STIVARGA® (regorafenib) Survives Challenge at PTAB: Difference = One Fluorine

February 8, 2017

FUSTIBAL LLC (Petitioner)  v. BAYER HEALTHCARE LLC, (Patent Owner)

Case IPR2016-01490
Patent 8,637,553 B2

Link to PTAB Decision Denying Institution

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Regorafenib (API of STIVARGA®)
Regorafenib.svg
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Prior art compound = Sorafenib (Nexavar®)
Sorafenib structure
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Summary

The Patent Trial and Appeal Board (PTAB) declined Fustibal’s petition to Institute an Inter Partes Review (IPR) trial of Bayer’s U.S. Patent 8,637,553 B2 claiming regorafenib (API of STIVARGA®).

The PTAB concluded that Fustibal did not establish a reasonable likelihood that Bayer’s claims are rendered as anticipated or obvious by the prior art.

At first glance, Fustibal’s petition looks strong because Bayer’s regorafenib merely differs from the prior art’s sorafenib by one fluorine on the center aromatic ring.  [Sorafenib does not have the extra fluorine] Fustibal argues that Bayer merely added fluorine as an obvious modification.

Fustibal challenged both regorafenib’s novelty and non-obviousness over the closest prior art publication WO 00/42012 to Riedl.

PTAB’s Deference to the Patent Examiner

The PTAB declined to second-guess the Patent Examiner because the examiner repeatedly reconsidered the prior art patent (Riedl) during prosecution and expressly allowed the claims over the prior art.

The patent examiner provided the following Reasons for Allowance:

“After a thorough search, the closest prior art, WO 00/42012 to Riedl, et al. was found to teach similar phenyl-urea derivatives as kinase inhibitors.  However, the WO document fails to teach or render obvious the instant claimed compounds according to Formula (I), and does not fairly suggest their salts or pharmaceutical compositions.”

The PTAB further declined to institute an IPR trial on the merits.

Anticipation / Novelty – §102

Even though the prior art recited a genus that would encompass regorafenib, the PTAB determined that the prior art genus was too vast to anticipate regorafenib.

  • Where “the number of compounds actually disclosed by [the asserted prior art] numbers in the millions (including all proposed alternative substituents),” the prior art genus cannot anticipate a later species claim.  (Eli Lilly & Co. v. Zenith Goldline Pharm., Inc., 471 F.3d 1369, 1376 (Fed. Cir. 2006))
  • Where a reference does not “clearly and unequivocally disclose the claimed compound,” to be anticipatory reference under 35 U.S.C. § 102, it must, nevertheless, “direct those skilled in the art to the compound without any need for picking, choosing, and combining various disclosures not directly related to each other by the teachings of the cited reference.”  In re Arkley, 455 F.2d 586, 587 (CCPA 1972).  For the reasons set forth at pages 9–16 of the Preliminarily Response, we agree with Patent Owner that the genus relied on by Petitioner, having “‘eight individual chemical compounds possible when substituting a halogen”—F, Cl, Br, or I—at position 2/2’ or 3/3’ of the central ring of sorafenib, does not exist in Riedl, and only results from Petitioner’s improper picking and choosing disparate aspects of the disclosure.  See Prelim. Resp. 13–15 (quoting Pet. 16).

Obviousness – § 103

As expected, the PTAB applied the two-prong inquiry [“lead compound analysis”] from Otsuka Pharm. Co. v. Sandoz, Inc., 678 F.3d 1280, 1291–93 (Fed. Cir. 2012) for determining whether a claimed compound would have been obvious over prior art compounds.  First, the PTAB determined whether a chemist of ordinary skill would have selected the asserted prior art compounds as lead compounds, or starting points, for further development efforts.  Second, the PTAB analyzed whether there was a reason to modify a lead compound to make the claimed compound with a reasonable expectation of success.

The PTAB noted that Fustibal’s petition did not include a “mandatory” lead compound analysis.  Fustibal merely assumed – without explanation – that a person of ordinary skill in the art would select sorafenib as a lead compound for modification.

The PTAB did not discern a reason to select from Sorafenib from the prior art Riedl reference because the reference does not highlight any of the vast number of disclosed compounds is having particularly beneficial properties or present any enzymatic or biological data.

No reason to modify Sorafenib by adding one fluorine to arrive at Regorafenib

Fustibal’s petition did not provide the necessary reasons why a chemist would modify the prior art in that particular manner. Even though the prior art discloses potential benefits of adding one or more fluorine atoms, the prior art merely indicates that the prior art compound can be halogenated.

The PTAB did not read the prior art to suggest that any fluorine substitution will result in improved pharmacological properties.  The PTAB agreed with the patent owner that if improvements by adding fluorine were always true, then “all pharmaceutical compounds would be fluorinated, which is plainly not the case.”  Meanwhile, the compound already had a trifluoromethyl group on it.  The petitioner could not explain why a chemist would add multiple additional fluorine atoms.

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Notes:

On November 22, 2013, the U. S. Food and Drug Administration approved sorafenib (NEXAVAR tablets, Bayer Healthcare Pharmaceuticals Inc.) for the treatment of locally recurrent or metastatic, progressive, differentiated thyroid carcinoma (DTC) refractory to radioactive iodine treatment. The FDA previously approved Sorafenib for treatment of renal cell carcinoma (2005) and hepatocellular carcinoma (2007).

http://www.fda.gov/Drugs/InformationOnDrugs/ApprovedDrugs/ucm376547.htm

The U.S. Food and Drug Administration approved Stivarga® (regorafenib) on September 27, 2012 to treat patients with colorectal cancer that has progressed after treatment and spread to other parts of the body (metastatic). http://www.fda.gov/NewsEvents/Newsroom/PressAnnouncements/ucm321271.htm

PTAB Denies Amneal’s Request to Institute IPR Against Hospira’s Dexmedetomidine Pharmaceutical Composition Patent

IPR2016-01580

AMNEAL PHARMACUTICALS LLC, (Petitioner)
v.
HOSPIRA INC. (Patent Owner)

February 3, 2017

Illustrative Claim of U.S. Patent 8,648,106 B2:

1.    A ready to use liquid pharmaceutical composition for parenteral administration to a subject, comprising dexmedetomidine or a pharmaceutically acceptable salt thereof disposed within a sealed glass container, wherein the liquid pharmaceutical composition when stored in the glass container for at least five months exhibits no more than about 2% decrease in the concentration of dexmedetomidine.

Correcting an Enantiomer without Invalidating a Patent is Possible

Inventors may correct a mistakenly claimed enantiomer, without invalidating their patent if their patent application describes the compound in other ways showing that they were otherwise in possession of the compound.  The US Court of Appeals for the Federal Circuit allowed such a correction in a dispute over daptomycin between Cubist and Hospira.

Cubist Pharmaceuticals, Inc. v. Hospira, Inc., (Fed. Cir. November 12, 2015)

Summary

Cubist’s correction of daptomycin’s mistaken enantiomer didn’t invalidate their patent’s claims because the patent specification described the compound in other ways to show that the inventors “were in possession of the invention” anyway.

Daptomycin_

Daptomycin Patent – RE 39,071

  • The case involved Cubist’s antibiotic daptomycin, US Patent RE 39,071 [Re-issue of US 5,912,226], which Cubist acquired from Eli Lilly.
  • S. Patent RE 39,071 claimed the pharmaceutical composition of CUBICIN® (daptomycin for injection) and expired in June 2016 [June 2011 + 5 years Hatch-Waxman Patent Term Restoration].
  • Eli Lilly originally filed the daptomycin patent application and the USPTO granted of US 5,912,226, which described daptomycin’s having the L‑isomer of asparagine.
  • Cubist requested a U.S. Patent and Trademark Office Certificate of Correction when they discovered that daptomycin’s asparagine residue was the D-isomer instead. The USPTO granted a Certificate of Correction from L-isomer to D-isomer on January 29, 2008 and the FDA relisted the patent in the Orange Book.

Cubist Defeats Hospira’s Challenge and Appeal

Written Description

  • Hospira challenged the patent, arguing unsuccessfully that the patent lacked written description. The Court of Appeals for the Federal Circuit (CAFC) sided with Cubist because the patent’s specification did not rely exclusively on the erroneous structural diagram to describe daptomycin.
    • Cubist described daptomycin in two additional ways. Firstly, Cubist described daptomycin using a consistent internal codename. Secondly, the patent specification described a process of making daptomycin, which Cubist successfully established that necessarily resulted in the correct D-isomer.
    • CAFC concluded that the specification “as a whole” showed that Cubist’s inventors had “possession of” daptomycin, even though they may not have had an accurate picture of daptomycin’s entire compound chemical structure.

Recapture Rule

  • Hospira also challenged the patent and argued unsuccessfully that the Certificate of Correction improperly broadened the scope of the claims violating the “recapture rule.”
  • The CAFC stated that the recapture rule does not apply because (1) the corrected claims are not broader original claims and (2) the amendment was not used to overcome a prior art rejection.

Appeal to Supreme Court Denied

The Supreme Court of the United Stated denied Hospira’s Petition for writ of certiorari on May 31, 2016.

Generic’s FDA Label Key Factor Determining Induced Infringement

A generic pharmaceutical’s FDA-approved label is a key factor in determining if marketing the generic pharmaceutical induces infringement of a patented method-of-treatment claim.

The Court of Appeals for the Federal Circuit (CAFC) most recently addressed the issue in Eli Lilly & Co. v. Teva Parenteral Meds., Inc. (Fed. Cir. No.: 15-2067), a Precedential Opinion published January 12, 2017. In reviewing the case, the Federal Circuit panel, compared two earlier cases:  AstraZeneca LP v. Apotex, Inc., 633 F.3d 1042 (Fed. Cir. 2010) and Takeda Pharmaceuticals U.S.A., Inc. v. West-Ward Pharmaceutical Corp., 785 F.3d 625 (Fed. Cir. 2015).

Eli Lilly v. Teva — Pemetrexed Disodium (ALIMTA®)

Eli Lilly markets pemetrexed disodium, a chemotherapy drug, under the brand name ALIMTA®. Teva submitted an Abbreviated New Drug Application (ANDA) seeking approval by the Food and Drug Administration (FDA) to market generic versions of ALIMTA®. Teva submitted Paragraph IV certifications under 21 U.S.C. § 355(j)(2)(A)(vii)(IV), declaring that Eli Lilly’s US Patent No. 7,772,209, issued in 2010, was invalid, unenforceable, or would not be infringed.  Eli Lilly subsequently brought a consolidated action against Teva for infringement under 35 U.S.C. § 271(e)(2).  The United States District Court for the Southern District of Indiana found direct infringement attributable to physicians and held Teva liable for inducing the physicians’ infringement because Teva’s product labeling would inevitably lead some physicians to infringe Eli Lilly’s patent.  The CAFC affirmed the District Court’s decision.

Eli Lilly’s patent claims methods of administering the chemotherapy drug pemetrexed disodium pemetrexed after pretreatment with common vitamins—folic acid and vitamin B12. Pemetrexed is an antifolate that kills cancer cells by inhibiting the function of folates, a class of nutrients necessary for cell reproduction. Physicians therefore prescribe pemetrexed to treat certain types of lung cancer and mesothelioma. The vitamin pre-treatments reduce the toxicity of pemetrexed.

CAFC Analysis & Decision

Teva’s FDA label spelled out the method claimed in Eli Lilly’s patent.  Moreover, the parties agreed that Teva’s product labeling would be materially the same as Eli Lilly’s ALIMTA® product labeling.  Importantly, both FDA labels provided instructions regarding the administration of folic acid including repeated instructions and warnings regarding the importance of and reasons for folic acid pre-treatment.  The District Court therefore found that the label’s instructions and warnings would inevitably lead some physicians to infringe Eli Lilly’s patent.  The Federal Circuit decided that the District Court did not clearly err because Teva’s pursuit of the FDA label was enough evidence establishing Teva’s requisite intent for inducement.

Comparison to Takeda case:

Takeda Pharmaceuticals U.S.A., Inc. v. West-Ward Pharmaceutical Corp., 785 F.3d 625 (Fed. Cir. 2015).
  • Takeda’s sells Colcrys®, colchicine for treating acute gout flares.
  • Hikma/West Ward launched the generic Mitigare®, colchicine for prophylactically treating gout.
  • Hikma /West Ward did not infringe Takeda’s patent because Hikma’s FDA label for prophylactic treatment did not describe Takeda’s method claim for acute treatment.
  • Subsequent litigation: After losing its appeal, Takeda filed an amended claim in Delaware. Then on May 16, 2016 (No. Civ. No. 14‑1268‑SLR) the Delaware District Court granted grants Hikma’s [West Ward] motion to dismiss.

Comparison to AstraZeneca case:

  • In the AstraZeneca case, the CAFC held that a label that instructed users to follow the instructions in an infringing manner was sufficient, even though some users would not follow the instructions because the product in question had substantial non-infringing uses.
  • A defendant’s decision to continue seeking FDA approval of instructions that teach an infringing use is sufficient evidence of specific intent to induce infringement.

Quotes Regarding Induced Infringement:

  • “Mere knowledge of the facts alleged to constitute infringement is not sufficient” (DSU Med.  471 F.3d at 1305).
  • When the alleged inducement relies on a drug label’s instructions, “[t]he question is not just whether [those] instructions describ[e] the infringing mode, . . . but whether the instructions teach an infringing use such that we are willing to infer from those instructions an affirmative intent to infringe the patent.” Takeda, 785 F.3d at 631 (internal quotation marks omitted).
  • “The label must encourage, recommend, or promote infringement.” For purposes of inducement, “it is irrelevant that some users may ignore the warnings in the proposed label.”  AstraZeneca LP v. Apotex, Inc., 633 F.3d 1042, 1060 (Fed. Cir. 2010).
  • The accused indirect infringer must have “knowingly aided and abetted” direct infringement. Warner‑Lambert v. Apotex, 316 F.3d 1348 (Fed. Cir. 2003)
  • The CAFC stated in Warner‑Lambert in the ANDA context, it is well-established that “mere knowledge of possible infringement by others does not amount to inducement; specific intent and action to induce infringement must be proven.” Warner-Lambert v. Apotex, 316 F.3d 1348 at 1364  (Fed. Cir. 2003) (citation omitted).
  • “The Hatch-Waxman Act was designed to enable the sale of drugs for non‑patented uses even though this would result in some off-label infringing uses.” See Caraco, 132 S.Ct. at 1681-82 (“Congress understood [that] a single drug may have multiple methods of use, only one or some of which a patent covers” and that the statute “contemplates that one patented use will not foreclose marketing a generic drug for other unpatented ones.”);
  • The Hatch-Waxman Act was not intended “as a sword against any competitor’s ANDA seeking approval to market an off-patent drug for an approved use not covered by the patent.” (Warner-Lambert v. Apotex, 316 F.3d 1348 at 1359)

Teva Liable for Induced Infringement of Eli Lilly’s Methods of Administering Pemetrexed (ALIMTA®)

Eli Lilly & Co. v Teva Parenteral Meds., Inc. (Fed. Cir. No.: 15-2067); January 12, 2017
CAFC Opinion PDF

Alimta_Structure

  • The Federal Circuit affirmed the District Court’s finding that Teva is liable for induced infringement of Eli Lilly’s US Patent No. 7,772,209 claiming methods for administering Pemetrexed.
    • The Federal Circuit addressed the issue of induced infringement and direct infringement by physicians even though one of the method steps is performed by patients. The Federal Circuit also addressed  indefiniteness, obviousness, and obviousness-type double patenting.
  • Eli Lilly markets pemetrexed under the brand name ALTIMA®
    • Pemetrexed is an antifolate that kills cancer cells by inhibiting the function of folates, a class of nutrients necessary for cell reproduction. The vitamin pretreatments reduce the toxicity of pemetrexed.
    • ALIMTA® is used to treat certain types of lung cancer and mesothelioma.
  • US Pat. No. 7,772,209 Claim 1:  A method for administering pemetrexed disodium to a patient in need thereof comprising administering an effective amount of folic acid and an effective amount of a methylmalonic acid lowering agent followed by administering an effective amount of pemetrexed disodium, wherein the methylmalonic acid lowering agent is selected from the group consisting of vitamin B12, hydroxycobalamin, cyano-10-chlorocobalamin, aquocobalamin perchlorate, aquo-10-cobalamin perchlorate, azidocobalamin, cobalamin, cyanocobalamin, or chlorocobalamin.

Reuters Article: “Eli Lilly defeats Teva Appeal over Alimta Cancer Drug”

Petitioner Must Prove Injury to Have Standing to Appeal an IPR Decision

January 11, 2017

Phigenix v. ImmunoGen (Fed. Cir. 2017) (Wallach, J)

  • Even though § 141(c) allows a party to appeal a PTAB’s IPR decision, the statute does not necessarily establish Article III standing.
    • One of Article III’s requirements is proving Injury-in-Fact.
  • Even if a petitioner loses an IPR challenge (i.e., Patent is still valid), the Petitioner may still not have standing if the petitioner has not suffered any damages yet. (For Example, the patent owner hasn’t sued the petitioner yet for infringement.)
  • Here, Phigenix [petitioner] lost an IPR (i.e., Immunogen [patent owner] won with a ruling of non-obviousness). But Phigenix did not have standing to appeal the IPR loss to the Federal Circuit because Phigenix did not have standing in part because they have not suffered any injury/damages yet.
    • Phigenix did not argue that it risked infringing ImmunoGen’s patent.  Phigenix argued instead that it suffered “actual economic injury” because the mere existence of ImmunoGen’s patent increased competition between itself and ImmunoGen. The Federal Circuit did not find Phigenix’s argument persuasive.

Claims:

Claim 1:  An immunoconjugate comprising an anti-ErbB2 antibody conjugated to a maytansinoid, wherein the antibody is huMAb4D5-8.

Claim 2:  The immunoconjugate of claim 1, wherein the maytansinoid is DM1 having the structure:
US08337856-Image


Related Blog Posts:

Patently-O Blog Post on Phigenix v. ImmunoGen (Fed. Cir. 2017)

PatentDocs Blog Post on Phigenix v. ImmunoGen (Fed. Cir. 2017)

For Fellow Coffee Lovers: PTAB Denies Keurig’s IPR Petition Against Touch Coffee

January 5, 2017

KEURIG GREEN MOUNTAIN, INC., Petitioner, v.
TOUCH COFFEE & BEVERAGES, LLC, Patent Owner.

Case IPR2016-01390; Patent 9,144,343 B2

According to the PTAB, Keurig did not provide adequate “articulated reasoning,” for establishing a reasonable likelihood of prevailing. Expert witnesses cannot merely say something is obvious. They need to explain why it’s obvious.

https://ptabdata.uspto.gov/ptab-api/documents/600671/native

Bristol-Myers Squibb’s CTLA4Ig Formulation Patent Survives IPR Obviousness Challenge from Momenta Pharmaceuticals

Momenta v. BMS

January 3, 2016

MOMENTA PHARMACEUTICALS, INC. (Petitioner)
v.
BRISTOL-MYERS SQUIBB COMPANY (Patent Owner)

Case IPR2015-01537
Patent 8,476,239
FINAL WRITTEN DECISION
December 22, 2016

The PTAB concluded that the preponderance of the evidence did not support Momenta’s argument that the challenged claims would have been obvious.

The claims of Patent US 8,476,239 are directed to stable liquid formulations of the therapeutic molecule CTLA4Ig.  CTLA4Ig is a protein molecule that is used to treat immune system diseases and disorders such as rheumatoid arthritis and adverse transplant reactions.

Claim1:  A stable formulation suitable for subcutaneous administration comprising:
[1]  at least 100mg/ml CTLA4Ig molecule,
[2]  a sugar selected from the group consisting of sucrose, lactose, maltose, mannitol and trehalose and mixtures thereof and
[3]  a pharmaceutically acceptable aqueous carrier, wherein the formulation has a
[4]  pH range of from 6 to 8 and
[5]  a viscosity of from 9 to 20 cps, and
[6]  the weight ratio of sugar:protein is 1.1:1 or higher.
(Bracketed numbers added)

Momenta argued that the inventors did “nothing more than the efforts of a skilled formulator choosing from a limited set of known formulations to subcutaneous liquid formulations.” Momenta further argued that “the inventors went to the formulator’s toolbox and tried the first line of excipients and formulation parameters.  And they worked.” The PTAB agreed that the prior art references provided general guidance for formulating proteins as stable liquids and that BMS followed certain aspects of those general teachings when creating its stable liquid formulation comprising CLTA4Ig, a known protein.  Momenta’s cited evidence, however, did not persuade the PTAB that an ordinarily skilled artisan would have reasonably expected to be successful in achieving the claimed formulations. The evidence was not persuasive because, despite the prior art teaching of general guidance for formulating proteins as stable liquids, the prior art also taught that maintaining physical and chemical stabilities for most proteins in aqueous solution for an extended period is extremely difficult. Expert testimony about testimony about routine trial-and-error optimization did not overcome the statements of difficulty. Such statements of difficulty in the art indicated to the PTAB that there would not have been a reasonable expectation of success in achieving the claimed formulations.

The PTAB highlighted in the importance of anticipated success and predictable results in determining obviousness. Citing the U.S. Supreme Court:

When there is a design need or market pressure to solve a problem and there are a finite number of identified, predictable solutions, a person of ordinary skill has good reason to pursue the known options within his or her technical grasp.  If this leads to the anticipated success, it is likely the product not of innovation but of ordinary skill and common sense.  In that instance the fact that a combination was obvious to try might show that it was obvious under § 103. KSR Int’l Co. v. Teleflex Inc., 550 U.S. 398, 421 (2007) (emphasis added); compare Merck & Co. v. Biocraft Labs., Inc., 874 F.2d 804, 809 (Fed. Cir. 1989) (“Reached by means of routine procedures, and producing only predictable results, the recited dosages therefore do not distinguish the claims of the ’430 patent from the amiloride/hydrochlorothiazide combination that the district court properly found was disclosed in the ’813 patent.” (emphasis added)).

Links:

PDF of Final Decision (IPR2015-01537)

Update 1/9/2017 – Link to Jones Day Blog:
“Routine Trial-and-Error Approach to Protein Formulation Is Not Sufficient to Establish Obviousness Absent a Reasonable Expectation of Success in Achieving the Claimed Formulation”

USPTO’s Patents Ombudsman Program

Check out the USPTO’s Patents Ombudsman program:

https://www.uspto.gov/patent/ombudsman-program

“The Patents Ombudsman Program enhances the USPTO’s ability to assist applicants or their representatives with issues that arise during patent application prosecution. More specifically, when there is a breakdown in the normal application process, including before and after prosecution, the Patents Ombudsman Program can assist in getting the application back on track.”

Medgraph v. Medtronic

December 13, 2016

Precedential Opinion today from the U. S. Court of Appeals for the Federal Circuit:

MEDGRAPH, INC. v. MEDTRONIC, INC.; No. 15-2019 (Fed. Cir. Dec. 13, 2016)

The Federal Circuit panel affirmed the District Court’s dismissal of Medgraph’s claims of infringement. Earlier, the Federal Circuit en banc, in Akamai v. Limelight, broadened the law attributing third-party acts to an accused infringer to include occasions when an accused infringer “conditions participation in an activity or receipt of a benefit upon performance of a step or steps” of a claimed method. Rather than remand the case to the district court, the Federal Circuit panel said that Medgraph did not produce facts meeting even the new more broad standard.

Link to CAFC Opinion PDF:
http://www.cafc.uscourts.gov/sites/default/files/opinions-orders/15-2019.Opinion.12-9-2016.1.PDF
Link to Finnegan’s Federal Circuit IP blog post:
“Change in Law Does Not Always Compel Remand”
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