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488 F.3d 1377, *; 2007 U.S. App. LEXIS 11886, **;
PFIZER, INC., Plaintiff-Appellee, v. APOTEX, INC. (formerly known as Tor- Pharm, Inc.) Defendant-Appellant. 2006-1261 UNITED STATES COURT OF APPEALS FOR THE FEDERAL CIRCUIT 488 F.3d 1377; 2007 U.S. App. LEXIS 11886; 82 U.S.P.Q.2D (BNA) 1852 May 21, 2007, Decided May 21, 2007, Filed PRIOR HISTORY: [**1] Appealed from: United
States District Court for the Northern District of Illinois.
of rehearing and rehearing en banc is de-
Pfizer, Inc. v. Apotex, Inc., 480 F.3d 1348, 2007 U.S. App. LEXIS 6623 (Fed. Cir., 2007)
JUDGES: Before MICHEL, Chief Judge, NEWMAN,
MAYER, LOURIE, RADER, SCHALL, BRYSON, GA-
JARSA, LINN, DYK, PROST, and MOORE, Circuit Judges. NEWMAN, LOURIE, and RADER, Circuit
Judges, would rehear the appeal. NEWMAN, Circuit
dissents in the denial of the petition for
Judge, dissents [**3] in the denial of the petition for
rehearing en banc in a separate opinion.
rehearing in a separate opinion. LOURIE, Circuit Judge, dissents in the denial of the petition for rehearing in a
separate opinion. RADER, Circuit Judge, dissents in the
the denial of the petition for rehearing en
denial of the petition for rehearing in a separate opinion.
the denial of the petition for rehearing en
The Appellee, Pfizer, Inc. filed a combined petition
for panel rehearing and rehearing en banc, and a re-
sponse thereto was invited by the court and filed by the
Appellant, Apotex, Inc. The petition for rehearing was
referred to the panel that heard the appeal, and thereafter the petition for rehearing en banc and response were re-
ferred to the circuit judges who are authorized to request
a poll whether to rehear the appeal en banc. A poll was
DISSENT BY: NEWMAN; LOURIE; RADER
Apotex, Inc. moves for expedited denial of rehearing
and rehearing en banc, and for expedited issuance of the
NEWMAN, Circuit Judge, dissenting from the de-
The court has not accepted the suggestion that this
case be reviewed en banc, and the panel was unper-
suaded by the argument that the decision is incorrect
when the law of precedent is applied. I write separately
because the panel's statement of the applicable law and
its application to the facts of this case are inconsistent
488 F.3d 1377, *; 2007 U.S. App. LEXIS 11886, **;
with the court's precedent. Our obligation as an appellate
panel further erred in declining to give weight to these
court is to assure that the law is both correctly stated and
acknowledged "secondary considerations" of unexpected
correctly applied. When inconsistency is raised by the
results. See Richardson-Vicks, Inc. v. Upjohn Co.,122
panel's treatment, our obligation is to assure that conflicts
F.3d 1476 (Fed. Cir. 1997) (evidence of unexpected re-
with precedent -- whether real or apparent -- are re-
sults must be considered); Ruiz v. AB Chance Co., 234
solved, as well [**5] as to assure that the law is cor-
F.3d 654, 667 (Fed. Cir. 2000) ("Our precedents clearly
rectly applied. From the court's denial of rehearing en
hold that secondary considerations, when present, must
be considered in determining obviousness.")
The ruling in this case has important policy as well
The panel decision changes the criteria as well as the
as legal implications, as the many amici curiae point out,
analysis of patentability, with results of particular sig-
each side stressing a different aspect of the effect on
nificance for their effect on the conduct of R&D, the
commercial activity in the pharmaceutical field. Both
costs of drug development, and the balance between ge-
sides acknowledge that the effects of chemical changes
neric access to established products and the incentive to
on properties of medicinal products is not predictable;
development of new products. The amici curiae on both
the difference residing in the panel's acceptance of the
sides of the issue stress different policy considerations:
long-discredited "obvious to try" standard, on which the
the pharmaceutical research companies point [**8] out
panel superimposes the theory that the skill of these in-
that diminished access to patenting will affect the kind
ventors guided them to trial of the besylate salt (despite
and direction of product development; the generic pro-
the prior art's preference for the maleate salt), thereby
ducers point out that the sooner they can enter the market
negating patentability. The panel's application of the ob-
for established drugs, the lower the consumer price. The
vious-to-try standard is in direct conflict with precedent;
placement of the balance in this ever-present conflict
it has long been the law that "patentability shall not be
between innovator and copier has long engaged the pub-
negated by the manner in which the invention is made."
lic and Congress, and needs must continue to do so.
35 U.S.C. § 103. In Gillette Co. v. S.C. Johnson & Son,
Meanwhile, however, it is inappropriate for a panel of
Inc., 919 F.2d 720, 725 (Fed. Cir. 1990) this court stated
this court to make a change in the precedent by which
that "we have consistently held that 'obvious to try' is not
both sides of the debate have heretofore been bound.
to be equated [**6] with obviousness." In In re
Stability of precedent and the uniform application of
Tomlinson, 53 C.C.P.A. 1421, 363 F.2d 928, 931 (CCPA
correct law to achieve the correct result are the assign-
1966) the court explained that "there is usually an ele-
ment of the Federal Circuit, for our rulings are of nation-
ment of 'obviousness to try' in any research endeavor,
wide effect. A primary purpose for which our court was
that . . . is not undertaken with complete blindness but
formed was to provide the judicial stability that supports
rather with some semblance of a chance of success." The
commercial investment -- this was a unique judicial role,
amici curiae representing research pharmaceutical indus-
and was adopted in recognition of the dependence of
tries in this petition point out that methodical experimen-
technology-based industry on an effective patent system.
tation is fundamental to scientific advance, and particu-
It was recognized that a nationally uniform, consistent,
larly for biological and medicinal products, where small
and correct patent law is an essential foundation of tech-
change can produce large differences. At the trial there
nological innovation, which is today the dominant con-
was no contradiction to the testimony of Pfizer's expert
tributor to the nation's economy. [**9] See the Report
witness Dr. Anderson that "one of ordinary skill in the
of the Domestic Policy Review of Industrial Innovation,
art could neither draw any conclusions nor have any ex-
Department of Commerce 1979 (stressing the need for
pectations about the properties of amlodipine besylate
judicial administration of correct and uniform patent
from the properties of a besylate salt of a different com-
law). In enacting the implementing statute, Congress
pound." Pfizer Br. at 7. Indeed, the parties stipulated this
Nor was there any evidence contradicting Pfizer's
position that "the superior properties at issue were not
Federal Circuit] is to resolve some of the
some abstract concept of 'good' properties, but specific
myriad structural administrative and pro-
properties which solved both the sticking and instability
problems of the [**7] prior art, while providing non-
ability of our Federal courts to deal with
hygroscopicity and good solubility. . . . Trade-offs in salt
the vast range of controversies among our
properties are the rule, and one of skill must usually ac-
cept some undesirable properties [*1380] to achieve
meaningfully to their demands for justice .
other desirable ones. Amlodipine besylate, unlike any
. . which include the inability of our pre-
other amlodipine salt, presented no trade-offs." Id. The
488 F.3d 1377, *; 2007 U.S. App. LEXIS 11886, **;
tive answer to legal questions of nation-
can remedy panel lapses, if indeed this decision repre-
sents such a lapse, or uniformly adopt panel advances in
the law, if indeed this decision represents such an ad-
vance. From the court's decision to decline this review, I
S. Comm. on the Judiciary, Federal Courts Improvement
Act of 1981, S. Rep. No. 97-275, at 1 (1981).
LOURIE, Circuit Judge, dissenting from the denial
When conflicts arise between panel decisions of the
Federal Circuit the ensuing uncertainty is of national
I respectfully dissent from the court's decision not to
scope, contravening the purpose of establishing this
rehear this case en banc. At bottom, I consider that the
court. This adds weight to our obligation to undertake en
decision of the panel was incorrect. But, we do not re-
banc review, both to reestablish consistency in the law
hear appeals simply because a non-panel member dis-
and to correct errors in panel decisions. In 1998, in a
agrees with its result. See Amgen Inc. v. Hoechst Marion
letter to the Commission on Structural [**10] Alterna-
Roussel, Inc., 469 F.3d 1039, 1043 (Fed. Cir. 2006)
tives for the Federal Courts of Appeals, Justice Scalia
(Lourie, J., concurring) [**12] ("I do not believe that
every error by a panel is enbancable. A panel is entitled
to err without the full court descending upon it.").
[T]he function of en banc hearings . . . is
Federal Rule of Appellate Procedure 35(a) provides that
"[a]n en banc hearing or rehearing is not favored and
flicts, [*1381] but also to correct and de-
ordinarily will not be ordered unless: (1) en banc consid-
ter panel opinions that are pretty clearly
eration is necessary to secure or maintain uniformity of
wrong . . . . The disproportionate segment
the court's decisions; or (2) the proceeding involves a
question of exceptional importance." Our Internal Oper-
docket that is consistently devoted to re-
ating Procedures ("IOPs") state that "[a]mong the reasons
for en banc actions are: (1) necessity of securing or
maintaining uniformity of decision; (2) involvement of a
question of exceptional importance; (3) necessity of
reduction function is not being performed
overruling a prior holding of this or a predecessor court
expressed in an opinion having precedential status; or (4)
the initiation, continuation, or resolution of a conflict
Letter dated Aug. 21, 1998, Hearing before the S. Sub-comm. on Administrative Oversight and the Courts of
However, consistent with those established criteria
the S. Comm. on the Judiciary, 106th Cong. 72 (1999).
for taking a case en banc, I consider that the panel erred
in its legal determinations, and that those errors will con-
It is important to the federal system as a
fuse the law relating to rebuttal of a prima facie case of
whole that the Courts of Appeals utilize
obviousness of a chemical compound. [**13] Thus, an
en banc hearing is warranted in this case in order to
within the circuit that are likely to other-
maintain uniformity of the court's decisions and [*1382]
because it presents questions of exceptional importance.
The panel reversed the district court's decision that
claims relating to amlodipine besylate (the active ingre-
dient in the hypertension drug Norvasc (R)) were valid
For the Federal Circuit, it was intended and expected
and nonobvious after a bench trial. Pfizer, Inc. v. Apotex,
that this court would provide uniform national law in all
Inc., 480 F.3d 1348 (Fed. Cir. 2007). In my view, several
of the fields assigned to our exclusive jurisdiction; not
legal errors were made in this decision, and improper
only in patent [**11] law. Our cases are rarely factually
deference was given to fact-findings of the district court.
simple, and when there arise apparently divergent panel
First, the panel failed to defer to fact-findings made
statements of the law and its application, the responsibil-
by the district court that were not clearly erroneous re-
ity for en banc review looms large. The goal of judging
garding the unexpected properties of amlodipine besy-
is "full, equal and exact" enforcement of the law. See
late. Evidence in the record, including trial testimony of
Roscoe Pound, "The Etiquette of Justice," 3 Proceedings
experts and Pfizer scientists, internal research and devel-
Neb. St. Bar Assn. 231 (1909) ("full, equal and exact
opment documents, and a scientific article, supported the
enforcement of substantive law is the end" of the judicial
district court's finding that "the besylate salt clearly and
process). Through the system of en banc review, courts
unexpectedly exhibited a superior combination of prop-
488 F.3d 1377, *; 2007 U.S. App. LEXIS 11886, **;
erties when compared to what was suggested in the pre-
fore was not patentable. See Pfizer, 480 F.3d at 1367
ferred preparation." District Court Oral Op. Tr. at 23:13-
(emphases added) (stating that the "type of experiments
15; see Pet. for Reh'g en banc at 5-6. The panel [**14]
used by Pfizer's scientists to verify the physicochemical
disregarded that express finding of fact, holding that
characteristics of each salt are not equivalent to the trial
"Pfizer has simply failed to prove that the results are un-
and error procedures often employed to discover a new
expected." Pfizer, 480 F.3d at 1371. Moreover, relying
compound where the prior art gave no motivation or
on the testimony of both parties' experts, the district
suggestion to make the new compound nor a reasonable
court found that there was no reasonable expectation of
expectation of success"). That conclusion conflicts with
success with regard to using the besylate salt form of
the statutory requirement that "[p]atentability shall not be
amlodipine. District Court Oral Op. Tr. at 23:1-9. How-
negatived by the manner in which the invention was
ever, rather than give deference to the district court's
made." 35 U.S.C. § 103(a). Moreover, the conclusion
fact-findings, the panel substituted its own finding that a
contradicts the district court's supported findings that the
reasonable expectation of success existed in the art. See
results were unexpected, and that the experiments led to
Pfizer, 480 F.3d at 1361, 1364-65 ("The record also sat-
showing the totality of the [**17] properties of the in-
isfies us that, contrary to the district court's finding, a
vention, see Papesch, 50 C.C.P.A. 1084, 315 F.2d 381,
reasonable fact-finder could only conclude that the
1963 Dec. Comm'r Pat. 334, which makes the compound
skilled artisan would have had a reasonable expectation
nonobvious, not merely to the verification of results.
of success with the besylate salt form of amlodipine.").
In addition, holding an inventor's expectations of
Much public discussion has occurred, and even judicial
success against the objective unexpectedness of the
comments in opinions, that we should defer to district
properties of the compound unfairly suggests that an
court judges concerning certain aspects of claim con-
inventor should try only that which he doubts will work.
struction, which we have held is a matter of law. Be that
See Pfizer, 480 F.3d at 1371 ("Dr. Wells' testimony re-
as it may, it is undisputed that we must defer to fact-
flects the fact that he believed that amlodipine besylate
findings by a district court, unless they are [**15]
would solve the problems of amlodipine maleate."). In-
clearly erroneous, and I do not believe that they were
ventors generally are optimistic about what they choose
to experiment with, but that does not necessarily suggest
In addition, the panel improperly placed greater im-
portance on the therapeutic value of a claimed compound
These issues are of exceptional importance. Chemi-
over the value of its physical properties. The panel con-
cal and pharmaceutical compounds often can be found to
cluded that the improvement of the invention, which
be prima facie obvious, as they are based on prior work
related to drug formulation, viz., increased stability and
that could reasonably suggest them, see KSR Int'l Co. v.
decreased stickiness, was "insufficient" to meet the stan-
Teleflex Inc., 127 S. Ct. 1727, 167 L. Ed. 2d 705, 2007
dards of patentability. Id. at 1368 (emphases added)
WL 1237837 (2007), but commercialization of such
("[W]e hold that the optimization of the acid addition salt
compounds may depend on their possession of unex-
formulation for an active pharmaceutical ingredient
pected properties. Such properties may be biological or
would have been obvious where as here the acid addition
physical. A failure to recognize all such properties that
salt formulation has no effect on the therapeutic effec-
[**18] may be relevant to the value of such a compound
tiveness of the active ingredient and the prior art heavily
may doom the compound to being poured down the drain
suggests the particular anion used to form the salt."). I
rather than becoming an important therapeutic. The gen-
read that conclusion as improperly requiring a compound
eral public, innovative companies, and, ultimately, ge-
to possess a specific type of improvement over the prior
neric companies, depend upon faithful adherence to this
art--in this case, improved therapeutic properties--to be
principle. In addition, our cases hold that unexpected
patentable, negating other important properties, a conclu-
properties make for non-obviousness, see Papesch, 50
sion that is not compelled by our case law and not sound.
C.C.P.A. 1084, 315 F.2d 381, 1963 Dec. Comm'r Pat.
Any useful and unexpected property should be eligible to
334, and this decision disdains such properties if they are
overcome a prima facie obviousness determination.
not biological. That is a conflict with our precedent that
[**16] See In re Papesch, 50 C.C.P.A. 1084, 315 F.2d
381, 391, 1963 Dec. Comm'r Pat. 334 (CCPA 1963) ("From the standpoint of patent law, a compound and all
Not least, the question of deference to district courts,
of its properties are inseparable; they are one and the
at least on fact issues, needs reaffirming. We must not
same thing. . . . There is no basis in law for ignoring any
shy away from reversing fact-findings that truly are
property in making such a comparison.").
clearly erroneous, as we do encounter them from time to time, but this case does not present them.
[*1383] Third, the panel also found that the inven-
tion was the result of routine experimentation, and there-
488 F.3d 1377, *; 2007 U.S. App. LEXIS 11886, **;
Thus, I would rehear this case, and I dissent from the
cerned a reasonable expectation of success by giving
undue emphasis to the inventor's subjective hopes for the outcome of his experiments.
RADER, Circuit Judge, dissenting from the denial
The panel also mistakenly determined that the supe-
rior properties of the besylate did not overcome a prima
I respectfully dissent from the decision to deny re-
facie case of obviousness because they showed no supe-
rior therapeutic value--the maleate salt form of amlodip-
In this case, the trial court made the factual determi-
ine worked just as well as the besylate form in clinical
nation that the besylate salt form of amlodipine had un-
trials. Therapeutic value, however, is just one property of
expected superior properties over the [**19] closest
a pharmaceutical. Other properties, such as solubility,
prior art. Accordingly, the underlying patent ('303) was
stability, hygroscopicity, and processability, must also
valid and nonobvious. Three separate district courts held
play a role in the analysis of advantages. The superior
trials involving the '303 patent. Indeed, each of those
properties of the besylate salt form of amlodipine, over-
three different district court judges came to the same
came the stability and stickiness problems that existed
[*1384] factual conclusion regarding the nonobvious-
with the maleate salt form and created a superior formu-
ness of amlodipine besylate. Because the factual deter-
lation. Although the maleate salt [**21] form was also
minations in the case below were not clearly erroneous,
therapeutically effective, the besylate form was still a
this court should have deferred to the district court's fac-
significant improvement because it overcame the stabil-
ity and processing problems that could have prevented successful commercial marketing.
As the testimony indicated, the properties of new
pharmaceutical salt forms are entirely unpredictable.
The panel also found that amlodipine besylate was
Even the Berge reference on which the panel relied
not patentable since it was made by a routine testing or a
clearly states: "Unfortunately there is no reliable way of
"well known problem solving strategy." This clearly vio-
predicting the influence of a particular salt species on the
lates the statutory mandate that "patentability shall not be
behavior of the parent compound." The district court
negatived by manner in which the invention was made."
agreed and made the factual determination that the supe-
35 U.S.C. 103(a). Many if not most pharmaceutical in-
rior properties of amlodipine besylate over the prior art
ventions are discovered through a routine screening pro-
(increased stability and decreased stickiness) were in-
tocol or through an established trial and error process.
deed unexpected--a finding that deserved deference.
Pharmaceutical inventions discovered by these routine screening methods include not only new formulations
Furthermore 'obvious to try' jurisprudence has a very
and salt forms, but also include the active pharmaceutical
limited application in cases of this nature. With unpre-
compounds themselves. Thus, this decision calls into
dictable pharmaceutical inventions, this court more
question countless pharmaceutical patents, which in turn
wisely employs a reasonable expectation [**20] of suc-
could have a profoundly negative effect on investments
cess analysis. In this case, salt selection is unpredictable,
into the design and development of new life-saving
thus rebutting, as most other courts found, any reason-
pharmaceuticals. With many questions about this case, I
able expectation of success. Although the panel gives
"lip service" to the principle that 'obvious to try' does not work in this field, it nonetheless appears to be the basis for its decision in this case. In addition, the panel dis-
Citation #3 2007 U.S. App. LEXIS 15349 TAKEDA CHEMICAL INDUSTRIES, LTD. and TAKEDA PHARMACEUTI- CALS NORTH AMERICA, INC., Plaintiffs-Appellees, v. ALPHAPHARM PTY., LTD. and GENPHARM, INC., Defendants-Appellants. UNITED STATES COURT OF APPEALS FOR THE FEDERAL CIRCUIT 492 F.3d 1350; 2007 U.S. App. LEXIS 15349; 83 U.S.P.Q.2D (BNA) 1169 June 28, 2007, Decided SUBSEQUENT HISTORY: Later proceeding at
similarly structured compounds exhibited negative side
Takeda Chem. Indus. v. Ranbaxy Labs., Ltd., 2007 U.S.
effects, while other compounds were more promising at
App. LEXIS 15883 (Fed. Cir., June 28, 2007)
the time of invention. The court of appeals concluded
US Supreme Court certiorari denied by Alphapharm Pty
that the district court did not err in determining that the
v. Takeda Chem. Indus., 2008 U.S. LEXIS 3015 (U.S.,
claimed compounds would not have been obvious in
light of the prior art, and that the patent had not been
shown to be invalid. The trial also did not err in holding
PRIOR HISTORY: [**1]
that the generic manufacturer failed to establish a prima
Appealed from: United States District Court for the
facie case of obviousness. Because the district court's
Southern District of New York Judge Denise Cote.
conclusions were not clearly erroneous and were sup-
Takeda Chem. Indus. v. Mylan Labs., Inc., 417 F. Supp.
ported by the record evidence, there was no basis to dis-
2d 341, 2006 U.S. Dist. LEXIS 6710 (S.D.N.Y., 2006)
DISPOSITION: AFFIRMED. OUTCOME: The judgment of the district court was CASE SUMMARY: JUDGES: Before LOURIE, BRYSON, and DYK, Cir- PROCEDURAL POSTURE: Defendant, the manufac-
cuit Judges. Opinion for the court filed by Circuit Judge
turer of a generic version of pioglitazone, a compound
LOURIE. Concurring opinion filed by Circuit Judge
successful in anti-diabetic treatment, appealed from a
holding of the United States District Court for the South-
ern District of New York that the generic manufacturer
OPINION BY: LOURIE
failed to prove by clear and convincing evidence that the
patent claims asserted by plaintiff patent holder were
invalid as obvious under 35 U.S.C.S. § 103, at the time
Alphapharm Pty., Ltd. and Genpharm, Inc. (collec-
OVERVIEW: The generic manufacturer filed an abbre-
tively "Alphapharm") appeal from the decision of the
viated new drug application seeking U.S. Food and Drug
United States District Court for the Southern District of
Administration approval to market its generic product
New York, following a bench trial, that U.S. Patent
under 21 U.S.C.S. § 355(j) et seq. The district court re-
4,687,777 was not shown to be invalid under 35 U.S.C. §
jected the obviousness argument, because the closest
103. Takeda Chem. Indus., Ltd. v. Mylan Labs., 417 F.
prior art compound exhibited negative properties that
Supp. 2d 341 (S.D.N.Y. 2006). Because we conclude
would have directed one of ordinary skill in the art away
[**2] that the district court did not err in determining that
from the compound that was eventually patented as the
the claimed compounds would not have been obvious in
lead compound for anti-diabetic treatment. The most
492 F.3d 1350, *; 2007 U.S. App. LEXIS 15349, **;
light of the prior art, and hence that the patent has not
Diabetes is a disease that is characterized by the
body's inability to regulate blood sugar. It is generally
caused by inadequate levels of insulin--a hormone pro-
duced in the pancreas. Insulin allows blood sugar or glu-
consists essentially of a compound of the
cose, which is derived from food, to enter into the body's
cells and be converted into energy. There are two types of diabetes, known as Type 1 and Type 2. In Type 1 dia-
betes, the pancreas fails to produce insulin, and individu-
als suffering from this type of diabetes must regularly
salt thereof, in association with a pharma-
receive insulin from an external source. In contrast, Type
cologically acceptable carrier, excipient or
2 diabetic individuals produce insulin. However, their
bodies are unable to effectively use the insulin that is
produced. This is also referred to as insulin resistance.
As a result, glucose is unable to enter the cells, thereby
depriving the body of its main source of energy. Type 2 diabetes is the most common form of diabetes--affecting
For purposes of this appeal, the critical portion of
the compound structure is the left moiety of the mole-cule, namely, the ethyl-substituted pyridyl ring. 1 That
In the 1990s, a class of drugs known as thiazolidin-
chemical structure, which has an ethyl substituent
ediones [**3] ("TZDs") was introduced on the market as
(C[2]H[5]) pictorially drawn to the center of the pyridyl
a treatment for Type 2 diabetes. Takeda Chemical Indus-
ring, indicates that the structure covers four possible
tries, Ltd., and Takeda Pharmaceuticals North America,
compounds, [**5] viz., compounds with an ethyl sub-
Inc. (collectively "Takeda") first invented certain TZDs
stituent located at the four available positions on the
in the 1970s. Takeda's research revealed that TZDs acted
pyridyl ring. Takeda, 417 F. Supp. 2d at 360. The for-
as insulin sensitizers, i.e., compounds that ameliorate
mula includes the 3-ethyl compound, 4-ethyl compound,
insulin resistance. Although the function of TZDs was
5-ethyl compound (pioglitazone), and 6-ethyl compound.
not completely understood, TZDs appeared to lower blood glucose levels by binding to a molecule in the nu-
[*1354] Claim 2 of the '777 patent covers the sin-
cleus of the cell known as PPAR-gamma, which acti-
gle compound pioglitazone. That claim, which depends
vates insulin receptors and stimulates the production of
glucose transporters. Takeda, 417 F. Supp. 2d at 348-49.
The transporters then travel to the cellular surface and
enable glucose to enter the cell from the bloodstream. Id.
wherein the compound is 5-4-[2-(5-ethyl-2-pyridyl)ethoxy]benzyl-2,4-
Takeda developed the drug ACTOS (R), which is
used to control blood sugar in patients who suffer from
Type 2 diabetes. ACTOS (R) has enjoyed substantial
commercial success since its launch in 1999. By [*1353]
'777 patent, claim 2. Pioglitazone is referred to as the 5-
2003, it held 47% of the TZD market, and gross sales for
ethyl compound because the ethyl substituent is attached
that year exceeded $ 1.7 billion. Id. at 386. The active
to the 5-position on the pyridyl ring. That portion of the
ingredient in ACTOS (R) is the TZD compound pioglita-
zone, a compound claimed in the patent in suit.
Takeda owns U.S. Patent 4,687,777 [**4] (the "'777
patent") entitled "Thiazolidinedione Derivatives, Useful
1 Pyridine is a "six-membered carbon-
As Antidiabetic Agents." The patent is directed to "com-
containing ring with one carbon replaced by a ni-
pounds which can be practically used as antidiabetic
trogen." Takeda, 417 F. Supp. 2d at 351.
agents having a broad safety margin between pharmacol-ogical effect and toxicity or unfavorable side reactions."
Alphapharm, a generic drug manufacturer, filed an
'777 patent col.1 ll.34-37. The asserted claims are claims
Abbreviated New Drug Application ("ANDA") pursuant
1, 2, and 5. Claim 1 claims a genus of compounds. Claim
to the Hatch-Waxman Act seeking U.S. Food and Drug
5 claims pharmaceutical compositions containing that
Administration ("FDA") approval under 21 U.S.C. §
genus of compounds. Those claims read as follows:
355(j) et seq. to manufacture and sell a generic version of
492 F.3d 1350, *; 2007 U.S. App. LEXIS 15349, **;
pioglitazone. Alphapharm filed a Paragraph IV certifica-
are [**8] such that the subject matter as a whole would
tion with its ANDA pursuant to § 505(j)(2)(B)(ii), [**6]
have been obvious at the time the invention was made to
asserting that the '777 patent is invalid as obvious under
a person having ordinary skill in the art." 35 U.S.C. §
35 U.S.C. § 103. In response, Takeda sued Alphapharm,
103(a). [HN2]Because a patent is presumed to be valid,
along with three other generic drug manufacturers who
35 U.S.C. § 282, the evidentiary burden to show facts
also sought FDA approval to market generic pioglita-
supporting a conclusion of invalidity, which rests on the
zone, alleging that the defendants have infringed or will
accused infringer, is one of clear and convincing evi-
dence. AK Steel Corp. v. Sollac & Ugine, 344 F.3d 1234, 1238-39 (Fed. Cir. 2003). Whether an invention would
On January 17, 2006, the district court commenced a
have been obvious under 35 U.S.C. § 103 is a "question
bench trial solely on the issues of validity and enforce-
of law, reviewed de novo, based upon underlying factual
ability of the '777 patent. Alphapharm advanced its inva-
questions which are reviewed for clear error following a
lidity argument, asserting that the claimed compounds
bench trial." Alza Corp. v. Mylan Labs., Inc., 464 F.3d
would have been obvious at the time of the alleged in-
vention. Alphapharm's obviousness contention rested
entirely on a prior art TZD compound that is referenced
in Table 1 of the '777 patent as compound b. The left moiety of compound b consists of a pyridyl ring with a
Alphapharm raises three main arguments in support
methyl (CH[3]) group attached to the 6-position of the
of its contention that the claims would have been obvi-
ring. That portion of its chemical structure is illustrated
ous. First, Alphapharm asserts that the district court mis-
applied the law, particularly the law governing obvious-ness in the context of structurally similar chemical com-
pounds. According to Alphapharm, the record estab-
Alphapharm asserted that the claimed compounds
lished that compound b was the most effective antidia-
would have been obvious over compound b.
betic compound in the prior art, and thus the court erred by failing to apply [**9] a presumption that one of ordi-
The district court found that Alphapharm failed to
nary skill in the art would have been motivated to make
prove by clear and convincing evidence that the asserted
the claimed compounds. Alphapharm asserts that such a
claims were invalid as obvious under 35 U.S.C. § 103.
conclusion is mandated by our case law, including our en
The court first [**7] concluded that there was no moti-
banc decision in In re Dillon, 919 F.2d 688 (Fed. Cir.
vation in the prior art to select compound b as the lead
1990). Second, Alphapharm argues that the court erred in
compound for antidiabetic research, and that the prior art
determining the scope and content of the prior art, in
taught away from its use. As such, the court concluded
particular, whether to include the prosecution history of
that Alphapharm failed to make a prima facie case of
the prior '779 patent. Lastly, Alphapharm assigns error to
obviousness. The court continued its analysis and found
numerous legal and factual determinations and certain
that even if Alphapharm succeeded in making a prima
evidentiary rulings that the court made during the course
facie showing, Takeda would still prevail because any
prima facie case of obviousness was rebutted by the un-expected results of pioglitazone's nontoxicity. The court
Takeda responds that the district court correctly de-
then rendered judgment in favor of Takeda. The district
termined that Alphapharm failed to prove by clear and
court also held that the '777 patent had not been procured
convincing evidence that the asserted claims are invalid
though inequitable conduct. That decision has been sepa-
as obvious. Takeda contends that there was overwhelm-
rately appealed and has been affirmed in a decision is-
ing evidence presented at trial to support the court's con-
clusion that no motivation existed in the prior art for one of ordinary skill in the art to select compound b as a lead
Alphapharm timely appealed. We have jurisdiction
compound, and even if there was, that the unexpected
results of pioglitazone's improved toxicity would have
rebutted any prima facie showing of obviousness. Ta-
keda further argues that all of Alphapharm's [**10] re-
maining challenges to the district court's legal and factual rulings are simply without merit.
In this appeal, we are presented with one issue,
namely, whether the asserted [*1355] claims of the '777
We agree with Takeda that the district court did not
patent would have been obvious under 35 U.S.C. § 103
err in concluding that the asserted claims of the '777 pat-
at the time the invention was made. [HN1]An invention
ent would not have been obvious. The Supreme Court
is not patentable, inter alia, "if the differences between
recently addressed the issue of obviousness in KSR In-
the subject matter sought to be patented and the prior art
ternational Co. v. Teleflex Inc., 127 S. Ct. 1727, 167 L.
492 F.3d 1350, *; 2007 U.S. App. LEXIS 15349, **;
Ed. 2d 705 (2007). The Court stated that[HN3] the
fied, however, that in order to find a prima facie case of
Graham v. John Deere Co. of Kansas City, 383 U.S. 1,
unpatentability in such instances, a showing that the
86 S. Ct. 684, 15 L. Ed. 2d 545 (1966), factors still con-
"prior art would have suggested making the specific mo-
trol an obviousness inquiry. Those factors are: 1) "the
lecular modifications necessary to achieve the claimed
scope and content of the prior art"; 2) the "differences
invention" was also required. Id. (citing In re Jones, 958
between the prior art and the claims"; 3) "the level of
F.2d 347 (Fed. Cir. 1992); Dillon, 919 F.2d 688;
ordinary skill in the pertinent art"; and 4) objective evi-
Grabiak, 769 F.2d 729; In re Lalu, 747 F.2d 703 (Fed.
dence of nonobviousness. KSR, 127 S. Ct. at 1734 (quot-
That test for prima facie obviousness for chemical
In a thorough and well-reasoned opinion, albeit ren-
compounds is consistent with the legal principles enunci-
dered before KSR was decided [*1356] by the Supreme
ated in KSR. 2 While the KSR Court rejected a rigid ap-
Court, the district court made extensive findings of fact
plication of the teaching, suggestion, or motivation
and conclusions of law as to the four Graham factors.
("TSM") test in an obviousness [**13] inquiry, the
Alphapharm's arguments challenge the court's determina-
Court acknowledged the importance of identifying "a
tions with respect to certain of these factors, which we
reason that would have prompted a person of ordinary
skill in the relevant field to combine [*1357] the ele-ments in the way the claimed new invention does" in an
1. Differences Between the Prior Art and the Claims
obviousness determination. KSR, 127 S. Ct. at 1731.
a. Selection of Compound b as Lead [**11] Com-
Moreover, the Court indicated that there is "no necessary
inconsistency between the idea underlying the TSM test and the Graham analysis." Id. As long as the test is not
Alphapharm's first argument challenges the court's
applied as a "rigid and mandatory" formula, that test can
determination with regard to the "differences between the
provide "helpful insight" to an obviousness inquiry. Id.
prior art and the claims." Alphapharm contends that the
Thus, in cases involving new chemical compounds, it
court erred as a matter of law in holding that the ethyl-
remains necessary to identify some reason that would
substituted TZDs were nonobvious in light of the closest
have led a chemist to modify a known compound in a
prior art compound, compound b, by misapplying the
particular manner to establish prima facie obviousness of
law relating to obviousness of chemical compounds.
We disagree. Our case law concerning prima facie
obviousness of structurally similar compounds is well-
2 We note that the Supreme Court in its KSR
established. We have held that [HN4]"structural similar-
opinion referred to the issue as whether claimed
ity between claimed and prior art subject matter, proved
subject matter "was" or "was not" obvious. Since
by combining references or otherwise, where the prior art
35 U.S.C. § 103 uses the language "would have
gives reason or motivation to make the claimed composi-
been obvious," and the Supreme Court in KSR
tions, creates a prima facie case of obviousness." Dillon,
did consider the particular time at which obvi-
919 F.2d at 692. In addition to structural similarity be-
ousness is determined, we consider that[HN7] the
tween the compounds, a prima facie case of obviousness
Court did not in KSR reject the standard statutory
also requires a showing of "adequate support in the prior
formulation of the inquiry whether [**14] the
art" for the change in structure. In re Grabiak, 769 F.2d
claimed subject matter "would have been obvious
at the time the invention was made." 35 U.S.C. § 103. Hence, we will continue to use the statutory
We elaborated on this requirement in the case of In re Deuel, 51 F.3d 1552, 1558 (Fed. Cir. 1995), where we stated that[HN5] "[n]ormally a prima facie case of obvi-
We agree with Takeda and the district court that Al-
ousness is based [**12] upon structural similarity, i.e.,
phapharm failed to make that showing here. Alphapharm
an established structural relationship between a prior art
argues that the prior art would have led one of ordinary
compound and the claimed compound." That is so be-
skill in the art to select compound b as a lead compound.
cause close or established "[s]tructural relationships may
By "lead compound," we understand Alphapharm to re-
provide the requisite motivation or suggestion to modify
fer to a compound in the prior art that would be most
known compounds to obtain new compounds." Id.
promising to modify in order to improve upon its
[HN6]A known compound may suggest its homolog,
antidiabetic activity and obtain a compound with better
analog, or isomer because such compounds "often have
activity. 3 Upon selecting that compound for antidiabetic
similar properties and therefore chemists of ordinary skill
research, Alphapharm asserts that one of ordinary skill in
would ordinarily contemplate making them to try to ob-
the art would have made two obvious chemical changes:
tain compounds with improved properties." Id. We clari-
first, homologation, i.e., replacing the methyl group with
492 F.3d 1350, *; 2007 U.S. App. LEXIS 15349, **;
an ethyl group, which would have resulted in a 6-ethyl
rivatives" ("Sodha II"). The Sodha II reference disclosed
compound; and second, "ring-walking," or moving the
data relating to hypoglycemic activity and plasma
ethyl substituent to another position on the ring, the 5-
triglyceride lowering activity for 101 TZD compounds.
position, thereby leading to the discovery of pioglita-
[**17] Those compounds did not include pioglitazone,
zone. Thus, Alphapharm's obviousness argument clearly
but included compound b. Significantly, Sodha II identi-
depends on a preliminary finding that one of ordinary
fied three specific compounds that were deemed most
skill in the art would have selected [**15] compound b
favorable in terms of toxicity and activity. Notably,
compound b was not identified as one of the three most
favorable compounds. On the contrary, compound b, was
3 The parties do not dispute that compound b
singled out as causing "considerable increases in body
was the closest prior art compound. Thus, the le-
gal question is whether or not the claimed subject
The court also considered Takeda's '779 patent. That
matter would have been obvious over that com-
patent covers a subset of compounds originally included
pound. We will, however, use Alphapharm's ter-
in the '200 patent application, namely, TZD compounds
minology of "lead compound" in this opinion, de-
"where the pyridyl or thiazolyl groups may be substi-
ciding the appeal as it has been argued.
tuted." Id. at 353. The broadest claim of the '779 patent
The district court found, however, that one of ordi-
covers over one million compounds. Id. at 378. Com-
nary skill in the art would not have selected compound b
pound b was specifically claimed in claim 4 of the pat-
as the lead compound. In reaching its determination, the
ent. The court noted that a preliminary amendment in the
court first considered Takeda's U.S. Patent 4,287,200
prosecution history of the patent contained a statement
(the "'200 patent"), which was issued on September 1,
that "the compounds in which these heterocyclic rings
1981, and its prosecution history. The court found that
are substituted have become important, especially [com-
the '200 patent "discloses hundreds of millions of TZD
compounds." 4 Takeda, 417 F. Supp. 2d at 378. The pat-
Based on the prior art as a whole, however, the court
ent specifically identified fifty-four compounds, includ-
found that a person of ordinary skill in the art would not
ing compound b, that were synthesized according to the
have selected compound b as a lead compound for
procedures described in the patent, but did not disclose
antidiabetic treatment. Although [**18] the prosecution
experimental data or test results for any of those com-
history of the '779 patent included the statement that
pounds. The prosecution history, however, disclosed test
characterized compound b as "especially important," the
results for nine specific compounds, including compound
court found that any suggestion to select compound b
b. That information was provided to the examiner in re-
was essentially negated by the disclosure of the Sodha II
sponse to a rejection in [**16] order to show that the
reference. The court reasoned that one of ordinary skill
claimed compounds of the '200 patent were superior to
in the art would not have chosen compound b, notwith-
the known compounds that were disclosed in a cited ref-
standing the statement in the '779 patent prosecution his-
erence. The court, however, found nothing in the '200
tory, "given the more exhaustive and reliable scientific
patent, or in its file history, to suggest to one of ordinary
analysis presented by Sodha II, which taught away from
skill in the art that those nine compounds, out of the
compound b, and the evidence from all of the TZD pat-
hundreds of millions of compounds covered by the pat-
ents that Takeda filed contemporaneously with the '779
ent application, were the best performing compounds as
[p]atent showing that there were many promising, broad
antidiabetics, and hence targets for modification to seek
avenues for further research." Id. at 380.
The court found that the three compounds that the
4 Three divisional applications derive from the
Sodha II reference identified as "most favorable" and
'200 patent. Those applications matured into U.S.
"valuable for the treatment of maturity-onset diabetes,"
Patent 4,340,605, U.S. Patent 4,438,141, and U.S.
not compound b, would have served as the best "starting
Patent No. 4,444,779 (the "'779 Patent"). The
point for further investigation" to a person of ordinary
'779 patent is of particular relevance in this ap-
skill in the art. Id. at 376. Because diabetes is a chronic
peal and is discussed below. Takeda, 417 F.
disease and thus would require long term treatment, the
court reasoned that researchers would have been dis-suaded from selecting a lead compound that [**19] ex-
[*1358] The court next considered an article that
hibited negative effects, such as toxicity, or other adverse
was published the following year in 1982 by T. Sodha et
side effects, especially one that causes "considerable
al. entitled "Studies on Antidiabetic Agents. II. Synthesis
increases in body weight and brown fat weight." Id. at
376-77. Thus, the court determined that the prior art did
benzyl]thiazolidine-2,4-dione (ADD-3878) and Its De-
not suggest to one of ordinary skill in the art that com-
492 F.3d 1350, *; 2007 U.S. App. LEXIS 15349, **;
pound b would be the best candidate as the lead com-
closed a broad selection of compounds any one of which
could have been selected as a lead compound for further investigation. Significantly, the closest prior art com-
Admissions from Alphapharm witnesses further but-
pound (compound b, the 6-methyl) exhibited negative
tressed the court's conclusion. Dr. Rosenberg, head of
properties that would have directed one of ordinary skill
Alphapharm's intellectual property department, testified
in the art away from that compound. Thus, this case fails
as a 30(b)(6) witness on behalf of Alphapharm. In dis-
to present the type of situation contemplated by the Court
cussing Sodha II, Dr. Rosenberg admitted that there was
when it stated that an invention may be deemed obvious
nothing in [*1359] the article that would recommend
if it was "obvious to try." The evidence showed that it
that a person of ordinary skill in the art choose com-
pound b over other compounds in the article that had the same efficacy rating. Dr. Rosenberg, acknowledging that
Similarly, Alphapharm's reliance on Pfizer fares no
compound b had the negative side effects of increased
better. [**22] In Pfizer, we held that certain claims cov-
body weight and brown fat, also admitted that a com-
ering the besylate salt of amlodipine would have been
pound with such side effects would "presumably not" be
obvious. The prior art included a reference, referred to as
a suitable candidate compound for treatment of Type II
the Berge reference, that disclosed a genus of pharma-
diabetes. Alphapharm's expert, Dr. Mosberg, concurred
ceutically acceptable anions that could be used to form
in that view at his deposition when he admitted that a
pharmaceutically acceptable acid addition salts, as well
medicinal chemist would find [**20] such side effects
as other publications that disclosed the chemical charac-
teristics of the besylate salt. Pfizer, 480 F.3d at 1363. Noting that our conclusion was based on the "particular-
Moreover, another Alphapharm 30(b)(6) witness,
ized facts of this case," we found that the prior art pro-
Barry Spencer, testified at his deposition that in review-
vided [*1360] "ample motivation to narrow the genus
ing the prior art, one of ordinary skill in the art would
of 53 pharmaceutically-acceptable anions disclosed by
have chosen three compounds in Sodha II as lead com-
Berge to a few, including benzene sulphonate." Id. at
pounds for research, not solely compound b. In addition,
1363, 1367. Here, the court found nothing in the prior art
Takeda's witness, Dr. Morton, testified that at the time
to narrow the possibilities of a lead compound to com-
Sodha II was published, it was known that obesity con-
pound b. In contrast, the court found that one of ordinary
tributed to insulin resistance and Type 2 diabetes. Thus,
skill in the art would have chosen one of the many com-
one of ordinary skill in the art would have concluded that
pounds disclosed in Sodha II, of which there were over
Sodha II taught away from pyridyl compounds because it
ninety, that "did not disclose the existence of toxicity or
associated adverse side effects with compound b.
side effects, and to engage in research to increase the
We do not accept Alphapharm's assertion that KSR,
efficacy and confirm the absence of toxicity of those
as well as another case recently decided by this court,
compounds, rather than to choose as a starting point
Pfizer, Inc. v. Apotex, Inc., 480 F.3d 1348 (Fed. Cir.
[**23] a compound with identified adverse effects."
2007), mandates reversal. Relying on KSR, Alphapharm
Thus, Pfizer does not control this case.
argues that the claimed compounds would have been
Based on the record before us, we conclude that the
obvious because the prior art compound fell within "the
district court's fact-findings were not clearly erroneous
objective reach of the claim," and the evidence demon-
and were supported by evidence in the record. Moreover,
strated that using the techniques of homologation and
we reject the assertion that the court failed to correctly
ring-walking would have been "obvious to try." Addi-
apply the law relating to prima facie obviousness of
tionally, Alphapharm argues that our holding in Pfizer,
chemical compounds. Because Alphapharm's obvious-
where we found obvious certain claims [**21] covering
ness argument rested entirely on the court making a pre-
a particular acid-addition salt, directly supports its posi-
liminary finding that the prior art would have led to the
selection of compound b as the lead compound, and Al-
We disagree. The KSR Court recognized that[HN8]
phapharm failed to prove that assertion, the court did not
"[w]hen there is a design need or market pressure to
commit reversible error by failing to apply a presumption
solve a problem and there are a finite number of identi-
of motivation. We thus conclude that the court did not err
fied, predictable solutions, a person of ordinary skill has
in holding that Alphapharm failed to establish a prima
good reason to pursue the known options within his or
facie case of obviousness. See Eli Lilly & Co. v. Zenith
her technical grasp." KSR, 127 S. Ct. at 1732. In such
Goldline Pharms., 471 F.3d 1369 (Fed. Cir. 2006) (af-
circumstances, "the fact that a combination was obvious
firming the district court's finding of nonobviousness
to try might show that it was obvious under § 103." Id.
upon concluding, in part, that the prior art compound
That is not the case here. Rather than identify predictable
would not have been chosen as a lead compound).
solutions for antidiabetic treatment, the prior art dis-
b. Choice of the Claimed Compounds
492 F.3d 1350, *; 2007 U.S. App. LEXIS 15349, **;
Even if Alphapharm had established that preliminary
data insufficient to show that the same effects would
finding, and we have concluded that it did [**24] not,
the record demonstrates that Alphapharm's obviousness
Alphapharm relies on In re Wilder, 563 F.2d 457
argument fails on a second ground. The district court
(CCPA 1977), for the proposition that differences in a
found nothing in the prior art to suggest making the spe-
chemical compound's properties, resulting from a small
cific molecular modifications to compound b that are
change made to the molecule, are reasonably expected to
necessary to achieve the claimed compounds. In reaching
vary by degree and thus are insufficient to rebut a prima
that conclusion, the court first found that the process of
facie case of obviousness. In Wilder, our predecessor
modifying lead compounds was not routine at the time of
court affirmed the Board's holding that a claimed com-
the invention. Takeda, 417 F. Supp. 2d at 380. Dr. Mos-
pound, which was discovered to be useful as a rubber
berg opined that the steps of homologation and ring-
antidegradant and was also shown to be nontoxic to hu-
walking were "routine steps in the drug optimization
man skin, would have been obvious in light of its ho-
process," but the court found that testimony unavailing in
molog and isomer that were disclosed in the prior art.
light of the contrary, more credible, testimony offered by
The evidence showed that the homolog was similarly
Takeda's experts. Id. at 381. In addition, the court relied
nontoxic to the human skin, whereas the isomer was
on Dr. Rosenberg's admission that a person of ordinary
toxic. [**27] The court held that [HN9]"one who claims
skill in the art would "look at a host of substituents, such
a compound, per se, which is structurally similar to a
as chlorides, halides and others, not just methyls" in
prior art compound must rebut the presumed expectation
that the structurally similar compounds have similar
Pioglitazone differs from compound b in two re-
properties." Id. at 460. While recognizing that the differ-
spects, and one would have to both homologate the
ence between the isomer's toxicity and the nontoxicity of
methyl group of compound b and move the resulting
the homolog and claimed compound "indicate[d] some
ethyl group to the 5-position on the pyridyl ring in order
degree of unpredictability," the court found that the ap-
to obtain pioglitazone. With regard to homologation, the
pellant failed to "point out a single actual difference in
court [**25] found nothing in the prior art to provide a
properties between the claimed compound and the homo-
reasonable expectation that adding a methyl group to
logue," and thus failed to rebut the presumption. Wilder,
compound b would reduce or eliminate its toxicity.
Based on the test results of the numerous compounds
We would note that since our Wilder decision, we
disclosed in Sodha II, the court concluded that "homolo-
have cautioned "that [HN10]generalization should be
gation had no tendency to decrease unwanted side ef-
avoided insofar as specific chemical structures are al-
fects" and thus researchers would have been inclined "to
leged to be prima facie obvious one from the other,"
focus research efforts elsewhere." Id. at 383. Indeed,
Grabiak, 769 F.2d at 731. In addition to this caution, the
several other compounds exhibited similar or better po-
facts of the present case differ significantly from the
tency than compound b, and one compound in particular,
facts of Wilder. Here, the court found that pioglitazone
compound 99, that had no identified problems differed
exhibited unexpectedly superior properties over the prior
significantly [*1361] from compound b in structure. Id.
art compound b. Takeda, 417 F. Supp. 2d at 385. The
at 376 n.51. Moreover, Dr. Mosberg agreed with Ta-
court considered a report entitled "Preliminary Studies
keda's expert, Dr. Danishefsky, that the biological activi-
on Toxicological Effects of Ciglitazone-Related Com-
ties of various substituents were "unpredictable" based
pounds [**28] in the Rats" that was presented in Febru-
on the disclosure of Sodha II. Id. at 384-85. The court
ary 1984 by Dr. Takeshi Fujita, then-Chief Scientist of
also found nothing in the '200 and '779 patents to suggest
Takeda's Biology Research Lab and co-inventor of the
to one of ordinary skill in the art that homologation
'777 patent. That report contained results of preliminary
would bring about a reasonable expectation of success.
toxicity studies that involved selected compounds, in-
As for ring-walking, the court found that there was
cluding pioglitazone and compound b. Compound b was
no reasonable expectation in the art that changing the
shown to be "toxic to the liver, heart and erythrocytes,
positions of a substituent on a pyridyl ring would result
among other things," whereas pioglitazone was "com-
in beneficial changes. [**26] Dr. Mosberg opined that
paratively potent" and "showed no statistically signifi-
the process of ring-walking was "known" to Takeda, but
cant toxicity." Id. at 356-57. During the following
the court found that testimony inapt as it failed to support
months, Takeda performed [*1362] additional toxicity
a reasonable expectation to one of ordinary skill in the
studies on fifty compounds that had been already synthe-
art that performing that chemical change would cause a
sized and researched by Takeda, including pioglitazone.
compound to be more efficacious or less toxic. Id. at 382.
The compounds were tested for potency and toxicity.
Moreover, Dr. Mosberg relied on the efficacy data of
The results were presented in another report by Fujita
phenyl compounds in Sodha II, but the court found those
entitled "Pharmacological and Toxicological Studies of
492 F.3d 1350, *; 2007 U.S. App. LEXIS 15349, **;
Ciglitazone and Its Analogues." Pioglitazone was shown
steps of homologation and ring-walking, to synthesize
to be the only compound that exhibited no toxicity, al-
the claimed compounds. Because the court's conclusions
though many of the other compounds were found to be
are not clearly erroneous and are supported by the record
evidence, we find no basis to disturb them.
Thus, the court found that there was no reasonable
The court properly concluded that Alphapharm did
expectation that pioglitazone would possess the desirable
not make out a prima facie case of obviousness because
property of nontoxicity, particularly in light of the toxic-
Alphapharm [*1363] failed to adduce evidence that
ity [**29] of compound b. The court's characterization
compound b would have been selected as the lead com-
of pioglitazone's unexpected results is not clearly errone-
pound and, even if that preliminary showing had been
ous. As such, Wilder does not aid Alphapharm because,
made, it failed to show that there existed a reason, based
unlike the homolog and claimed compound in Wilder
on what was known at the time of the invention, to per-
that shared similar properties, pioglitazone was shown to
form the chemical modifications necessary to achieve the
differ significantly from compound b, of which it was
not a homolog, in terms of toxicity. Consequently, Ta-
In light of our conclusion that Alphapharm failed to
keda rebutted any presumed expectation that compound
prove that the claimed compounds would have been
b and pioglitazone would share similar properties.
prima facie obvious, we need not consider any objective
Alphapharm also points to a statement Takeda made
during the prosecution of the '779 patent as evidence that
there was a reasonable expectation that making changes
5 The concurrence, while agreeing that the ques-
to the pyridyl region of compound b would lead to "bet-
tion of the "overbreadth" of claims 1 and 5 has
ter toxicity than the prior art." During prosecution of the
been waived, states further that the 6-ethyl com-
'779 patent, in response to an enablement rejection, Ta-
pound, which is within the scope of claims 1 and
keda stated that "there should be no reason in the instant
5, has not been [**32] shown to possess unex-
case for the Examiner to doubt that the claimed com-
pected results sufficient to overcome a prima fa-
pounds having the specified substituent would function
cie case of obviousness, and hence claims 1 and 5
as a hypolipidemic and hypoglycemic agent as specified
are likely invalid as obvious. Since waiver is suf-
in the instant disclosure." That statement, however, indi-
ficient to answer the point being raised, no further
cates only that changes to the left moiety of a lead com-
comment need be made concerning its substance.
pound would create compounds with the same properties
2. Scope and Content of the Prior Art
as the [**30] compounds of the prior art; it does not represent that lower toxicity would result. And even if
Alphapharm also assigns error to the district court's
the statement did so represent, it does not refer to any
determination regarding the scope and content of the
specific substituent at any specific position of TZD's left
prior art. Alphapharm asserts that the court excluded the
moiety as particularly promising. As the court correctly
prosecution history of the '779 patent from the scope of
noted, the compounds disclosed in the '779 patent in-
the prior art after wrongly concluding that it was not ac-
cluded a variety of substituents, including lower alkyls,
cessible to the public. Takeda responds that the court
halogens, and hydroxyl groups, attached to a pyridyl or
clearly considered the '779 patent prosecution history,
thiazolyl group. As discussed supra, the district court
which was admitted into evidence on the first day of tes-
found that the claims encompassed over one million
timony. Takeda urges that the court's consideration of the
compounds. Thus, we disagree with Alphapharm that
prosecution history is apparent based on its extensive
that statement provided a reasonable expectation to one
analysis of the '779 patent and the file history that ap-
of ordinary skill in the art that performing the specific
steps of replacing the methyl group of the 6-methyl com-
We agree with Takeda that the district court did not
pound with an ethyl group, and moving that substituent
err in its consideration of the scope of the prior art. As
to the 5-position of the ring, would have provided a
discussed above, the court considered the prosecution
broad safety margin, particularly in light of the district
history, and even expressly considered one of the key
court's substantiated findings to the contrary.
statements in the prosecution [**33] history upon which
We thus conclude that Alphapharm's challenges fail
Alphapharm relies in support of its position that com-
to identify grounds for reversible error. The court prop-
pound b would have been chosen as the lead compound.
erly considered the teachings of the prior art and made
Takeda, 417 F. Supp. 2d at 378. In considering the
credibility determinations regarding the witnesses at trial.
prosecution history of the '779 patent, the court noted
[**31] We do not see any error in the district court's de-
that Takeda filed a preliminary amendment on March 15,
termination that one of ordinary skill in the art would not
1983, in which its prosecuting attorney stated that "the
have been prompted to modify compound b, using the
compounds in which these heterocyclic rings are substi-
492 F.3d 1350, *; 2007 U.S. App. LEXIS 15349, **;
tuted have become important, especially [the 6-methyl
ent No. 4,287,200 ("'200 patent"). Unfortunately our law
compound]." Id. The court rejected Alphapharm's asser-
concerning when a species [**35] is patentable over a
tion that that statement supported the conclusion that
genus claimed in the prior art is less than clear. It is, of
compound b would have been selected as a lead com-
course, well established that a claim to a genus does not
pound. Rather, the court found that viewing the prior art
necessarily render invalid a later claim to a species
as a whole, the prior art showed "that Takeda was ac-
within that genus. See Eli Lilly & Co. v. Bd. of Regents of
tively conducting research in many directions, and had
Univ. of Wash., 334 F.3d 1264, 1270 (Fed. Cir. 2003). In
not narrowed its focus to compound b." Id. at 379. Thus,
my view a species should be patentable over a genus
while the district court may have incorrectly implied that
claimed in the prior art only if unexpected results have
prosecution histories are not accessible to the public, see
been established. Our case law recognizes the vital im-
id. at n.59, see also Custom Accessories, Inc. v. Jeffrey-
portance of a finding of unexpected results, both in this
Allan Indus., 807 F.2d 955 (Fed. Cir. 1986)
context and in the closely related context where a prior
([HN11]"[t]he person of ordinary skill is a hypothetical
art patent discloses a numerical range and the patentee
person who is presumed to be aware of all the pertinent
seeks to claim a subset of that range. See Application of
prior art"), the court nonetheless considered [**34] the
Petering, 301 F.2d 676, 683, 49 C.C.P.A. 993, 1962 Dec.
prosecution history of the '779 patent in its obviousness
Comm'r Pat. 232 (C.C.P.A. 1962) (species found pat-
analysis and accorded proper weight to the statements
entable when genus claimed in prior art because unex-
contained therein. Thus, any error committed by the
pected properties of the species were shown); see also
court in this regard was harmless error.
Pfizer, Inc. v. Apotex, Inc., 480 F.3d 1348, 1371 (Fed. Cir. 2007) (relying on lack of unexpected results in de-
We have considered Alphapharm's remaining argu-
termining that species claim was obvious in view of prior
ments and find none that warrant reversal of the district
art genus claim); In re Woodruff, 919 F.2d 1575, 1578
(Fed. Cir. 1990) (when applicant claims a subset of a
range disclosed in a prior art patent, the applicant [**36] must generally show that "the claimed range achieves
We affirm the district court's determination that
unexpected results relative to the prior art range.").
claims 1, 2, and 5 of the '777 patent have not been shown to have been obvious and hence invalid.
While the 5-ethyl compound (pioglitazone) is within
the scope of the '200 patent, there is clear evidence, as
the majority correctly finds, of unexpected results re-
garding that compound, and therefore its validity is not
CONCUR BY: DYK
in question on this ground. However, at oral argument
the patentee admitted that the prior art '200 patent also
generically covers the 6-ethyl compound, which is within
the scope of claims 1 and 5 of the '777 patent, and admit-ted that there is no evidence of unexpected results for the
I join the opinion of the court insofar as it upholds
6-ethyl compound. Under such circumstances, I believe
the district court judgment based on a determination that
that the 6-ethyl is likely obvious, and consequently
a claim to pioglitazone (the 5-ethyl compound) would be
claims 1 and 5 are likely invalid for obviousness. How-
non-obvious over the prior art. The problem is that only
ever, the argument as to the overbreadth of claims 1 and
one of the three claims involved here--claim 2--is limited
5 has been waived, because it was not raised in the open-
to pioglitazone. In my view, the breadth of the other two
ing brief. In any event, as a practical matter, the judg-
claims, claims 1 and 5 of U.S. Patent No. 4,867,777
ment finding that the appellants' filing of the ANDA for
("'777 patent")--which are also referenced in the judg-
pioglitazone is an infringement and barring the making
of pioglitazone is supported by the finding that claim 2
All of the compounds claimed in claims 1, 2 and 5
standing alone is not invalid and is infringed.
were included in generic claims in the prior art U.S. Pat-
Procédure N° 009 Rédacteurs Date Validation Dr A. BARONDEAU-LEURET, SAU Chalon/Saône Approbation Conférences d’actualisation SFAR 1998, pp 635-47Elsevier, Paris Sources Révision de la 3ème Conférence de consensus : Prise en charge des crises d’asthme aiguës graves de l’adulte et de OBJET : Préciser les éléments de gravité et la prise
Nuclear Medicine Myocardial Perfusion Patient Handout You have been scheduled for a myocardial perfusion study so your doctors can evaluate the blood flow to your heart muscle during exercise (stress) and rest. This test is usually performed in two parts on the same day. Pictures of your heart will be taken on the gamma camera, once at “rest,” and again after “stress.” For the stres