14613657 (P.T.A.B. Feb. 4, 2019)

Ex Parte CHARNEAU et al

Patent Trial and Appeal BoardFeb 4, 2019

14613657 (P.T.A.B. Feb. 4, 2019)

UNITED STA TES p A TENT AND TRADEMARK OFFICE APPLICATION NO. FILING DATE FIRST NAMED INVENTOR 14/613,657 02/04/2015 Pierre CHARNEAU 76392 7590 02/06/2019 ARRIGO, LEE, GUTTMAN & MOUTA-BELLUM LLP 2200 Pennsylvania Ave NW Suite 400E WASHINGTON, DC 20037 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 ATTORNEY DOCKET NO. CONFIRMATION NO. DI99-79-F 4455 EXAMINER ANGELL, JONE ART UNIT PAPER NUMBER 1635 NOTIFICATION DATE DELIVERY MODE 02/06/2019 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): SALÂ© ARRIGO. US scott@arrigo.us carla@arrigo.us PTOL-90A (Rev. 04/07) UNITED STATES PATENT AND TRADEMARK OFFICE BEFORE THE PATENT TRIAL AND APPEAL BOARD Ex parte PIERRE CHARNEAU, VERONIQUE ZENNOU, FRANCOISE PFLUMIO, AUDE SIRVEN, and ANNE DUBART KUPPERSCHMITT (APPLICANT: Institut Pasteur, Centre National De La Recherche Scientifique, and Institut National De La Sante et De La Recherche Medicale Appeal2017-007404 Application 14/613,657 1 Technology Center 1600 Before FRANCISCO C. PRATS, RACHEL H. TOWNSEND, and DAVID COTTA, Administrative Patent Judges. TOWNSEND, Administrative Patent Judge. DECISION ON APPEAL This is an appeal under 35 U.S.C. Â§ 134 involving claims to a method of expressing a protein of interest in vivo, which have been rejected as being unpatentable on the ground of nonstatutory double patenting. Oral argument 1 Appellants identify the real party in interest as Institut Pasteur, Centre National De La Recherche Scientifique and Institut National De La Sante et De La Recherche Medicale. (Appeal Br. 3.) Appeal2017-007404 Application 14/613,657 was heard on January 17, 2019. 2 We have jurisdiction under 35 U.S.C. Â§ 6(b ). We reverse. STATEMENT OF THE CASE "[L ]entiviruses have been shown to infect both dividing and non- dividing cells." (Spec. 2.) They "have evolved a nuclear import strategy which allows their DNA genome to cross the nuclear membrane of a host cell." (Id.) In addition, "at the origin of their in vivo replication strategy and hence of their pathogenicity" replication of lentiviruses is mitosis- independent (Id.) "The invention provides a nucleic acid comprising a triple-stranded (triplex) structure, such as one from a lentivirus[, which] ... stimulates entry of nucleic acids into the nucleus of cells." (Id. at 4.) Claims 44--53 are on appeal. Claim 44 is representative and reads as follows: 44. A method of expressing a protein of interest in vivo compnsmg: b) administering a lentiviral particle encoding the protein of interest to an individual; c) transducing a cell of the individual with the lentiviral particle; and d) expressing the protein of interest encoded by the lentiviral particle in the cell of the individual, wherein the lentiviral particle comprises: at least one copy of lentiviral cPPT and CTS reg10ns; a heterologous nucleic acid sequence encoding the protein of interest under the control of an internal 2 Administrative Patent Judge Katz, who heard oral argument, but otherwise did not participate in this decision, was replaced by Administrative Patent Judge Prats. See Panel Change Order entered, January 25, 2019. 2 Appeal2017-007404 Application 14/613,657 promoter not naturally associated with the heterologous nucleic acid sequence; a lentiviral L TR that is deleted for the promoter and the enhancer of U3; (Appeal Br. 17 .) a lentiviral integrase protein; a lentiviral reverse transcriptase protein; a lentiviral Gag protein; and an envelope protein. The following ground of rejection by the Examiner is before us on review: Claims 44--53 on the ground of non-statutory obviousness-type double patenting as being unpatentable over claims 1-20 of U.S. Patent No. 8,512,993. DISCUSSION The Examiner finds that the method of claim 1 of the issued patent [US Patent No. 8,512,993] is drawn to a method comprising transducing a cell with a lentiviral vector particle comprising a cPPT and CTS sequence of a retrovirus which induces a three-stranded DNA structure, a heterologous sequence, and a HIV- I L TR that is deleted for the promoter and enhancer of U3. (Final Action 5.) The Examiner notes that the claims on appeal are drawn to a method of expressing a protein of interest by administering a lentiviral particle encoding the protein of interest such that is transduces a cell and expressed the protein of interest wherein the lentiviral particle comprises a number of specific limitations including a lentiviral L TR deleted for the promoter and enhancer of U3. (Id. at 4.) According to the Examiner the broader claims on appeal "are anticipated by the narrower embodiments of the issued claims." (Id. at 5.) 3 Appeal2017-007404 Application 14/613,657 In particular, the Examiner contends that the issued claims are a species embraced within the broader genus claims on appeal. (Id. at 6.) According to the Examiner, "using the disclosure of the ... '993 patent[] to define the specific embodiments encompassed by the patented claims, it is clear that the instant claims and the patented claims are not patentably distinct." (Id. at 10.) In that regard, the Examiner finds that "although the [patented] claims do not explicitly indicate that the cell is in vivo, the specification [ of the '993 patent] clearly indicates that the cell may be in vivo" and that "the specification [ of the '993 patent] also discloses that the method also encompasses expressing the protein of interest." (Id. at 9.) The Examiner finds that the "specification of the '993 patent also indicates that the heterologous nucleic acid of interest can be under the control of a promoter not naturally associated with the heterologous nucleic acid sequence." (Id.) Finally, the Examiner finds that while the patented claims do not explicitly recite all of the protein components of the lentiviral particle recited in the claims on appeal, the specification indicates that the production of the particle "is the exact same way the instant application describes production of lentiviral vector particles." (Id.) Consequently, the Examiner concludes that "producing the lentiviral vectors as disclosed in the [ '993] specification ( as evidenced by Yee et al., 1994 and N aldini et al. 1996) would necessarily result in a lentiviral vector particle comprising the four indicated proteins (lentiviral integrase, reverse transcriptase, Gag, and envelope proteins)." (Id.) We conclude that the Examiner has erroneously used Appellants' specification as prior art against them in coming to the conclusion that the claims on appeal are obvious variants of the '993 patent claims. While it is 4 Appeal2017-007404 Application 14/613,657 permissible to look to a reference patents' disclosures of utility in determining whether the claims of the reference patent directed to a compound are patentably distinct from the claims in a later expiring patent directed to a method of using that compound, see, e.g., Abbvie Inc. v. Mathilda & Terence Kennedy Institute of Rheumatology Trust, 764 F.3d 1366, 1380 (Fed. Cir. 2014) (citing In re Vogel, 422 F.2d 438, 441--42 (CCPA 1970)), see also Sun Pharm. Indus., Ltd. v. Eli Lilly & Co., 611 F.3d 1381, 1387-88 (Fed. Cir. 2010), that is not the case here. The two sets of claims are not compound claims and methods of their use. Moreover, the Examiner did not simply look to the reference patent for purposes of assessing the utility of compound claims, but rather for how one might extend the method invention recited in the claims of the '993 patent. As Appellants explain, the '993 patent claims are directed to a method of introducing a heterologous nucleic acid sequence into the nucleus of a cell, which cell may be "in vivo." The claimed invention on appeal is directed to a method of expressing a protein of interest in vivo. Introducing a nucleic acid sequence does not require protein expression. The fact that there is overlap between the two sets of claims, in that the cell has to be transduced with the nucleic acid of interest, is not dispositive of whether the additional requirements of the claims on appeal that enable protein expression result in an obvious variation of the reference patent claims. The Examiner has failed to identify the missing elements from the reference patent as being in the prior art. Instead, the Examiner simply notes that the Appellants' Specification teaches these missing elements in a method of expressing proteins. One would of course expect such a disclosure in the reference patent, since the specification of the reference patent is the same as 5 Appeal2017-007404 Application 14/613,657 the one supporting the claimed invention. That however, does not establish that these elements were in the prior art, nor does the Examiner make such an assertion. Moreover, the Examiner has failed on this record to establish some reason that would have led one of ordinary skill in the art to modify the invention of the reference patent to make the invention on appeal with a reasonable expectation of success. Thus, we do not sustain the Examiner's obviousness-double patenting rejection. SUMMARY We reverse the rejection of claims 44--53 on the ground of non- statutory obviousness-type double patenting as being unpatentable over claims 1-20 of U.S. Patent No. 8,512,993. REVERSED 6