is
used than that employed with clarithromycin.
[63]
Dr.
Robert McClelland is a Professor of Chemistry at the University of Toronto
in Toronto. He said
that he is considered an international expert on Physical Organic Chemistry and
Biological Chemistry. He has more than thirty years of research and teaching experience.
He provided a lengthy affidavit setting out his opinion on the allegations
raised in the NOA.
[64]
Dr.
McClelland took the position that the procedures for crystallising and
recrystallising as set out in the Abbott Patents are common methods with which
a person skilled in the art would be very familiar. He expressed the view that
there was no inventive step involved in the ethanol crystallizations set out in
the Abbott Patents.
[65]
With
respect to Iwasaki, Dr. McClelland said that this article taught a method,
prior to 1996, by which a person skilled in the art would be led directly and
without difficulty to the polymorph of clarithromycin. In addition, the methods
set by Watanabe made and taught a person skilled in the art how to make Form II
(substantially free of Form I).
[66]
Further
issues were identified relative to the ’361 Patent. Dr. McClelland said that
there was no sound basis in this patent of teaching how a person skilled in the
art could obtain or identify Form 0 solvate or use Form 0 solvate in the
process for preparing Form II. He later testified in cross-examination that
there is nothing in the prior art about heating clarithromycin over 70° Celsius
but that heating below 70° Celsius was obvious.
[67]
Dr.
Nicholas J. Taylor is a Professor of Chemistry and X-ray Service Manager for
the Department of Chemistry at the University of Waterloo, Ontario. He holds a
Doctorate in Chemistry and has more than twenty-five years of experience
teaching at the university level. He was provided with copies of the Abbott
Patents, the NOA, the prior art and the affidavits of the Applicants’ experts.
He was asked to determine the single crystal x-ray structure for clarithromycin
obtained by crystallization/recrystallization from various solvent preparations
according to the teachings of the ’606, ’527, ’534, ’274, ’356 and ’361
Patents. He was also asked to provide his opinion in respect of the affidavits
of Dr. Zaworotko and Dr. Chyall. He was asked, in addition, to determine the
single crystal x-ray structure for clarithromycin by crystallization/recrystallization
from acetone and methanol, each according to the teachings of the ’732 Patent.
[68]
He
determined that crystallization/recrystallization of clarithromycin yields a
mono-acetone solvate. Crystallization/recrystallization of clarithromycin from
methanol yields a mono-methanol solvate that agrees with the mono-methanol
solvate published by Iwasaki in the prior art.
[69]
Dr.
Robert S. Brown is a Professor of Chemistry at Queen’s University in Kingston, Ontario. He has more
than thirty years of experience in teaching and research in the field of
chemistry. He was asked to provide an opinion with respect to the allegations
of non-infringement and invalidity of the Abbott Patents, as set out in the
NOA.
[70]
In
his affidavit, Dr. Brown set out the position that Form II was an “old”
substance, having been disclosed in European patent applications, two articles
by Morimoto and three articles by Watanabe. Although these articles do not
disclose the drying process, he is certain that they disclose Form II.
[71]
He
expressed the opinion that methods A and B in Watanabe’s 1993 Article were
“obvious chemical equivalents” to the methods described in the ’732 Patent. As
well, he concluded that the Medicorp process to be used to make clarithromycin
for Apotex do not infringe the Abbott Patents.
[72]
In
cross-examination, Dr. Brown testified that, absent experimentation, it would
not be possible to predict the results as to whether one would obtain a
desolvated solvate, amorphous material, a new crystal form, or a change from
one form to another. The results would not be obvious to a person skilled in
the art.
[73]
He
further agreed that none of the cited prior art indicated that clarithromycin
was polymorphic or indicated appropriate drying procedures, that is temperature
and time. Finally, he agreed that it would not be possible for a person skilled
in the art to read the prior art and deduce that someone had produced an
ethanol solvate of clarithromycin.
[74]
Dr.
Michael J. Cima is a Professor of Materials Science and Engineering at MIT in Massachusetts. He was
asked to provide an opinion upon the Stephenson thesis, particularly whether
that document anticipated or made obvious Form II of clarithromycin as claimed
in the ’732 Patent, the ’606 Patent and the ’527 Patent.
[75]
Dr.
Allan W. Rey is the Manager, Intellectual Property/Program Research and
Development of Apotex Pharmachem Inc. (“API”), and is responsible for a group
of chemists and engineers, including supervision of their work. In that
capacity, he was asked to carry out and/or supervise certain procedures
relative to the ’732 Patent. He provided the patent to Dr. Zetina, told him
what was required and supervised certain procedures. Dr. Rey also supervised
the control of certain procedures by Mr. Matthew Buck.
[76]
Mr.
Matthew Buck is a Research and Development Associate (Level II) with API. He
was asked to carry out certain procedures including the
crystallization/recrystallization of clarithromycin from various solvents and
mixed solvent systems according to various examples disclosed in the ’732, ’527
and ’274 Patents. Copies of pages from his laboratory notebooks were attached
as exhibits to his affidavit.
[77]
Mr.
William Kitt Sudin is a registered patent agent. He conducted certain
literature searches relative to clarithromycin. His searches included reference
to patents related to clarithromycin, including the prior art referenced in the
Respondent’s NOA.
VII. Issues
[78]
The
following issues were raised in the written and oral submissions of the
parties.
1.
Who
bears the burden of proof in light of the presumption of validity arising from
section 43 of the Patent Act, R.S.C. 1985, c. P-4?
2.
Are
the Applicants entitled to a prohibition order with respect to the Respondent’s
allegations relative to the ’732 Patent?
3.
Does
the ’606 Patent render Form II of clarithromycin anticipated or obvious?
4.
Are
claims 31 and 62 of the ’361 Patent eligible and valid?
VIII. Discussion and Disposition
[79]
This
application seeks to prohibit the issuance of an NOC to the Respondent in
respect of its generic version of clarithromycin. According to its NOA, the
Respondent has filed an Abbreviated New Drug Submission (“ANDS”) with the
Minister in support of its request for an NOC for 250 mg and 500 mg clarithromycin
tablets for oral administration referencing the Applicants’ 250 mg and 500 mg
BIAXIN clarithromycin film-coated tablets for oral administration in this
respect. The Respondent, in its NOA, refers to the Abbott Patents and alleges
that the said patents are invalid or, alternatively that its proposed
pharmaceutical products will not infringe.
[80]
An
NOC grants marketing approval for drugs in Canada. It is
issued by the Federal Government, indicating that all requirements have been
met pursuant to the Food and Drug Regulations, for the protection of public
health and safety. The NOC Regulations authorize owners of existing patents for
pharmaceutical products to file a "patent list" relative to those
products for which they hold a NOC. The NOC Regulations refer to the person
filing such a list as the "first person". In this case, the
Applicants are the "first person".
[81]
The
framework of the NOC Regulations allows generic drug manufactures to rely on
prior approval of related pharmaceutical products in applying for marketing
approval of their generic form of the products. Manufacturers who produce the
same drug may file an application for an NOC that refers to and relies on the
fact that prior approval has been granted for the brand-name version of the
drug. Such a manufacturer is known as the "second person" and that is
the Respondent's status.
[82]
The
NOC Regulations prohibit the Minister of Health from issuing an NOC until all
relevant product and use patents in the earlier approved medicine, as described
in the patent list, have expired. Consequently, a second person must either
wait until patent expiry before receiving an NOC or it may submit an NOA to the
Minister with its ANDS.
[83]
The
NOC Regulations require service of the NOA upon the first person. Section 5
sets out the grounds upon which an NOA is to be based. Briefly, the NOA must
assert either that the first person is not the patentee, that the patent is
expired or invalid, or that it would not be infringed if a NOC were issued.
[84]
Following
service of the NOA, the Minister may issue an NOC to the second person, unless
the first person avails of its right, pursuant to section 6(1) of the NOC
Regulations, to seek an order from the Federal Court prohibiting the Minister
from issuing the NOC. Any such step must be taken by the first person within 45
days after receipt of the NOA and once such a proceeding is commenced, the
issuance of an NOC to the second person is stayed for a maximum period of
twenty-four months. In the present proceeding, the statutory period will expire
on December 30, 2006, following an extension on consent of the parties.
i. Burden of Proof
[85]
The
Applicants argue that the statutory presumption of validity granted by section 43(2)
of the Patent Act, R.S.C. 1985, c. P-4 (the “Patent Act”) shifts the
burden to the Respondent to invalidate each and every one of the patent claims.
They further argue that they are entitled to an
order of prohibition should the Respondent
fail to establish invalidity in respect of even one of the claims.
[86]
Apotex
disputes these arguments. It submits that the jurisprudence has definitively
established that the burden lies on the Applicants to show, on a balance of
probabilities, that the second person’s allegations of ineligibility,
non-infringement and invalidity are not justified. It argues that the burden does
not shift from the Applicants to the second person and relies on the following decided
cases: Abbott Laboratories v. Canada (Minister of
Health)
(2005), 45 C.P.R. (4th) 81 at paras. 23-29 (F.C.); Pfizer Canada
Inc. v. Canada (Minister of Health) (2006), 46
C.P.R. (4th) 281 at paras. 9-12 (F.C.), rev’d. on other grounds
(2006), 351 N.R. 189 (F.C.A.); Bayer Inc. v. Canada (Minister of
National Health and Welfare) (2000), 6 C.P.R. (4th) 285 at
para. 5 (F.C.A).
[87]
In
Smith Kline Beecham Pharma Inc. v. Apotex Inc., [2001] 4 F.C. 518
(T.D.), aff’d. [2003] 1 F.C. 118 (F.C.A.), Justice Gibson considered the
evidentiary burden in proceedings under the NOC Regulations where invalidity of
a patent is alleged. At pages 533 to 534 he wrote the following:
Against the foregoing, I conclude that
while an evidential burden lies on Apotex to put each of the issues raised in
its Notice of Allegation in play, if it is successful in doing so, the persuasive
burden or legal burden then lies with SmithKline. Assuming Apotex to be successful
in putting the issue of validity of the ’637 Patent in play, SmithKline is
entitled to rely on the presumption of validity of the patent created by
subsection 43(2) of the Act.
The persuasive burden or legal burden
that lies with SmithKline in the circumstances described in the preceding
paragraph is, however, impacted by the nature of the proceeding here before the
Court. In Merck Frosst Canada Inc. v. Canada (Minister of National Health and
Welfare),
[(1994), 55 C.P.R. (3d) 302 (F.C.A.)] Mr. Justice Hugessen, for the Court,
wrote at pages 319-20:
As I understand the scheme of the
regulations, it is the party moving under s. 6, in this case Merck, which, as
the initiator of the proceedings, has the carriage of the litigation and bears
the initial burden of proof. That burden, as it seems to me, is a difficult one
since it must be to disprove some or all of the allegations in the notice of
allegation which, if left unchallenged, would allow the Minister to issue a
notice of compliance.
…
In this connection, it may be noted that,
while s. 7(2)(b) [of the Regulations] seems to envisage the court making a
declaration of invalidity or non-infringement, it is clear to me that such
declaration could not be given in the course of the s. 6 proceedings themselves.
Those proceedings, after all, are instituted by the patentee and seek a
prohibition against the Minister; since they take the form of a summary
application for judicial review, it is impossible to conceive of them giving
rise to a counterclaim by the respondent seeking such a declaration. Patent
invalidity, like patent infringement, cannot be litigated in this kind of
proceeding.
Thus, the burden on SmithKline is only to
disprove the allegations in the notice of allegation, not to justify declarations
of validity and infringement or conversely to negative claims for declarations
of invalidity and non-infringement.
[88]
The
burden lies on Abbott, as the Applicants, to refute the allegations set forth
by Apotex in its NOA dated August 21, 2003. Therefore, like any plaintiff or
applicant, Abbott has the overall legal burden of proof. Apotex, as the
Respondent, has an obligation to put the allegations set out in its NOA in
play.
[89]
Abbott
accepts that it carries the legal burden with respect to the allegation of
non-infringement. However, it argues that Apotex carries the burden of proof
in relation to the allegation of invalidity, on the basis of the presumption of
validity that arises under section 43 of the Patent Act.
[90]
Apotex
disputes this argument. Relying on the decision in Bayer Inc. v. Canada (Minister of
National Health and Welfare) (2000), 6 C.P.R. (4th) 285 (F.C.A.), it
acknowledges that Abbott enjoys the presumption of validity, however, this does
not relieve the Applicants of the burden to adduce evidence to show that the
allegations of invalidity are not justified. If they fail to do so, then the
application for prohibition must fail, see Bayer Inc. v. Canada (Minister of
National Health and Welfare) (2000), 6 C.P.R. (4th) 285.
[91]
In
Janssen-Ortho Inc. v. Novopharm Ltd. (2004), 35 C.P.R. (4th) 353
(F.C.T.D.), Justice Mosley concluded that as long as the second person adduces
evidence that is not clearly incapable of establishing its allegation of
invalidity, then the statutory presumption is spent and cannot assist the first
person for the purpose of a prohibition proceeding.
[92]
In
my opinion, the Applicants’ arguments on the burden of proof are unsound. In Pfizer
Canada Inc. v. Canada (Minister of Health) (2006), 46
C.P.R. (4th) 281 (F.C.) at para. 12 and Abbott Laboratories v. Canada (Minister of
Health)
(2005), 45 C.P.R. (4th) 81 (F.C.), the Court clearly rejected
arguments about a shifting burden. Although the Respondent characterizes the
Applicants’ arguments in this regard as being an abuse of process, on the
grounds that the issue has already been determined and that the jurisprudence
is known to the Applicants, I decline to
comment on that submission. I do not accept
the Applicants’ arguments, having regard to the prevailing jurisprudence.
[93]
The
present proceeding is a summary proceeding pursuant to the NOC Regulations and
the Federal Court Rules, 1998, SOR/98-106 (the “Rules”) governing
application for judicial review. Again, a finding of invalidity or infringement
in the context of this type of proceeding is not determinative of that issue in
any subsequent action; see Pharmacia Inc. v. Canada (Minister of National
Health and Welfare) (1994), 58 C.P.R. (3d) 209 (F.C.A.) at page 216 where
the Court said as follows:
... these proceedings are not actions for
determining validity or infringement: rather they are proceedings to determine
whether the Minister may issue a notice of compliance. That decision must turn
on whether there are allegations by the generic company sufficiently
substantiated to support a conclusion for administrative purposes (the issue of
a notice of compliance) that the applicant's patent would not be infringed if
the generic's product is put on the market....
[94]
I
conclude that the Applicants bear the burden of establishing that Apotex’s
allegations of invalidity are not justified.
[95]
At
the outset of the hearing counsel for the parties confirmed on the record that
infringement is not an issue, although the NOA makes allegations of
non-infringement. The Respondent’s position is that its product will not
infringe because it is made in a different process than the Applicants’ product.
[96]
The
three patents that will be considered are ’732, ’606 and ’361.
ii. The ’732 Patent
[97]
The
Applicants assert that the Respondent is estopped from arguing non-infringement
of the ’732 Patent, on the ground that it did not raise that issue in
proceedings T-1133-02, that is the decision of Justice Phelan, reported at Abbott
Laboratories v. Canada (Minister of Health) (2005), 45 C.P.R. (4th)
81 (F.C.). The Applicants argue that they could not raise this issue prior to
the delivery of judgment in T-1133-02; that judgment was delivered on September
28, 2005. In support of this submission, the Applicants rely upon an Order that
was signed on September 9, 2002 by Prothonotary Lafrenière.
[98]
For
its part, the Respondent submits that the Applicants did not raise this issue
in their Notice of Application and it is too late for them to raise the
argument only in the written argument filed in support of this application. The
Respondent argues that an argument respecting issue estoppel requires an
evidentiary foundation and the failure of the Applicants to raise this issue in
their Notice of Application is prejudicial and improper. In this regard, it
relies on the decision of Justice Layden-Stevenson in Astrazeneca
AB
v. Apotex Inc. (2006), 46 C.P.R. (4th) 418 (F.C.)
[99]
The
Notice of Application served by the Applicants in this matter sets out the
following relative to the ’732 Patent:
13.
Canadian
Patent 2,261,732 (the “’732 Patent”) was issued to Abbott U.S.A. on July 24, 2001. It concerns
a process for the preparation of 6-O-methylerythromycin A Form II and 6-O-methylerythromycin
A crystal Form II prepared according to said process. The ’732 Patent contains
15 claims to the process for the preparation of 6-O-methylerythromycin A
Form II as well as 6 claims directed to 6-O-methylerythromycin A crystal
Form II prepared according to said process.
14.
On August
9, 2001, and within the 30 days prescribed by Section 4(4) of the NOC
Regulations, Abbott Canada submitted Form IV Patent Lists containing the ’732
Patent.
15.
Apotex had
made allegations under paragraphs 5(1)(b)(iv) [non-infringement] and
5(1)(b)(iii) [invalidity] of the Regulations in regard to the ’732
Patent. None of these allegations are justified.
[100] There is
nothing here to suggest that the Applicants intend to argue issue estoppel.
There is nothing on the record to show that any efforts were made to seek leave
to amend the Notice of Application. Indeed, although this matter was initially
scheduled to be heard in October 2005, the parties had requested an adjournment
of that hearing date in June 2005 and a new hearing date was set by Order dated
July 15, 2005.
[101] I agree with
the submissions of the Respondent on this point and refer to the decision of
Justice Mosley in Pfizer Canada Inc v. Apotex Inc. (2005), 43 C.P.R. (4th)
81 F.C. at paragraph 100 where he said the following:
As provided for in Rule 301(e) of the Federal
Courts Rules, 1998, SOR/98-106, an application shall set out a complete
statement of the grounds intended to be argued. As noted by Weston, J. in Pharmacia,
supra at page 339, it also flows from the legal burden on the applicants
under section 6 of the regulations to inform the respondent as to what “vexes”
the patentee so that it may, if necessary, tender evidence in response.
[102] The
Applicants said nothing about this issue when they commenced this proceeding by
filing their Notice of Application on October 7, 2003. It was too late to raise
this matter in their written memorandum that was filed on July 13, 2006.
[103] In the
circumstances, I will not entertain the arguments relative to issue estoppel in
respect of the ’732 Patent. The Applicants raised no other submissions and
accordingly, no Order of Prohibition will issue with respect to the ’732
Patent.
iii. Claims Construction
[104] The first
step in assessing the allegations of invalidity is to construe the disputed
claim of the patent. In Whirlpool Corp. v. Camco Inc., [2000] 2 S.C.R.
1067 and Free World Trust v. Électro Santé Inc., [2000] 2 S.C.R. 1024
the Supreme Court of Canada held that the patent claim is to be construed in a purposive
way and that the Court must consider the entire specification of the patent in
order to understand the words as stated in a disputed claim. In Free World
Trust, at pages 1043-1044, Justice Binnie identified a list of principles
that guide the purposive approach to the construction of a claim, as follows:
a. The Patent Act
promotes adherence to the language of the claims.
b. Adherence to the
language of the claims in turn promotes both fairness and predictability.
c. The claim language
must, however, be read in an informed and purposive way.
d. The language of the
claims thus construed defines the monopoly. There is no recourse to such vague
notions as the “spirit of the invention” to expand it further.
e.
The claims
language will, on a purposive construction, show that some elements of the
claimed invention are essential while others are non-essential. The
identification of elements as essential or non-essential is made:
i. on the basis of
the common knowledge of the worker skilled in the art to which the patent
relates;
ii. as of the date the patent is
published;
iii. having regard to
whether or not it was obvious to the skilled reader at the time the patent was
published that a variant of a particular element would not make a
difference to the way in which the invention works; or
iv. according to the
intent of the inventor, expressed or inferred from the claims, that a particular
element is essential irrespective of its practical effect;
v. without, however,
resort to extrinsic evidence of the inventor’s intention.
f. There is no
infringement if an essential element is different or omitted. There may still
be infringement, however, if non-essential elements are substituted or omitted.
[105] The decisions
in Whirlpool and Free World Trust provide clear instructions that
claims are to be interpreted in light of the patent specification. In following
the purposive approach to interpreting the words or phrases of a claim, the
Court should stay within the four corners of the specification and limit itself
to the words of the claim interpreted in the context of the specification as a
whole, avoiding reliance on extrinsic evidence of intent; see Whirlpool at
page 1095. Expert
evidence is admissible, but only to assist
the Court in interpreting the claim in a knowledgeable way; see Whirlpool
at page 1102.
iv. The ’606 Patent
[106] The ’606
Patent is entitled “Crystal Form II of Clarithromycin”. Its filing date is July
27, 1997, with a publication date of February 5, 1998. It claims priority from
U.S. Patent 08/681,723, with a priority date of July 29, 1996.
[107] The ’606
Patent consists of four claims, as follows:
1.
6-O-methylerythromycin
A Form II is characterized by peaks in the powder x-ray diffraction pattern
having the following 2θ values: 8.5°±0.2, 9.5°±0.2, 10.8°±0.2, 11.5°±0.2,
11.9°±0.2, 12.4°±0.2, 13.7°±0.2, 14.1°±0.2, 15.2°±0.2, 16.5°±0.2, 16.9°±0.2,
17.3°±0.2, 18.1°±0.2, 18.4°±0.2, 19.0°±0.2, 19.9°±0.2, and 20.5°±0.2.
2.
6-O-methylerythromycin
A Form II is characterized by peaks in the powder x-ray diffraction pattern
having the following 2θ values: 8.52°±0.2, 9.48°±0.2, 10.84°±0.2,
11.48°±0.2, 11.88°±0.2, 12.36°±0.2, 13.72°±0.2, 14.12°±0.2, 15.16°±0.2,
16.48°±0.2, 16.92°±0.2, 17.32°±0.2, 18.08°±0.2, 18.40°±0.2, 19.04°±0.2,
19.88°±0.2, and 20.48°±0.2.
3.
6-O-methylerythromycin
A Form II, substantially free of 6-O-methylerythromycin A Form I,
characterized by peaks in the powder x-ray diffraction pattern having the
following 2θ values: 8.5°±0.2, 9.5°±0.2, 10.8°±0.2, 11.5°±0.2, 11.9°±0.2,
12.4°±0.2, 13.7°±0.2, 14.1°±0.2, 15.2°±0.2, 16.5°±0.2, 16.9°±0.2, 17.3°±0.2, 18.1°±0.2,
18.4°±0.2, 19.0°±0.2, 19.9°±0.2, and 20.5°±0.2.
4.
6-O-methylerythromycin
A Form II, substantially free of 6-O-methylerythromycin A Form I, characterized
by peaks in the powder x-ray diffraction pattern having the following 2θ
values: 8.52°±0.2, 9.48°±0.2, 10.84°±0.2, 11.48°±0.2, 11.88°±0.2,
12.36°±0.2, 13.72°±0.2, 14.12°±0.2, 15.16°±0.2, 16.48°±0.2, 16.92°±0.2,
17.32°±0.2, 18.08°±0.2, 18.40°±0.2, 19.04°±0.2, 19.88°±0.2, and 20.48°±0.2.
[108] Again, the
first step is the construction of the patent. This involves reading the claims
through the eyes of a skilled worker and informed by the disclosure, as well as
expert evidence if necessary.
[109] The claims
are directed to a product per se. In claims 1 and 2, the product is
clarithromycin Form II, characterized by its PXRD pattern. The PXRD for each
claim is the same, except that in claim 2 that pattern is described to two
digits after the decimal point, rather than one digit.
[110] Claims 3 and
4 claim clarithromycin Form II substantially free of Form I. Again, these
claims are characterized by PXRD patterns, with the pattern in claim 4 being
described to two digits after the decimal point, where the pattern for claim 3
is brought to one digit after the decimal point.
[111] The
Respondent alleged in its NOA that the ’606 Patent is invalid on the grounds of
anticipation and obviousness. It relied on prior art including an article by
Iwasaki, the Stephenson thesis, the Ethanol Art, the USP Standard and the prior
sale of BIAXIN.
[112] In light of
the decision of Justice von Finckenstein in Abbott Laboratories v. Canada (Minister of
Health)
(2005), 42 C.P.R. (4th) 121 (F.C.), aff’d. by the Federal Court of
Appeal in Abbott Laboratories v. Canada (Minister of
Health),
2006 F.C.A. 187 (“Ratiopharm”) in which the ’606 Patent was found to be
anticipated by Iwasaki, the arguments with respect to this patent can be
disposed of summarily.
[113] Iwasaki is
cited as prior art in the present case. The article was published on June 15,
1993 in “Crystal Structure Communication”, Volume 49, Part 6 and is Document
No. 29 in the documents produced by Apotex here. The same evidence was before
Justice von Finckenstein and the Federal Court of Appeal. Iwasaki teaches a
product that is defined by PXRD data that matches the PXRD data set out in the
claim of the ’606 Patent. This article is relevant and probative evidence on
the issue of anticipation, in light of the test established in Beloit Canada
Ltd. et al. v. Valmet Oy (1986), 8 C.P.R. (3d) 289 (F.C.A.). That is enough
to establish anticipation.
[114] Both the
trial judge and the Federal Court of Appeal found on the PXRD patterns as being
a defining and critical element of the claim of the ’606 Patent. No extrinsic
evidence, expert or otherwise, can change the plain language of the claims. The
Iwasaki article establishes anticipates the ’606 Patent.
[115] It is not
necessary for me to comment on the other pieces of prior art cited by the
Respondent. The application for a prohibition order is dismissed with respect
to the ’606 Patent.
v. The ’361 Patent
[116] The ’361
Patent is entitled “Crystal Form 0 and Form II of Clarithromycin and Uses
thereof”. It contains 68 claims. Claims 1 to 7 are process claims. The
remaining claims relate to use, forms and compositions of the drug. The filing
date of this patent is December 19, 1997 and it was open for inspection as of
July 23, 1998. The Patent issued on May 25, 2003. It is a divisional of the ’274
Patent and claims priority to U.S. Patent application 08/785,623 dated January
17, 1997.
[117] The
Applicants address claim 31 as a representative claim in their written
memorandum but also addressed claim 62 in the course of oral argument.
[118] The first
matter to be addressed is the construction of the patent. What do claims 31 and
62 mean?
[119] Claim 31 and
62 read as follows:
31. The use of 6-O-methylerythromycin
A Form 0∙ethanolate in the preparation of 6-O-methylerythromycin A
Form II for use as an antibiotic.
62.
The use of
6-O-methylerythromycin A Form 0∙ethanolate, substantially free of
6-O-methylerythromycin A Form I, in the preparation of 6-O-methylerythromycin
A Form II, substantially free of 6-O-methylerythromycin A Form I and 6-O-
methylerythromycin A Form 0∙ethanolate, for use as an antibiotic, wherein
said 6-O-methylerythromycin A Form 0∙ethanolate is characterized
by peaks in the powder x-ray diffraction pattern having the following 2θ
values: 4.72°±0.2, 6.60°±0.2, 7.72°±0.2, 9.30°±0.2, 10.40°±0.2, 11.10°±0.2,
11.86°±0.2, 12.72°±0.2, 13.90°±0.2, 15.02°±0.2, 17.18°±0.2, 18.50°±0.2,
19.08°±0.2, 19.68°±0.2, 23.14°±0.2, and 23.98°±0.2 and said 6-O-methylerythromycin
A Form II is characterized by peaks in the powder x-ray diffraction pattern
having the following 2θ values: 8.52°±0.2, 9.48°±0.2, 10.84°±0.2,
11.48°±0.2, 11.88°±0.2, 12.36°±0.2, 13.72°±0.2, 14.12°±0.2, 15.16°±0.2, 16.48°±0.2,
16.92°±0.2, 17.32°±0.2, 18.08°±0.2, 18.40°±0.2, 19.04°±0.2, 19.88°±0.2, and
20.48°±0.2.
[120] In my
opinion, the plain reading of the language of claim 31 shows that it claims the
use of Form 0 to make something else, that is Form II.
[121] Claim 62, according
to its plain words, claims the use of Form 0 solvate in the preparation of Form
II substantially free of Form I.
[122] The first
argument raised by the Respondent is that all of the claims of the ’361 Patent
are ineligible for listing on the Patent Register because they claim the use of
Form 0 as an intermediary in the preparation of Form II. The second ground
advanced by the Respondent is that the ’361 Patent is anticipated and/or
obvious in light of the prior art, in particular the ethanol art and the melting
point references.
[123] It submits
that claim 31 speaks to the use of Form 0 in the preparation of Form II without
any other intermediate steps. Generally, claim 62 addresses the same thing. The
Respondent argues that the words in claim 31 “for use as an antibiotic” are not
essential to the claim and in any event, it is not disputed that clarithromycin
is useful as an antibiotic. Further, the Court of Appeal in Ratiopharm
has found Form 0 to be old and Justice Phelan has found Form II to be old.
[124] In response,
the Applicants submit that the Federal Court of Appeal in Ratiopharm has
conclusively said that each of Form 0, Form I and Form II is a medicine. The
Applicants rely on paragraphs 5 and 6 of that decision as follows:
5. Abbott claims to have discovered
three forms of clarithromycin, which it has named "Form 0",
"Form I" and "Form II". It is undisputed that
clarithromycin, whether in Form 0, Form I, or Form II, is an antibiotic, and
that each of those forms of clarithromycin is within the definition of the word
"medicine" in the NOC Regulations, which reads as follows:
"medicine" means a substance
intended or capable of being used for the diagnosis, treatment, mitigation or
prevention of a disease, disorder or abnormal physical state, or the symptoms thereof.
"médicament" Substance destinée
à servir ou pouvant servir au diagnostic, au traitement, à l'atténuation ou à
la prévention d'une maladie, d'un désordre, d'un état physique anormal, ou de
leurs symptômes.
6. Ratiopharm's proposed clarithromycin
product contains Form II. It is common ground that Form 0 is produced in the
process of making Form I or Form II. However, the Form 0 so produced is
unstable, in the sense that if nothing is done to it, it becomes a different
form of clarithromycin within a short period of time. It appears that Form 0
was not identified as a unique substance until it was stabilized by the
inventors named in the 274 patent.
[125] The terms
“claim for the medicine itself”, “claim for the use of the medicine” and
“medicine” are defined in section 2 of the NOC Regulations as follows:
|
2. In
these Regulations,
"claim
for the medicine itself" includes a claim in the patent for the medicine
itself when prepared or produced by the methods or processes of manufacture
particularly described and claimed or by their obvious chemical equivalents;
"claim
for the use of the medicine" means a claim for the use of the medicine
for the diagnosis, treatment, mitigation or prevention of a disease, disorder
or abnormal physical state, or the symptoms thereof;
|
2. Les
définitions qui suivent s'appliquent au présent règlement.
«revendication
pour le médicament en soi» S'entend notamment d'une revendication, dans le
brevet, pour le médicament en soi préparé ou produit selon les modes du
procédé de fabrication décrits en détail et revendiqués ou selon leurs
équivalents chimiques manifestes.
«revendication
pour l'utilisation du médicament» Revendication pour l'utilisation du
médicament aux fins du diagnostic, du traitement, de l'atténuation ou de la
prévention d'une maladie, d'un désordre, d'un état physique anormal, ou de
leurs symptômes.
|
[126] Section 4 of
the NOC Regulations addresses the patent list and provides as follows:
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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.
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4.(1)
La personne qui dépose ou a déposé une demande d'avis de conformité pour une
drogue contenant un médicament ou qui a obtenu un tel avis peut soumettre au
ministre une liste de brevets à l'égard de la drogue, accompagnée de
l'attestation visée au paragraphe (7).
(2)
La liste de brevets au sujet de la drogue doit contenir les renseignements
suivants :
a)
la forme posologique, la concentration et la voie d'administration de la
drogue;
b)
tout brevet canadien dont la personne est propriétaire ou à l'égard duquel
elle détient une licence exclusive ou a obtenu le consentement du
propriétaire pour l'inclure dans la liste, qui comporte une revendication
pour le médicament en soi ou une revendication pour l'utilisation du
médicament, et qu'elle souhaite voir inscrit au registre;
c)
une déclaration portant, à l'égard de chaque brevet, que la personne qui
demande l'avis de conformité en est le propriétaire, en détient la licence
exclusive ou a obtenu le consentement du propriétaire pour l'inclure dans la
liste;
d)
la date d'expiration de la durée de chaque brevet aux termes des articles 44
ou 45 de la Loi sur les brevets;
e)
l'adresse de la personne au Canada aux fins de signification de tout avis
d'allégation visé aux alinéas 5(3)b) ou c), ou les nom et adresse au Canada
d'une autre personne qui peut en recevoir signification avec le même effet
que s'il s'agissait de la personne elle-même.
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[127] The
jurisprudence is clear that an intermediate is not a “claim for the medicine
itself” nor a “claim for the use of the medicine”.
[128] In Deprenyl
Research Ltd. et al. v. Apotex Inc. et al. (1984), 55 C.P.R. (3d) 171
(F.C.T.D.) at page 176 the Court said the following:
Therefore, the phrase “claim for the medicine
itself”, in the Patented Medicines (Notice of Compliance) Regulations
means a claim for the medicine itself, in the ordinary and natural sense of the
words, and a claim for the medicine when prepared by a particular process, in
the ordinary and natural sense of the words used in s.2. There is nothing in
the language of the legislation which suggests the phrase also covers a claim
for a particular process used to produce a medicine. Such an interpretation
would, in my view, be an unwarranted enlargement of the natural sense of the
words used in the regulations.
[129] In Eli
Lilly and Co. et al. v. Apotex Inc. et al. (1996), 68
C.P.R. 2d 126 (F.C.A.), the Federal Court of Appeal commented on the definition
of “medicine” in section 2 of the NOC Regulations at page 128 as follows:
The definition in section 2 of the
Regulations is clear and entirely unambiguous: in order to be a “medicine” a
substance must be intended for or capable of one or more of the precise listed
medical uses. Chemical conversion or synthesis into another substance which may
itself be used as a medicine is not one of them. The French text of the
definition is, if possible, even clearer than the English in its emphasis on
the end use to which the substance itself must be put in order to meet the
definition.
[130] The thrust of
the Respondent’s argument here is that claims 31 and 62 of the ’361 Patent
address the use of Form 0 not as a medicine but as a product to make another
product. It argues that this interpretation arises from a plain reading of the
language of the claims and that the conclusions of the Federal Court of Appeal
in Ratiopharm do not govern since the Court in that case was considering
a different patent, with different claims.
[131] In Bristol
Myers-Squibb Co. v. Canada (Attorney General) (2005), 39
C.P.R. (4th) 499 (S.C.C.), the Supreme Court discussed the scope and
function of the NOC Regulations and noted
that this regulatory scheme is intended to
provide limited protection. It is directed to those persons using the patented
invention. In this case, the “patented invention” is Form II made from Form 0.
[132] More
recently, in AstraZeneca Canada Inc. v. Canada (Minister of
Health),
[2006] S.C.J. No. 49, the Supreme Court of Canada again addressed the purpose
of the NOC Regulations and said, in paragraph 39, that subsection 5(1) of the
NOC Regulations requires a “patent specific analysis”. Although AstraZeneca
was concerned with the issue of “evergreening”, in my opinion, the direction to
take a patent specific analysis is equally applicable here. The ’361 Patent is
directed to the use of Form 0 as an intermediary, not as a medicine. The status
of Form 0 as a medicine in another context does not change its status here.
[133] Finally, with
respect to the decision of the Federal Court of Appeal in Ratiopharm, I
note that the Court said that Abbott described the ’361 Patent “as a patent
claiming a method of making Form II from Form 0”. This means that, at least in
the Court of Appeal, the Applicants referred to the ’361 as a process patent.
Such a claim is ineligible under the NOC Regulations.
[134] Accordingly,
I conclude that the relevant claims of the ’361 Patent do not meet the
eligibility requirements for inclusion on the Patent List. This issue is
dispositive concerning the ’361 Patent and it is not necessary to address the
other arguments raised by the parties.
IX. Conclusion
[135] For the
reasons above, this application is dismissed.
[136] This
application proceeded upon the basis of a confidential record. The parties were
asked if they wished to proceed on an in camera basis and advised that
such hearing was not necessary. However, in the interests of avoiding any
inadvertent disclosure of confidential material, these reasons will be issued
on a confidential basis. The parties will advise the Court within fifteen (15)
days of the release of these reasons.
[137] The parties
requested the opportunity to make submissions on costs. In that regard, the
parties shall file their submissions, not to exceed five (5) pages, on or before
January 26, 2007.
“E. Heneghan”
Ottawa,
Ontario
January
11, 2007
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