Ex Parte Matsuyama

Patent Trial and Appeal BoardMar 14, 2017

13679439 (P.T.A.B. Mar. 14, 2017)

United States Patent and Trademark Office UNITED STATES DEPARTMENT OF COMMERCE United States Patent and Trademark Office Address: COMMISSIONER FOR PATENTS P.O.Box 1450 Alexandria, Virginia 22313-1450 www.uspto.gov APPLICATION NO. FILING DATE FIRST NAMED INVENTOR ATTORNEY DOCKET NO. CONFIRMATION NO. 13/679,439 11/16/2012 Shigemi Matsuyama CWR-019245US CON-1 9748 68705 7590 03/16/2017 TAROLLI, SUNDHEIM, COVELL & TUMMINO, LLP 1300 EAST NINTH STREET SUITE 1700 CLEVELAND, OH 44114 EXAMINER KAUFMAN, CLAIRE M ART UNIT PAPER NUMBER 1646 NOTIFICATION DATE DELIVERY MODE 03/16/2017 ELECTRONIC Please find below and/or attached an Office communication concerning this application or proceeding. The time period for reply, if any, is set in the attached communication. Notice of the Office communication was sent electronically on above-indicated "Notification Date" to the following e-mail address(es): rkline @ tarolli. com docketing@tarolli.com PTOL-90A (Rev. 04/07) UNITED STATES PATENT AND TRADEMARK OFFICE BEFORE THE PATENT TRIAL AND APPEAL BOARD Ex parte SHIGEMI MATSUYAMA1 Appeal 2016-003978 Application 13/679,439 Technology Center 1600 Before ERIC B. GRIMES, RYAN H. FLAX, and DEVON ZASTROW NEWMAN, Administrative Patent Judges. GRIMES, Administrative Patent Judge. DECISION ON APPEAL This is an appeal under 35U.S.C. § 134 involving claims to a pharmaceutical composition, which have been rejected as being directed to patent-ineligible subject matter. We have jurisdiction under 35 U.S.C. § 6(b). We affirm. 1 Appellant identifies the Real Party in Interest as Case Western Reserve University. (Appeal Br. 2.) Appeal 2016-003978 Application 13/679,439 STATEMENT OF THE CASE The Specification states that the “cellular attrition observed in most degenerative conditions is apoptotic in nature.” (Spec.213.) “Bax is . . . involved in regulating programmed cell death. Bax plays a key role in the intrinsic pathway of apoptosis.” {Id. 14.) The Specification discloses “a method of inhibiting apoptosis in a cell. The method includes administering to the cell a therapeutically effective amount of cell penetrating peptide (CPP). The CPP consists of about 5 to about 41 amino acids and is substantially homologous to a portion of the C- terminal region of interferon gamma receptor 2 (IFNyR2).’’ {Id. 1 5.) “An ‘effective amount’ or ‘therapeutically effective amount’ of CPP administered to a cell is the amount of the CPP effective to mitigate Bax mediated apoptosis in the cell.” {Id. 133.) Claims 36, 38-40, 42, and 43 are on appeal. Claim 36 is the only independent claim and reads as follows: Claim 36: A pharmaceutical composition comprising: a synthetic peptide for inhibiting apoptosis in a cell consisting of about 5 to about 41 amino acids of SEQ ID NO: 1; and a pharmaceutically acceptable carrier. DISCUSSION The Examiner has rejected all of the claims on appeal under 35 U.S.C. § 101 on the basis that they are directed to patent-ineligible subject matter; specifically, “a law of nature/natural principle.” (Ans. 2.) The Examiner 2 Our citations are to the “Clean Specification” filed Feb. 12, 2013. 2 Appeal 2016-003978 Application 13/679,439 finds that natural products are not patent-eligible, and a “fragment of a natural product which does not possess[] properties different than those it possesses when part of the full-length protein (aside from size) may also be considered a natural product.” (Id.) The Examiner finds that “the claimed peptide is part of the Bax-inhibiting domain of IFNyR2 and naturally has the property of inhibiting Bax-mediated apoptosis both as a fragment and as part of IFNyR2,” and therefore is not patentable subject matter. (Id.) We agree with the Examiner that claim 36 is not patent-eligible subject matter. Claim 36 is directed to composition comprising a carrier and a peptide that is a fragment of the naturally occurring IFNyR2 protein. Thus, Association for Molecular Pathology v. Myriad Genetics, Inc., 133 S.Ct. 2107 (2013), is controlling. In Myriad, the Court considered claims directed to isolated DNA encoding the BRCA1 polypeptide and fragments of at least 15 nucleotides of that DNA. Id. at 2113. The Court held that “Myriad did not create anything. To be sure, it found an important and useful gene, but separating that gene from its surrounding genetic material is not an act of invention.” Id. at 2117. “Myriad found the location of the BRCA1 and BRCA2 genes, but that discovery, by itself, does not render the BRCA genes ‘new . . . composition^] of matter,’ § 101, that are patent eligible.” Id. “Nor are Myriad’s claims saved by the fact that isolating DNA from the human genome severs chemical bonds and thereby creates a nonnaturally occurring molecule.” Id. at 2118. The same analysis applies here. Claim 36 is directed to fragments of a naturally occurring protein, separated from the rest of the protein. Appellant has identified certain peptides, with naturally occurring amino acid 3 Appeal 2016-003978 Application 13/679,439 sequences, that have the property of inhibiting Bax-mediated apoptosis, but this property does not render the peptides new compositions of matter that are patent-eligible. Rather, claim 36 is directed to products of nature.3 Appellant argues that the claimed composition modifies the structure of the naturally occurring IFNyR2 peptide by only using a fragment, the IFNyR2296-337 domain (SEQ ID NO: 1), of the full-length peptide. The synthetic peptide has a markedly different structure than IFNyR2 in that it only has about 5 to about 41 amino acids of SEQ ID NO: 1, whereas IFNyR2 has 337 amino acids. (Br. 6—7.) Appellant argues that “[t]he synthetic peptides involve the creation of a new compound, unlike the isolated DNA that coded for a BRCA1 polypeptide in [Myriad].” (Id. at 10.) This argument is not persuasive because the Myriad Court expressly held that the isolated BRCA genes were not patent-eligible even though isolating the DNA required severing chemical bonds. Myriad, 133 S.Ct. at 2118. The same conclusion would follow even if the peptide were manufactured rather than isolated from the whole protein. See also In re BRCA1- and BRCA2-based Hereditary Cancer Test Patent Litigation, 11A F.3d 755, 760 (Fed. Cir. 2014) (“The Supreme Court held ineligible claims directed to segments as short as 15 nucleotides, the same length as the primer claims at issue here, suggesting that even short strands identical to 3 Claim 36 recites a “synthetic” peptide but “[a]s the Supreme Court made clear, neither naturally occurring compositions of matter, nor synthetically created compositions that are structurally identical to the naturally occurring compositions, are patent eligible.” In re BRCA1- and BRCA2-based Hereditary Cancer Test Patent Litigation, 11A F.3d 755, 760 (Fed. Cir. 2014). 4 Appeal 2016-003978 Application 13/679,439 those found in nature are not patent eligible.”). The logic of the Myriad Court also applies when the naturally occurring product is a fragment of a protein rather than a gene. Appellant also argues that the claimed composition comprises a carrier in addition to the peptide, and that “pharmaceutically acceptable carriers comprise excipient[s] and auxiliaries that facilitate processing of the active agents into preparations that can be used pharmaceutically. The carrier modifies the properties of the peptide so that it is easier for processing and administration to a subject.” (Br. 8, citing Spec. 151.) Appellant argues that “since the carrier modifies the properties of the synthetic peptide so that it is easier for processing and administration to a subject, the claimed composition has markedly different characteristics than the naturally occurring IFNyR2 peptide and is not a ‘product of nature.’” (Id. at 10.) This argument is also unpersuasive. The Specification states that “[t]he pharmaceutical compositions of the present invention can include pharmaceutically acceptable carriers comprising excipients and auxiliaries that facilitate processing of the active agents into preparations that can be used pharmaceutically.” (Spec. 1 51, emphasis added.) Thus, the Specification does not define “pharmaceutically acceptable carriers” to require excipients and auxiliaries, but only states that they are possible components of a carrier. The Specification also states that “[fjormulations for parenteral administration include aqueous solutions of the active compounds in water- soluble form, for example, water-soluble salts and alkaline solutions.” (Id. 5 Appeal 2016-003978 Application 13/679,439 at | 52, emphasis added.) Thus, the broadest reasonable interpretation of a “pharmaceutically acceptable carrier,” read in light of the Specification, includes water—the carrier in the case of an aqueous solution. We agree with the Examiner (Ans. 4) that combining the naturally occurring peptide recited in claim 36 with water would not result in a composition with markedly different properties from those of the peptide itself, and does not render the composition of claim 36 patent-eligible. Finally, Appellant argues that the peptide recited in claim 36 “has different properties than those of the naturally occurring IFNyR2 that can be attributed to the structural changes.” (Br. 11.) Appellant argues that “[t]he naturally occurring IFNyR2 peptide can participate in JAK/STAT signaling while the synthetic peptide cannot.” (Id.) These arguments are not persuasive, because they are not supported by the evidence provided by Appellant’s Specification. With regard to JAK/STAT signaling, the Specification states that [t]o confirm that IFNyR2 does not require Jak2-mediated signaling for Bax inhibition, human cell lines lacking IFNyR2 and Jak2[ ]were examined. . . . IFNyR2296-337 and IFNyR2wild type were both able to inhibit etoposide-induced [i.e., Bax- mediated] apoptosis in these cells, but IFNyR21.295 could not (Fig. 2B-E). These results support the hypothesis that IFNyR2 can rescue cells from apoptosis independent of Jak2-mediated signal transduction. (Spec. 1 87.) “IFNyR2296-337” is the peptide of SEQ ID NO: 1. (Id. 130.) Thus, the Specification states that both the full-length (wild-type) IFNyR2 and the peptide corresponding to SEQ ID NO: 1 both inhibit Bax-mediated apoptosis in cells lacking Jak2; i.e., independent of JAK/STAT signaling. 6 Appeal 2016-003978 Application 13/679,439 Appellant also argues that “the new peptide demonstrates increased inhibition of Bax-mediated apoptosis compared to the natural product.” (Br. 11.) Appellant points specifically to the results shown in Figures 2B—E, 4A, and 7C—E. (Id.) Again, the evidence provided in the Specification does not support Appellant’s argument. Figures 2B—2E relate to the experiments done in cells lacking Jak2, and are discussed above. Regarding Figure 4A, the Specification states that “IFNyR2wild type as well as IFNyR2296-337 were able to inhibit apoptosis induced by Bim overexpression.” (Spec. 1 89.) Regarding Figures 7C—E, the Specification states that “IFNyR2296-337-GFP as well as IFNyR2wild type-GFP (Fig. 7C and D) inhibited STS-induced Bax activation. . . . The inhibition of Bax activation by IFNyR2296-337-GFP as well as IFNyR2 wild type-GFP was statistically significant (Fig. 7E).” (Spec. 195.) Thus, the Specification states that the results for the full-length IFNyR2 and those for the peptide of SEQ ID NO: 1 were comparable, not that those for the peptide were significantly different from those for the full- length protein. In summary, we agree with the Examiner that the claimed composition is not markedly different from a naturally occurring product. We therefore affirm the rejection of claim 36 under 35 U.S.C. § 101. Claims 38-40, 42, and 43 have not been argued separately and therefore fall with claim 36. 37 C.F.R. § 41.37(c)(l)(iv). 7 Appeal 2016-003978 Application 13/679,439 TIME PERIOD FOR RESPONSE No time period for taking any subsequent action in connection with this appeal may be extended under 37 C.F.R. § 1.136(a). AFFIRMED 8