13077686 (P.T.A.B. Feb. 27, 2017)

Ex Parte Marletta et al

Patent Trial and Appeal BoardFeb 27, 2017

13077686 (P.T.A.B. Feb. 27, 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. 13/077,686 03/31/2011 Michael A. Marietta BERK-135 6006 84220 7590 03/01/2017 UC Berkeley - OTL Bozicevic, Field & Francis LLP 201 REDWOOD SHORES PARKWAY SUITE 200 REDWOOD CITY, CA 94065 EXAMINER GAR YU, LIANKO G ART UNIT PAPER NUMBER 1676 NOTIFICATION DATE DELIVERY MODE 03/01/2017 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): docket@bozpat.com PTOL-90A (Rev. 04/07) UNITED STATES PATENT AND TRADEMARK OFFICE BEFORE THE PATENT TRIAL AND APPEAL BOARD Ex parte MICHAEL A. MARLETTA, MICHAEL B. WINTER, EMILY J. MCLAURIN, STEVEN Y. REECE, CHARLES OLEA JR., and DANIEL G. NOCERA1 Appeal 2015-004849 Application 13/077,686 Technology Center 1600 Before JOHN G. NEW, RICHARD J. SMITH, and TAWEN CHANG, Administrative Patent Judges. SMITH, Administrative Patent Judge. DECISION ON APPEAL This is an appeal under 35U.S.C. § 134 involving claims to a non- naturally occurring photoactive polypeptide. We have jurisdiction under 35 U.S.C. § 6(b). We affirm. 1 According to Appellants, the real parties in interest are: a) The Massachusetts Institute of Technology; and b) The Regents of the University of California. (Br. 3.) Appeal 2015-004849 Application 13/077,686 STATEMENT OF THE CASE Claims on Appeal Claims 1—5, 7, 11—14, 35, and 36 are on appeal.2 (Claims Appendix, Br. i—ii.) Claim 1 is illustrative and reads as follows: 1. A non-naturally occurring photoactive polypeptide comprising: a) an H-NOX3 domain-containing heme binding polypeptide comprising a heme-binding fragment of the Tar4H protein from Thermoanaerobacter tengcongensis; and b) a prosthetic group other than heme, wherein the prosthetic group is bound to the heme-binding polypeptide, wherein the photoactivity of the photoactive polypeptide is altered upon exposure to oxygen. Examiner’s Rejection Claims 1—5, 7, 11—14, 35, and 36 stand rejected under pre-AIA 35 U.S.C. § 103(a) as unpatentable over Cary4 and Paulson.5 (Final Act. 8— 12.) FINDINGS OF FACT We adopt as our own the Examiner’s findings regarding the scope and content of the prior art, and reasons to combine the cited references. The following findings are included for emphasis and reference convenience. 2 Claims 6, 10, and 15—34 are withdrawn from consideration. (Final Act. dated October 25, 2013, at 2.) 3 The Specification states that H-NOX stands for “(Heme Nitric oxide/OXygen binding).” (Spec. 137.) 4 Cary et al., WO 2007/139767 A2, published Dec. 6, 2007 (“Cary”). 5 Paulson et al., Preparation of Ruthenium(II) and Ruthenium(III) Myoglobin and the Reaction of Dioxygen, and Carbon Monoxide, with Ruthenium(II) Myoglobin, 254 The Journal of Biological Chemistry 15, 7002-06 (1979) (“Paulson”). 2 Appeal 2015-004849 Application 13/077,686 FF 1. The Examiner finds that Cary teaches H-NOX proteins derived from bacterial protein such as [T. Tengcongenisis] (the heme-binding polypeptide is an H-NOX domain containing polypeptide (elected species) other than soluble guanylate cyclase) bound to heme (prosthetic group). (Final Act. 9, citing Cary H 17, 36, 54, 59, and Figure IB.) FF 2. Cary states that “[h]eme may or may not be bound to the H- NOX protein. In some embodiments of the isolated H-NOX proteins, NO is bound to the H-NOX protein.” (Cary 117.) FF 3. Cary states that The H-NOX proteins and compositions described herein can also be used for a number of in vitro or industrial applications .... Particular H-NOX proteins can be selected for such applications based on the desired NO dissociation constant.... Moreover, the H-NOX proteins can be used to remove NO from solutions requiring the removal of NO. For example, the H-NOX proteins may be used to absorb or remove NO in bioreactors where NO is an inhibitor of cellular proliferation and/or mitochondrial function. (Cary 11 137-138.) FF 4. The Examiner finds that “Paulson [] teach[es] reconstituting myoglobin (heme-binding polypeptide) with ruthenium porphyrins to form ruthenium(II) (prosthetic group other than heme) substituted Myoglobin (heme-binding polypeptide), RuMb, and ruthenium(Ill) mesoporphyrin (prosthetic group other than heme) substituted Myoglobin (heme-binding polypeptide), RuMb+.” (Final Act. 9, citing Paulson Abstract; 7003 rt. col, par. 2; 7004 rt. col., par. 1—3; Figures 3—6.) FF 5. The Examiner finds that one of ordinary skill in the art would have been motivated to substitute the heme of Cary with ruthenium (II) mesoporphyrin, or ruthenium (III) mesoporphyrin, of Paulson, with a 3 Appeal 2015-004849 Application 13/077,686 reasonable expectation of success, “because Paulson [] states that ruthenium, the second row transition metal analogue of iron, is an obvious choice for further studies on metal ion substitution in heme proteins.” (Final Act. 10, citing Paulson 7002, left col., par. 2.) DISCUSSION We adopt, and agree with, the Examiner’s findings, analysis, and conclusions, as set forth in the Final Action (Final Act. 8—12), Advisory Action dated Feb. 10, 2014 (Adv. Act. 2—4), and Answer (Ans. 2—4). We discern no error in the Examiner’s rejection of claims 1—5, 7, 11— 14, 35, and 36 as obvious. (FF 1—5.) The claims are not separately argued, and we therefore limit our discussion to claim 1. Issue Whether a preponderance of evidence of record supports the Examiner’s rejection for obviousness under 35 U.S.C. § 103(a). Analysis Appellants contest the motivation to combine the teachings of Cary and Paulson by arguing that substitution of heme from the H-NOX protein (from Cary) with a ruthenium (II) mesoporphyrin or ruthenium (III) mesoporphyrin from Paulson, would render the H-NOX protein of Cary unsatisfactory for its intended purpose. The intended purpose of the Cary is to use an H-NOX protein as a physiologically compatible mammalian blood nitric oxide (NO) gas carrier that can deliver NO to tissues of the body (i.e., “for blood gas NO delivery”) (see e.g., the abstract of Cary). In order achieve this goal, Cary describes the generation of mutations of the polypeptide that alter the binding affinity (and/or binding kinetics) of the protein complex (polypeptide plus heme) so that NO can be released to tissues. (Br. 5.) 4 Appeal 2015-004849 Application 13/077,686 In support of that argument, Appellants refer to several articles for the proposition that “it was known in the art at the time of filing that ruthenium could be used as an NO scavenger in biological systems (precisely because Ruthenium binds NO with high affinity).” (Id. at 5—6.) Thus, according to Appellants, “one of ordinary skill in the art would readily recognize that an H-NOX protein of Cary with an incorporated [ruthenium mesoporphyrin] from Paulson (instead of heme) would bind to NO with much too high an affinity to be used to deliver NO to tissues.” (Id. at 5.) Appellants thus argue that the substitution of heme from the H-NOX protein of Cary with a ruthenium (II/III) mesoporphyrin of Paulson would render Cary unsatisfactory for its intended purpose or change its mode of operation. (Br. 4—6.) As so argued, the question to address is: What is the intended purpose or overall principle of operation of Cary? See In re Mouttet, 686 F.3d 1322, 1331-33 (Fed. Cir. 2012). As an initial matter, a reference (e.g., Cary) “may be read for all that it teaches, including uses beyond its primary purpose.” See Mouttet, 686 F.3d at 1331. While Cary may well teach the use of its H-NOX proteins for delivery of NO to body tissues, even as a preferred or primary use, Cary also teaches other uses of its H-NOX proteins, including for absorption or removal of NO in bioreactors where a high binding affinity would be desirable. (Ans. 3^4; FF 3.) Accordingly, for purposes of this appeal, we find that the intended purpose, or overall principal of operation, of Cary is the in vivo or in vitro or industrial use of the disclosed H-NOX proteins for the delivery or absorption/removal of NO. (See, e.g., Cary Abstract and 10, 12, 17, 137, and 138; FF 3.) Based on the forgoing, we do not find that the substitution of 5 Appeal 2015-004849 Application 13/077,686 ruthenium (II/III) mesoporphyrin in place of the heme from the H-NOX protein of Cary would render Cary unsatisfactory for its intended purpose or change its overall principle of operation. Rather, it would be consistent with Cary’s intended purpose of using its H-NOX proteins for absorbing or removing NO. (Cary || 137, 138; Ans. 4.) Thus, unlike the facts in In re Gordon cited by Appellants, the prior art suggests the desirability of the modification. (FF 1—5.) See In re Gordon, 733 F.2d 900, 902 (Fed. Cir. 1984) (“The mere fact that the prior art could be so modified would not have made the modification obvious unless the prior art suggested the desirability of the modification.”) (citing cases); see also Allied Erecting v. Genesis, 825 F.3d 1373, 1380-81 (Fed. Cir. 2016); In reNuVasive, 841 F.3d 966, 973-74 (Fed. Cir. 2016). Accordingly, the rejection of claim 1 is affirmed. Conclusion of Law A preponderance of evidence of record supports the Examiner’s rejection of claim 1 under 35 U.S.C. § 103(a). Claims 2—5, 7, 11—14, 35, and 36 were not argued separately and fall with claim 1. SUMMARY We affirm the rejection of all claims on appeal. 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 6