10380442 (B.P.A.I. Jun. 10, 2009)

Ex Parte Srivastava

Board of Patent Appeals and InterferencesJun 10, 2009

10380442 (B.P.A.I. Jun. 10, 2009)

UNITED STATES PATENT AND TRADEMARK OFFICE ____________ BEFORE THE BOARD OF PATENT APPEALS AND INTERFERENCES ____________ Ex parte PRAMOD K. SRIVASTAVA ____________ Appeal 2009-003454 Application 10/380,442 Technology Center 1600 ____________ Decided1: June 10, 2009 ____________ Before DONALD E. ADAMS, LORA M. GREEN, and JEFFREY N. FREDMAN, Administrative Patent Judges. ADAMS, Administrative Patent Judge. DECISION ON APPEAL This appeal under 35 U.S.C. § 134 involves claims 1-7, 9-13, 15-27, 66, 67, 70-78, 82-86, 101-107, and 110-126, the only claims pending in this application. We have jurisdiction under 35 U.S.C. § 6(b). 1 The two-month time period for filing an appeal or commencing a civil action, as recited in 37 C.F.R. § 1.304, begins to run from the decided date shown on this page of the decision. The time period does not run from the Mail Date (paper delivery) or Notification Date (electronic delivery). Appeal 2009-003454 Application 10/380,442 STATEMENT OF THE CASE The claims are directed to a method of inducing an immune response against a type of cancer (claims 1-3, 7, 9-13, 15-27, 70-78, 101-107, and 110-112 ); a method of treating cancer (claims 4-7, 9-13, 15-27, 66, 70-78, and 101-107, and 110-120); and a kit effective for the treatment of a type of cancer (claim 67, 82-86, and 121-126). Claim 1 is illustrative: 1. A method of inducing an immune response against a type of cancer in a human subject having cancer, comprising administering to said subject a composition comprising an amount of unfractionated cytosolic soluble proteins obtained from human cells of said type of cancer or metastasis thereof effective to induce said immune response, wherein the proteins are not subjected to any methods that selectively remove particular soluble proteins, and wherein the proteins substantially lack intact cells, cell debris, nuclei, organelles and membranes. The Examiner relies on the following evidence: Kwak et al. US 6,562,347 B1 May 13, 2003 Nair et al. WO 97/41210 Nov. 6, 1997 Srivastava et al. WO 98/34641 Aug. 13, 1998 The rejection presented by the Examiner is as follows: Claims 1-7, 9-13, 15-27, 66, 67, 70-78, 82-86, 101-107, and 110-126 stand rejected under 35 U.S.C § 103(a) as unpatentable over the combination of Srivastava, Kwak and Nair. We affirm-in-part. 2 Appeal 2009-003454 Application 10/380,442 ISSUE Did Appellant establish that the Examiner erred in concluding that the combination of references make obvious the administration of a composition comprising unfractionated cellular proteins, wherein the proteins substantially lack intact cells? FINDINGS OF FACT FF 1. Srivastava teaches a method that comprises administering (1) a heat shock protein noncovalently bound to a first antigenic molecule and (2) antigen presenting cells (APCs) sensitized in vitro with a second heat shock protein non covalently bound to a second antigenic molecule (Ans. 3; Srivastava 63: 3-9 and 72: 14-21; see also App. Br. 5). FF 2. Srivastava does “not teach the administration of unfractionated cellular proteins” (Ans. 4; see also App. Br. 6-8). FF 3. Kwak teaches “that Il-2, Il-4, INFg and TNF function as adjuvants” (Ans. 4; see also App. Br. 12). FF 4. Nair teaches APCs “sensitized with unfractionated RNA derived from a tumor cell for the induction of a therapeutic immune response against cancer” (Ans. 4; see also App. Br. 9). FF 5. Appellant’s Specification defines the term “unfractionated cytosolic soluble proteins” as a “collection of proteins contained within a clarified extract of lysed cells, wherein the clarified extract is not subjected to any methods that selectively remove particular soluble proteins, and substantially lacks not only intact cells, but also cell debris, nuclei, organelles and membranes” (Spec. 24: 24-30). 3 Appeal 2009-003454 Application 10/380,442 FF 6. “The term ‘unfractionated cellular proteins’ . . . encompasses ‘unfractionated cytosolic soluble proteins’” (Spec. 24: 31-33). PRINCIPLES OF LAW “In proceedings before the Patent and Trademark Office, the Examiner bears the burden of establishing a prima facie case of obviousness based upon the prior art.” In re Fritch, 972 F.2d 1260, 1265 (Fed. Cir. 1992). On appeal to this Board, Appellants must show that the Examiner has not sustained the required burden. See (1) Ex parte Yamaguchi, http://www.uspto.gov/web/offices/dcom/bpai/ prec/fd074412.pdf, slip op. at 5 and 23 (BPAI Aug. 29, 2008) (precedential); (2) Ex parte Fu, http://www.uspto.gov/web/offices/ dcom/bpai/prec/fd080601.pdf, slip op. at 5 and 20 (BPAI Mar. 31, 2008) (precedential); (3) Ex parte Catan, http://www.uspto.gov/web/ offices/dcom/bpai/prec/fd070820.pdf, slip op. at 3 and 21 (BPAI Jul. 3, 2007) (precedential), and (4) Ex parte Smith, http://www.uspto.gov/web/offices/dcom/bpai/prec/fd071925.pdf, slip op. at 4, 9 and 23 (BPAI Jun. 25, 2007). Obviousness requires a suggestion of all the elements in a claim (CFMT, Inc. v. Yieldup Int’l Corp., 349 F.3d 1333, 1342 (Fed. Cir. 2003)) and “a reason that would have prompted a person of ordinary skill in the relevant field to combine the elements in the way the claimed new invention does.” KSR Int’l Co. v. Teleflex Inc., 550 U.S. 398, 418 (2007). 4 Appeal 2009-003454 Application 10/380,442 ANALYSIS Notwithstanding the Examiner’s discussion of Srivastava (Ans. 3-4), we note that while every claim on appeal requires unfractionated cytosolic soluble proteins or “unfractionated cellular proteins” (see, e.g., Claims 1 and 66); the Examiner finds that Srivastava does not teach the administration of unfractionated cellular proteins to induce an immune response to a cancer cell (Ans. 4). To be complete, Srivastava also fails to teach unfractionated cytosolic soluble proteins. The Examiner’s reliance on Kwak to teach “that Il-2, Il-4, INFg and TNF function as adjuvants” (FF 3) fails to make up for the deficiency in Srivastava (see, e.g., App. Br. 12). The Examiner relies on Nair to teach priming APCs with unfractionated tumor cell RNA (Ans. 4). As Appellant explains “[a]ccording to Nair, the RNA is translated within the antigen presenting cells and the resulting protein is processed by the MHC class I or class II pathways for presentation to the immune system” (App. Br. 9). Thus, Nair teaches the administration of APCs expressing tumor cell protein in the context of MHC class I or class II. Nair does not, however, teach the administration of unfractionated protein the substantially lacks intact cells (see, e.g., Claim 1). Accordingly, we find that the Examiner has failed to establish a prima facie case of obviousness with regard to claims 1-7, 9-13, 15-27, 66, 67, 70- 78, 82-86, 101-107, 110-112, and 121-126. All of these claims require cytosolic soluble protein or unfractionated cellular protein, wherein the proteins substantially lack intact cells. 5 Appeal 2009-003454 Application 10/380,442 Claims 113-120 stand on a different footing. As Appellant recognizes [c]laim 113 is directed to a method of treating cancer in a human subject, comprising administering to said subject a composition comprising an amount of [(unfractionated cellular proteins)] UCPs obtained from human cells of said type of cancer or a metastasis thereof, wherein the UCPs are from 107 cell equivalents or less of said human cells, and wherein the UCPs comprise proteins associated with organelles and cellular membranes. (App. Br. 19.) Claims 114-120 depend directly from claim 113. As Appellant recognizes, Nair teaches unfractionated proteins (e.g., the proteins expressed by the unfractionated RNA introduced into the APCs) that are associated with cellular membranes (e.g., are processed by the MHC class I or class II pathways for presentation to the immune system) (App. Br. 9). As Appellant recognizes, according to the teachings of Nair, APCs express “unfractionated RNA as a means for directing antigens into an immune presentation pathway” (App. Br. 17). In contrast to Appellant’s argument, claims 113-120 do not require the administration of “UCPs directly to a patient” (id.). To the contrary, claims 113-118 are open to include the presentation of antigen (e.g., unfractionated protein) through the administration of APCs directly to a patient. As Appellant recognizes “Nair teaches the administration of recombinant antigen presenting cells” (App. Br. 20). Accordingly, we are not persuaded by Appellant’s contention that “Nair, alone or in combination with Srivastava, does not give reason to administer a composition comprising unfractionated proteins, much less the UCPs . . . for eliciting an immune response or treating cancer” (id.). 6 Appeal 2009-003454 Application 10/380,442 CONCLUSION OF LAW Appellant established error in the Examiner’s conclusion that the combination of references make obvious the administration of a composition comprising unfractionated cellular proteins, wherein the proteins substantially lack intact cells. Therefore, the rejection of claims 1-7, 9-13, 15-27, 66, 67, 70-78, 82-86, 101-107, 110-112, and 121-126 under 35 U.S.C § 103(a) as unpatentable over the combination of Srivastava, Kwak and Nair is affirmed. Claims 113-120 do not require the proteins substantially lack intact cells. Therefore, the rejection of claims 113-120 under 35 U.S.C § 103(a) as unpatentable over the combination of Srivastava, Kwak and Nair is reversed. 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-IN-PART Ssc: JONES DAY 222 EAST 41ST STREET NEW YORK, NY 10017 7