11101287 (B.P.A.I. Sep. 28, 2010)

Ex Parte Martin

Board of Patent Appeals and InterferencesSep 28, 2010

11101287 (B.P.A.I. Sep. 28, 2010)

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. 11/101,287 04/07/2005 J. Tyler Martin 8325-0040 5737 20855 7590 09/28/2010 ROBINS & PASTERNAK 1731 EMBARCADERO ROAD SUITE 230 PALO ALTO, CA 94303 EXAMINER HAMA, JOANNE ART UNIT PAPER NUMBER 1632 MAIL DATE DELIVERY MODE 09/28/2010 PAPER 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. PTOL-90A (Rev. 04/07) UNITED STATES PATENT AND TRADEMARK OFFICE __________ BEFORE THE BOARD OF PATENT APPEALS AND INTERFERENCES __________ Ex parte J. TYLER MARTIN __________ Appeal 2010-004652 Application 11/101,287 Technology Center 1600 __________ Before DEMETRA J. MILLS, FRANCISCO C. PRATS, and JEFFREY N. FREDMAN, Administrative Patent Judges. PRATS, Administrative Patent Judge. DECISION ON APPEAL1 This appeal under 35 U.S.C. § 134 involves claims to methods of treating diabetic neuropathy. The Examiner rejected the claims as obvious. We have jurisdiction under 35 U.S.C. § 6(b). We affirm. 1 The two-month time period for filing an appeal or commencing a civil action, as recited in 37 C.F.R. § 1.304, or for filing a request for rehearing, as recited in 37 C.F.R. § 41.52, begins to run from the “MAIL DATE” (paper delivery mode) or the “NOTIFICATION DATE” (electronic delivery mode) shown on the PTOL-90A cover letter attached to this decision. Appeal 2010-004652 Application 11/101,287 2 STATEMENT OF THE CASE Claims 1-3 are pending and on appeal (App. Br. 2). Because Appellant did not argue the patentability of the claims separately, they stand or fall together. See 37 C.F.R. § 41.37(c)(1)(vii). Claim 1 is representative of the rejected claims, and reads as follows: 1. A method for treating a diabetic neuropathy, a spinal cord injury or a crushed nerve in a subject, the method comprising: introducing a nucleic acid into a human subject, wherein the nucleic acid encodes a polypeptide, wherein the polypeptide comprises: (i) a zinc finger DNA-binding domain that is engineered to bind to a target site in the vascular endothelial growth factor-A (VEGF-A) gene; and (ii) a transcriptional activation domain; such that the nucleic acid is expressed in one or more cells of the subject, whereby the polypeptide binds to the target site and activates transcription of the VEGF-A gene. The sole rejection before us for review is the Examiner’s rejection of claims 1-3 under 35 U.S.C. § 103(a) as obvious over Isner,2 Rebar,3 Hirai,4 McLaren,5 Beerli,6 Rebar II,7 and Koike8 (Ans. 3-5).9 2 Jeffrey M. Isner et al., CLINICAL PROTOCOL: VEGF Gene Transfer for Diabetic Neuropathy, 12 HUMAN GENE THERAPY 1593-94 (2001). 3 U.S. Patent App. Publication, US 2003/0021776 A1 (published Jan. 30, 2003). 4 M. Hirai et al., Expression of Vascular Endothelial Growth Factors (VEGF-A/VEGF-1 and VEGF-C/VEGF-2) in Postmenopausal Uterine Endometrial Carcinoma, 80 GYNECOLOGIC ONCOLOGY 181-188 (2001). 5 J. McLaren, Vascular endothelial growth factor and endometriotic angiogenesis, 6 HUMAN REPRODUCTION UPDATE 45-55 (2000). 6 Roger R. Beerli et al., Positive and negative regulation of endogenous genes by designed transcription factors, 97 PNAS 1495-1500 (2000). Appeal 2010-004652 Application 11/101,287 3 OBVIOUSNESS ISSUE The Examiner cites Isner as disclosing a clinical trial proposal in which a plasmid encoding VEGF-A was to be injected into patients to treat diabetic neuropathy (Ans. 4). The Examiner concedes that, unlike claim 1, Isner did not teach using a nucleic acid construct encoding a VEGF-A- targeted zinc finger protein linked to a transcriptional activation domain as the therapeutic agent (id.). The Examiner cites Rebar as teaching the nucleic acid construct recited in claim 1, and further notes that the construct was used to induce angiogenesis (id.). Based on these teachings, the Examiner concludes that, “[b]ecause both Isner et al. and Rebar et al. teach methods of increasing VEGF-A expression and inducing angiogenesis, it would have been obvious 7 Edward J. Rebar et al., Induction of angiogenesis in a mouse model using engineered transcription factors, 8 NATURE MEDICINE 1427-1432 (2002). 8 Hiromi Koike et al., Enhanced angiogenesis and improvement of neuropathy by cotransfection of human hepatocyte growth factor and prostacyclin synthase gene, 17 THE FASEB JOURNAL 779-781 (2003). 9 The Examiner appears to rely only on Isner, Rebar, and McLaren to show prima facie obvious, and does not point to any disclosures in any of the other cited references to support the prima facie case (see Ans. 4-5). Koike, Beerli, and Rebar II are cited in the Examiner’s response to Appellant’s arguments, apparently as rebuttal evidence (id. at 7, 13). Hirai does not appear to be mentioned anywhere in the Examiner’s Answer other than on page 3 (in the “Evidence Relied Upon” section and the statement of rejection). According to Appellant, however, the Examiner relied on Hirai in an Advisory Action to show that VEGF-A is the same protein as VEGF-1 (App. Br. 3). Thus, the Examiner appears to have cited Hirai in the Answer solely because it was relied on during earlier prosecution. Appeal 2010-004652 Application 11/101,287 4 to one skilled in the art to substitute the VEGF-A overexpression construct taught by Isner et al. with that of the construct taught by Rebar” (id.). Appellant contends that the Examiner has not “shown that VEGF-A administration is a predictable, known element for treating diabetic neuropathy, let alone that a zinc finger protein (ZFP) that modulates VEGF- A expression treats this disease. Furthermore, the claimed invention solves a long-felt need for treatment of diabetic neuropathy” (App. Br. 5). Appellant also argues that the cited references do not teach or suggest all of the claimed elements (Reply Br. 3-6). In particular, Appellant urges that because Isner did not present any actual data on the efficacy of the proposed treatment, Isner’s clinical trial proposal would not have provided an ordinary artisan with a reasonable expectation that administering a nucleic acid encoding VEGF-A, much less a VEGF-A-stimulating zinc finger protein, would successfully treat diabetic neuropathy (App. Br. 5-6; see also Reply Br. 6-7). Appellant urges that none of the other cited references remedies Isner’s deficiency in this regard (App. Br. 6-7; see also Reply Br. 7-8). Moreover, Appellant argues, the apparent decision to conduct Isner’s proposed clinical trial using a plasmid encoding VEGF-2, a different protein than the originally proposed VEGF-A, and the failure of the VEGF-2 plasmid to successfully treat diabetic neuropathy, demonstrate that an ordinary artisan lacked a reasonable expectation in treating diabetic neuropathy with VEGF-A (App. Br. 8-9 (citing VEGF Gene Transfer Appeal 2010-004652 Application 11/101,287 5 clinical trial webpage (App. Br. Appendix A);10 Corautus Genetics Press Release of October 19, 2005 (Appendix B);11 Corautus Genetics Press Release of October 10, 2006 (Appendix C);12 Corautus Genetics Press Release of November 3, 2007 (Appendix D));13 see also Reply Br. 8-9). Appellant argues that Rebar and Beerli would also have failed to provide a reasonable expectation that VEGF-A-targeted zinc finger proteins would treat diabetic neuropathy (App. Br. 9). Further, Appellant argues, the evidence of record shows that the claimed methods meet a long-felt, but unsolved need (id. at 10-11 (citing Sangamo BioSciences Press Release of April 11, 2006 (App. Br. Appendix E));14 see also Reply Br. 9-11). In view of the positions advanced by Appellant and the Examiner, the issues with respect to this rejection are whether the evidence of record supports the Examiner’s position that an ordinary artisan would have considered it obvious that Rebar’s VEGF-A-stimulating nucleic acid 10 VEGF Gene Transfer for Diabetic Neuropathy, http://clinicaltrials.gov/ct2/show/NCT00056290 (February 9, 2009). 11 Corautus Genetics Inc, (VEGF) Announces Collaboration And Licensing Agreement For Treatment Of Diabetic Neuropathy With VEGF-2, http://www.biospace.com/news_print.aspx?NewsEntityId=20849420 (October 19, 2005). 12 Corautus Genetics Announces Final Efficacy Results of GENASIS Phase IIb Clinical Trial, http://www.prnewswire.com/cgi- bin/stories.pl?ACCT=104&STORY=/www/story/10-10-20... (October 10, 2006). 13 Corautus Genetics Announces Redirection of Focus and Transition Of Officers, http://www.prnewswire.com/cgi-bin/stories.pl?ACCT= 104&STORY=/www/story/11-03-20... (November 3, 2007). 14 Diabetic Neuropathy Treatment Has Passed The First Clinical Trial, http://www.medicalnewstoday.com/printerfriendlynews.php?newsid=41158 (April 11, 2006). Appeal 2010-004652 Application 11/101,287 6 construct would successfully treat diabetic neuropathy when administered to patients suffering from that disorder, and if so, whether the secondary indicia of obviousness, in particular long-felt but unsolved need, are sufficient to outweigh the evidence of prima facie obviousness. FINDINGS OF FACT (“FF”) Isner 1. Isner discloses: Among diabetics, peripheral neuropathy is common and ultimately accounts for significant morbidity. The ultimate consequence of such sensory defects involving the lower extremities may be foot ulceration initiated by trauma that is inapparent to the patient. Such ulcerations often lead to lower extremity amputation, a complication that is 15 times higher in diabetic versus non- diabetic patients. (Isner 1594.) 2. Isner discloses: Preliminary clinical studies have demonstrated improvement in signs and symptoms of sensory neuropathy in patients with lower extremity vascular occlusive disease following intramuscular injection of naked DNA encoding vascular endothelial growth factor (VEGF). To determine if such a strategy could be applied to diabetic patients, including those without evidence of large vessel occlusive disease, we investigated the hypothesis that experimental diabetic neuropathy results from destruction of the vasa nervorum and can be reversed by administration of an angiogenic growth factor. (Id.) 3. Isner discloses: In two different animal models of diabetics, nerve blood flow and the number of vasa nervorum were found to be markedly Appeal 2010-004652 Application 11/101,287 7 attenuated resulting in severe peripheral neuropathy. In contrast, following VEGF gene transfer, vascularity and blood flow in nerves of treated animals were similar to those of non- diabetic controls; constitutive overexpression of VEGF resulted in restoration of large and small fiber peripheral nerve function. These findings implicate microvascular disruption as the basis for diabetic neuropathy and suggest that angiogenic growth factors may constitute a novel treatment strategy for this pernicious disorder. (Id.) 4. Based on the preliminary results, Isner describes its proposed clinical trial: The protocol outlined in this Investigational New Drug Application has been designed as a Phase I/II, single-site, dose escalating, double-blind, placebo controlled study to evaluate the safety and impact of phVEGF165 gene transfer on sensory neuropathy in patients with diabetes with or without macrovascular disease involving the lower extremities. . . . A total of 192 patients will be recruited into two arms of the study . . . . (Id.) 5. It is undisputed that Isner’s phVEGF165 is a plasmid encoding the 165 amino acid isoform of VEGF-A which was to be injected into the foot, calf, or thigh muscle of the affected extremity (see id. at 1593). Rebar 6. Rebar discloses, as background to its invention, that “VEGF-A acts to regulate the generation of new blood vessels during embryonic vasculogenesis and then subsequently plays an important role in regulating angiogenesis later in life” (Rebar [0008]). Appeal 2010-004652 Application 11/101,287 8 7. Rebar discloses, in particular, that “the VEGF-A165 isoform is a 165 amino acid species and has a molecular weight of approximately 46 kD; this isoform is the predominant molecular form found in normal cells and tissues” (id. at [0009]). 8. Rebar further discloses that “VEGF-C is also referred to as VEGF- related protein (hence VRP) or VEGF-2. The protein is roughly 30% identical to the amino acid sequence of VEGF-A . . . . Although the protein induces vascular permeability and promotes endothelial growth, it is less potent than VEGF-A” (id. at [0012]). 9. Rebar describes its inventions as “methods and compositions for regulating angiogenesis” (abstract). Rebar’s methods use “various zinc finger proteins that bind to particular target sites in one or more VEGF genes. Nucleic acids encoding the zinc finger proteins are also disclosed. Methods for modulating the expression of one or more VEGF genes with the zinc finger proteins and nucleic acids are also disclosed” (id.). 10. Rebar discloses that its VEGF-targeted zinc finger proteins can act to increase or repress angiogenesis, in the appropriate situation: [W]ith angiogenesis, for example, by attaching an activation domain to a ZFP [zinc finger protein] that binds to a target sequence within a gene that affects angiogenesis, one can enhance certain beneficial aspects associated with angiogenesis (e.g., alleviation of ischemia). In contrast, if angiogenesis is associated with harmful processes (e.g., delivery of blood supply to tumors) one can reduce angiogenesis by using ZFPs that are fused to a repressor. Hence, binding of this type of ZFP to a gene involved in angiogenesis can significantly reduce angiogenesis. (Id. at [0021].) Appeal 2010-004652 Application 11/101,287 9 11. Accordingly, where undesired angiogenesis contributes to a disease, Rebar’s “ZFPs find use in preventing unwanted processes by repressing vessel formation. Thus, for example, ZFPs can be used in treating diabetic retinopathy, psoriasis, arthropathies and tumor growth” (id. at [0027]; see also [0160]). 12. In contrast, Rebar discloses that its zinc finger proteins can also be used to increase angiogenesis in conditions that warrant such treatment: [T]he ZFPs can be used to activate expression of VEGF genes to trigger beneficial angiogenesis in cell populations, both in vitro and in vivo. Such activation can be utilized for example to promote the formation of new blood vessels and capillaries in treatments for ischemic conditions. For instance, the ZFPs can be used to stimulate the development of collateral circulation in individuals having any of a variety of arterial or venous obstructions, such as individuals having arthrosclerosis. The ZFPs can also be used to promote lymphogenesis (the formation of lymphatic vessels) and myelopoiesis (the formation of the tissue elements of bone marrow and/or types of blood cells derived from bone marrow), and can be used to regenerate blood vessels and tissue in wounds. (Id. at [00159].) 13. Rebar discloses that its angiogenesis-modulating zinc finger proteins can be introduced into cells and tissues by way of nucleic acid constructs encoding the proteins: Conventional viral and non-viral based gene transfer methods can be used to introduce nucleic acids encoding the present ZFPs in mammalian cells or target tissues. Such methods can be used to administer nucleic acids encoding ZFPs to cells in vitro. In some instances, the nucleic acids encoding ZFPs are administered for in vivo or ex vivo gene therapy uses. (Id. at [0253].) Appeal 2010-004652 Application 11/101,287 10 14. Rebar thus discloses preparation of a nucleic acid construct encoding a VEGF-A-targeted zinc finger protein linked to a viral transcription activation domain (see id. at [0381]), and further discloses that injection of that nucleic acid into a mouse resulted in stimulation of angiogenesis: E. Induction of Angiogenesis Subcutaneous injection of recombinant adenovirus encoding VEGF regulating zinc finger proteins induces angiogenesis in the mouse ear. To assess the ability of VEGF- A regulating zinc finger proteins to induce angiogenesis in vivo we injected recombinant adenovirus encoding VEGF-A regulating ZFP's subcutaneously into the mouse ear. . . . Three days and six days later the animals were visualized and digital photographs of the ears were taken. As shown in FIGS. 18A-D, adenovirus-mediated delivery of genes encoding VEGF-A regulating ZFP's (VOP30A or VOP 32B) resulted in augmented ear vascularization. These results were correlated with data from formal vessel counts, as shown in FIG. 18E. (Id. at [0414]-[0415].) 15. Rebar describes the advantages of its compositions: [T]he designed ZFPs disclosed herein upregulate each major splice variant of VEGF-A, in proportions similar to those observed under physiological conditions (e.g., hypoxia). This is important because recent studies suggest that proper isoform balance is crucial for VEGF-A function. . . . . Currently, most VEGF-A gene therapy trials involve the application of just a single VEGF-A splice variant cDNA or protein isoform. Isner et al. (1996) Lancet 348: 370-374; Esakof et al. (1999) Hum. Gene Ther. 10: 2307-2314; Rosengart et al. (1999a) Ann. Surg. 230: 466-470, discussion 470-472; Rosengart et al. (1999b) Circulation 100: 468-474; Hendel et al. (2000) Circulation 101: 118-121. It has been suggested that an ideal gene therapy agent should be able to recapitulate natural ratios of various different VEGF-A isoforms. Activation of VEGF-A using the designed ZFPs disclosed herein therefore offers Appeal 2010-004652 Application 11/101,287 11 advantages in this regard, providing key components of pro- angiogenic gene therapy agents. (Id. at [0361].) VEGF Gene Transfer for Diabetic Neuropathy (App. Br. Appendix A) 16. This document, presented at the ClinicalTrials.gov website, describes the following clinical trial: This gene therapy study is being conducted to evaluate intramuscular gene transfer using VEGF (Vascular Endothelial Growth Factor) in patients with diabetic neuropathy in the legs. This condition causes a decrease in feeling and sensation due to diabetes. VEGF is DNA, or genetic material that is injected into the muscles of the leg. Once in the leg, it has been shown to cause new blood vessels to grow under a variety of conditions. (http://clinicaltrials.gov/ct2/show/NCT00056290 (February 9, 2009).) Corautus Genetics Inc, (VEGF) Announces Collaboration And Licensing Agreement For Treatment Of Diabetic Neuropathy With VEGF-2 (App. Br. Appendix B) 17. This document describes a clinical trial in which “Corautus will provide its proprietary vascular endothelial growth factor, VEGF-2 for evaluation in the 64-patient, Phase I trial for treating diabetic neuropathy now underway at CSEMC that is funded by a grant from the National Institutes of Health (‘NIH’)” (http://www.biospace.com/news _print.aspx?NewsEntityId=20849420 (October 19, 2005)). Corautus Genetics Announces Final Efficacy Results of GENASIS Phase IIb Clinical Trial (App. Br. Appendix C) Appeal 2010-004652 Application 11/101,287 12 18. This document describes an announcement from Corautus Genetics Inc. regarding termination of a clinical trial using the VEGF-2 gene as the therapeutic agent: Corautus Genetics Inc. (Nasdaq: VEGF), a clinical stage biopharmaceutical company, announced today that the final efficacy results from its GENASIS Phase IIb clinical trial did not achieve a statistically significant difference from placebo in any active dose group for the primary efficacy endpoint. . . . . The data indicated considerable overlap in results between the active and placebo groups for the secondary endpoints as well, and no clear dose effect was seen. (http://www.prnewswire.com/cgi-bin/stories.pl?ACCT=104&STORY=/ www/story/10-10-20... (October 10, 2006).) Corautus Genetics Announces Redirection of Focus and Transition Of Officers (App. Br. Appendix D) 19. This document describes an announcement from Corautus Genetics explaining that it “does not plan to conduct further clinical trials for VEGF-2 for the treatment of cardiovascular and peripheral vascular disease and is redirecting its focus to other life sciences opportunities” (http://www.prnewswire.com/cgi-bin/stories.pl?ACCT= 104&STORY= /www/story/11-03-20... (November 3, 2007)). Medical News Today Article: “Diabetic Neuropathy Treatment Has Passed The First Clinical Trial” (App. Br. Appendix E) 20. The Medical News Today article describes the following announcement: Appeal 2010-004652 Application 11/101,287 13 Sangamo BioSciences, Inc. (Nasdaq: SGMO) announced today positive results from the Phase 1 human clinical trial of SB-509, the Company’s ZFP Therapeutic for the treatment of diabetic neuropathy. Safety data and preliminary findings regarding improvement of symptoms were presented at the 58th Annual Meeting of the American Academy of Neurology in San Diego by David Cornblath, M.D., Professor of Neurology at The Johns Hopkins University School of Medicine and a consultant to Sangamo. The results are the first publicly reported data from a human clinical trial of a ZFP Therapeutic. (http://www.medicalnewstoday.com/printerfriendlynews.php?newsid=41158 (April 11, 2006).) 21. The Medical News Today article describes SB-509, the therapeutic agent, as follows: SB-509 is administered as an injectable formulation of plasmid DNA that encodes a zinc finger DNA- binding protein transcription factor (ZFP TFTM), designed to upregulate the VEGF-A gene. VEGF-A has been demonstrated to have direct neurotrophic and neuroprotective properties. In preclinical animal efficacy studies in a diabetic rat model, SB-509 has proven effective in protecting motor and sensory nerve function from disease-induced nerve damage. (Id.) 22. The Medical News Today article discloses: Dale Ando, M.D., Sangamo’s vice president of therapeutic development and chief medical officer [stated] . . . “that a single treatment of our ZFP Therapeutic resulted in improvements in symptoms of pain, numbness and nerve testing in a number of subjects. Most significantly, we did not observe any dose- limiting toxicity, and we were able to treat subjects within the pharmacologically effective dose range that we had demonstrated to be efficacious in preclinical animal studies. This is important, as previous therapies designed to halt or reverse the nerve deterioration that is characteristics of this Appeal 2010-004652 Application 11/101,287 14 condition had dose-limiting toxicities that prevented testing at dosing proven to be effective and tolerated in animal studies.” . . . “Existing treatments for diabetic neuropathy are limited to the use of antidepressants, analgesics or other agents for the management of pain,” commented Mark Kipnes, M.D., a principal clinical investigator for Sangamo and Endocrinologist at the Diabetes and Glandular Disease Clinic in San Antonio, Texas. (Id.) PRINCIPLES OF LAW As the Supreme Court pointed out in KSR Int'l Co. v. Teleflex Inc., 550 U.S. 398 (2007), when determining whether the prior art supplied a reason for practicing the claimed subject matter, the analysis “need not seek out precise teachings directed to the specific subject matter of the challenged claim, for a court can take account of the inferences and creative steps that a person of ordinary skill in the art would employ.” Id. at 418; see also id. at 421 (“A person of ordinary skill is . . . a person of ordinary creativity, not an automaton.”). The Court also reaffirmed that prima facie obviousness requires a reasonable expectation of success: 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. Id. at 421 (emphasis added). Appeal 2010-004652 Application 11/101,287 15 The KSR Court further reaffirmed that secondary considerations of non-obviousness, including long-felt but unsolved needs, should be weighed in the ultimate obviousness evaluation. Id at 406-407. ANALYSIS Appellant’s arguments do not persuade us that the cited references would have failed to provide an ordinary artisan with a reasonable expectation that Rebar’s VEGF-A-stimulating nucleic acid construct would successfully treat diabetic neuropathy when administered to patients suffering from that disorder. Nor are we persuaded that the cited references fail to suggest all of the claimed elements. Regarding Isner, we first note that the reference appears to present encouraging preliminary clinical, i.e. human, data in addition to the animal data that prompted the clinical trial proposal (FF 2, 3). Moreover, we are not persuaded that the document’s status as a clinical trial proposal undermines its value as a teaching that would have provided an ordinary artisan with a reasonable expectation that a plasmid encoding VEGF-A would successfully treat diabetic neuropathy. Rather, given that the preliminary data had so convinced the investigators of success that they were willing to subject a relatively large number of human patients to treatment with the VEGF-A-encoding plasmid (FF 4, 5), we agree with the Examiner that Isner would have prompted an ordinary artisan to treat diabetic neuropathy in humans using methods that increased the amount of VEGF-A in the target tissue. Cf., In re Merck & Co., Inc., 800 F.2d 1091, 1096-97 (Fed. Cir. 1986) (similarity of claim- designated compound to prior art compound, combined with prior art Appeal 2010-004652 Application 11/101,287 16 suggestion for testing in humans held sufficient to support prima facie case of obviousness for claims directed to human therapeutic treatment). We note, as Appellant argues, that Isner does not appear to describe administering a nucleic acid construct encoding a VEGF-A-targeted zinc finger protein, as recited in claim 1. However, as the Examiner points out, Isner teaches that its plasmid was useful for treating diabetic neuropathy because it stimulated angiogenesis (FF 3). As the Examiner also points out, Rebar’s nucleic acid construct, which encodes a VEGF-A-targeted zinc finger protein, stimulated angiogenesis in an animal model (FF 14). Thus, we agree with the Examiner that an ordinary artisan, advised by Isner that VEGF-A-generating, angiogenesis-stimulating nucleic acids were useful for treating diabetic neuropathy, and further advised by Rebar that nucleic acids encoding VEGF-A-targeted zinc finger proteins stimulated angiogenesis in an animal model by upregulating VEGF-A, would have been prompted to use Rebar’s VEGF-A-activating nucleic acids to stimulate angiogenesis and thereby treat diabetic neuropathy in humans. We also note Rebar’s disclosure that certain prior art suggests that proper VEGF-A isoform ratios are required to provide pro-angiogenic therapy (FF 15). However, Rebar explicitly discloses that its VEGF-A- targeted zinc finger proteins actually solve the isoform ratio problem (id.), and further discloses that administering the same nucleic acid as that recited in Appellant’s claim 1 actually stimulated angiogenesis in a mouse (FF 14). Thus, given Rebar’s teachings and successful in vivo experiments, we are not persuaded that concerns over VEGF-A isoform ratios would have dissuaded an ordinary artisan from administering VEGF-A-activating Appeal 2010-004652 Application 11/101,287 17 nucleic acid constructs to treat disorders disclosed as benefiting from angiogenesis-stimulating therapy, such as diabetic neuropathy. Nor are we persuaded that such concerns would have undermined the artisan’s reasonable expectation of success, given Rebar’s positive in vivo results. We also note Rebar’s disclosure that nucleic acid constructs encoding VEGF-A-suppressing zinc finger proteins can be used to treat diabetic retinopathy by suppressing, rather than activating, VEGF-A-generated angiogenesis (FF 10, 11). We acknowledge that diabetes underlies both diabetic retinopathy and diabetic neuropathy. However, Appellant presents no direct evidence that the specific symptomology of diabetic retinopathy would have been treated in the same way as the claimed disorder, diabetic neuropathy. To the contrary, Isner specifically teaches that angiogenesis-stimulating agents should be used to treat diabetic neuropathy (FF 3). Accordingly, the evidence of record does not suggest that an ordinary artisan would have considered Rebar’s disclosure regarding suppressing angiogenesis in diabetic retinopathy clearly relevant, much less predictive, of whether stimulating angiogenesis in the manner taught by Rebar and Isner would be useful in treating diabetic neuropathy. Rather, for the reasons discussed, we agree with the Examiner that an ordinary artisan would have been prompted by the cited references to treat diabetic neuropathy using agents that stimulate angiogenesis, such as Rebar’s nucleic acid constructs encoding VEGF-A-stimulating zinc finger proteins. Regarding the various press releases urged by Appellant as showing that an ordinary artisan would have lacked a reasonable expectation that the claimed nucleic acid construct would have treated diabetic neuropathy, we Appeal 2010-004652 Application 11/101,287 18 first note that every press release appears to have a publication date after the April 7, 2005 filing date of the instant application (see App. Br. Appendices A through E). Appellant has not adequately explained how or why these post-filing disclosures demonstrate the state of the art at the time the instant application was filed. Nor are we persuaded that the various press releases demonstrate that an ordinary artisan, prompted by Isner to administer angiogenesis-inducing therapeutic agents to diabetic neuropathy patients, would have lacked a reasonable expectation that Rebar’s angiogenesis-inducing nucleic acid would be useful in treating diabetic neuropathy. We note that the press release in Appendix A announces a clinical trial, apparently of VEGF-A (FF 16), and that the press release in Appendix B announces a clinical trial of VEGF-2 (FF 17), a very different protein than VEGF-A (see FF 8). However, Appellant points to no specific language in Appendix B’s press release mentioning any VEGF-A trial, nor does Appellant point to any specific teaching in either press release suggesting that any VEGF-A clinical trial failed to provide positive results. Thus, we are not persuaded that Corautus’ decision to perform a clinical trial using VEGF-2 would have suggested to an ordinary artisan that VEGF-A would be inactive in treating diabetic neuropathy. We also note Corautus’ decision, announced in the press releases in Appendices C and D, to abandon clinical trials for VEGF-2 (FF 18, 19). However, as noted above, VEGF-2 is a very different protein than the VEGF-A of Isner and Rebar, and is, in fact, “less potent than VEGF-A” (Rebar [0012] (FF 8)). Thus, we are not persuaded that Corautus’ decision to abandon its VEGF-2 clinical trials would have undermined an ordinary Appeal 2010-004652 Application 11/101,287 19 artisan’s reasonable expectation that VEGF-A-activating, angiogenesis- stimulating, nucleic acids would be useful for treating diabetic neuropathy. Nor are we persuaded that the secondary considerations of non-obviousness outweigh the Examiner’s prima facie case. We acknowledge Isner’s disclosure that diabetic neuropathy is a pernicious disorder (FF 3), and also acknowledge Sangamo’s press release regarding the positive results obtained using, apparently, a nucleic acid encompassed by claim 1 (FF 20, 21). We further acknowledge the statements in the Sangamo press release to the effect that the described agent is advantageous when compared to other therapies (FF 22). We are not persuaded, however, that this evidence shows that treating diabetic neuropathy was an unmet need. Specifically, the Sangamo press release concedes that “previous therapies” and “[e]xisting treatments” for the disorder were available (FF 22). Moreover, at the time Appellant’s application was filed, Isner had also already met this need by teaching that diabetic neuropathy should be treated using VEGF-A-generating, angiogenesis-stimulating, nucleic acids (FF 2-4). Accordingly, we are not persuaded that the evidence proffered by Appellant to show a long-felt but unmet need is sufficient to overcome the Examiner’s prima facie case of obviousness. In sum, for the reasons discussed, we agree with the Examiner that an ordinary artisan would have been prompted by Isner and Rebar to administer a nucleic acid construct encoding a VEGF-A-activating zinc finger protein to human patients suffering from diabetic neuropathy. As discussed above, we are not persuaded that the evidence regarding the secondary considerations of non-obviousness is sufficient to outweigh the Examiner’s Appeal 2010-004652 Application 11/101,287 20 prima facie case. Accordingly, we affirm the Examiner’s obviousness rejection of claim 1, as well as claims 2 and 3, which fall with claim 1. TIME PERIOD 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 alw ROBINS & PASTERNAK 1731 EMBARCADERO ROAD SUITE 230 PALO ALTO, CA 94303