11582596 (P.T.A.B. Apr. 15, 2013)

Ex Parte Humphreys et al

Patent Trial and Appeal BoardApr 15, 2013

11582596 (P.T.A.B. Apr. 15, 2013)

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. 11/582,596 10/18/2006 Robert Humphreys AEX-2002US01 1958 7590 04/15/2013 Kevin M. Farrell Pierce Atwood Suite 350 One New Hampshire Avenue Portsmouth, NH 03801 EXAMINER KINSEY WHITE, NICOLE ERIN ART UNIT PAPER NUMBER 1648 MAIL DATE DELIVERY MODE 04/15/2013 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 PATENT TRIAL AND APPEAL BOARD __________ Ex parte ROBERT HUMPHREYS, DOUGLAS MACMILLAN POWELL, and JOHN ZINCKGRAF __________ Appeal 2012-000374 Application 11/582,596 Technology Center 1600 __________ Before DONALD E. ADAMS, ERIC GRIMES, and MELANIE L. McCOLLUM, Administrative Patent Judges. GRIMES, Administrative Patent Judge. DECISION ON APPEAL This is an appeal under 35 U.S.C. § 134 involving claims to a method of increasing the potency of a vaccine, which have been rejected as anticipated, obvious, and nonenabled. We have jurisdiction under 35 U.S.C. § 6(b). We affirm the rejections based on prior art but reverse the rejection for nonenablement. Appeal 2012-000374 Application 11/582,596 2 STATEMENT OF THE CASE The Specification states that the invariant chain (Ii) protein blocks antigenic peptide binding sites of newly synthesized MHC class II molecules, preventing them from binding endogenous antigenic peptides (Spec. 1-2, ¶ 3). “Complexes of MHC class II molecules and Ii protein are transported from the endoplasmic reticulum to a post-Golgi compartment where Ii is released by proteolysis after which a specific antigenic peptide binds to the MHC class II molecule. MHC class II molecules bind only exogenous antigens, internalized via endocytosis.” (Id.) The Specification states that application “11/033,039[1] disclose[s] . . . that an MHC Class II-restricted antigenic epitope which is covalently linked to a mammalian Ii-Key peptide by an appropriate intervening chemical structure, forming a hybrid polypeptide, is presented to T lymphocytes by antigen presenting cells with significantly higher efficacy than is the precursor antigenic epitope” (id. at 2, ¶ 5). “Ii-Key” is the immuno- regulatory motif within the Ii protein (id. at 9, ¶ 33). Claims 1-4 and 6-23 are on appeal. Claims 1, 8, and 19 are representative and read as follows: 1. A method for increasing the potency of a vaccine directed toward a pathogen of interest in a subject, the method comprising: a) providing a vaccine, the vaccine comprising an epitope-containing protein or portion thereof which is encoded by the genome of the pathogen, or a DNA encoding the same; b) providing an Ii-key hybrid construct comprising: i) the LRMK residues of Ii-key protein; and 1 Application 11/033,039 corresponds to the Humphreys ‘947 publication relied on by the Examiner. Appeal 2012-000374 Application 11/582,596 3 ii) an MHC class II epitope contained within the protein or portion thereof of step a); or; iii) DNA encoding the elements of i) and ii); c) priming the immune system of the subject by administering the Ii-key construct of step b) under conditions appropriate for the stimulation of an immune response in the subject; and d) administering the vaccine of step a) under conditions appropriate to boost the immune response of step c) thereby increasing the potency of the vaccine relative to a non-primed administration. 8. The method of Claim 1 wherein the subject is a bird. 19. The method of Claim 1 wherein the pathogen is HIV. The claims stand rejected as follows: • Claims 19-23 under 35 U.S.C. § 112, first paragraph, for lack of enablement (Answer 5); • Claims 1, 2, 4, 6, and 7 under 35 U.S.C. § 102(b) as anticipated by Humphreys ‘5942 (Answer 8); • Claims 1, 2, 4, 6, 7, and 10-18 under 35 U.S.C. § 102(e) as anticipated by Humphreys ‘9473 (Answer 11); • Claims 3, 8-18, 22, and 23 under 35 U.S.C. § 103(a) as obvious based on Humphreys ‘594, Kotsopoulou,4 Kallinteris,5 Humphreys (PharmaDD),6 and Hackett7 (Answer 14); and 2 Humphreys et al., US 2003/0235594 A1, Dec. 25, 2003. 3 Humphreys et al., US 2006/0002947 A1, Jan. 5, 2006. 4 Kotsopoulou et al., A Rev-Independent Human Immunodeficiency Virus Type 1 (HIV-1)-Based Vector That Exploits a Codon-Optimized HIV-1 gag- pol Gene, 74 J. VIROL. 4839-4852 (2000). 5 Kallinteris et al., Ii-Key/MHC class II epitope hybrid peptide vaccines for HIV, 21 VACCINE 4128-4132 (2003). Appeal 2012-000374 Application 11/582,596 4 • Claims 3, 8, 9, 22, and 23 under 35 U.S.C. § 103(a) as obvious based on Humphreys ‘947 and Kotsopoulou (Answer 17-18). I. The Examiner has rejected claims 19-23 under 35 U.S.C. § 112, first paragraph, on the basis that the Specification does not provide sufficient guidance to enable those skilled in the art to make and use an HIV vaccine (Answer 5-8). The Examiner finds that the term “vaccine” implies a preparation that provides actual protection from infection, not just increasing immune responses (id. at 6); that no HIV vaccine exists and developing one involves inherent difficulties (id.); that the Specification’s working examples do not show actual protection from HIV infection (id. at 7); and that the state of the art in HIV vaccine development is unpredictable (id. at 8). The Examiner therefore concludes that undue experimentation would be required to practice the claimed method (id.). Appellants argue that those skilled in the art do not require a preparation to provide complete protection to qualify as a “vaccine” (Appeal Br. 4-5) and that the “invention is directed towards ‘increasing the potency’ . . . of a vaccine and not directed towards providing ‘complete protection’” 6 Humphreys et al., Synthetic Peptide Vaccine Against Pandemic H5N1 Influenza Based on Li-Key Modifies MHC Class II Epitopes, PHARMADD, May/June 2006, www.pharmadd.com/archives/May_16_2006/BN%20Tech%20Brief.asp (accessed Dec. 27, 2006). 7 Hackett et al., Immunogenic Peptides of Influenza Virus Subtype N1 Neuraminidase Identify a T-Cell Determinant Used in Class II Major Histocompatibility Complex-Restricted Responses to Infectious Virus, 65 J. VIROL. 672-676 (1991). Appeal 2012-000374 Application 11/582,596 5 (id. at 6). Appellants “submit that the pending specification provides adequate working examples to support the presently pending claims” (id.) and that “it would not require undue experimentation to practice the invention as claimed in pending Claims 19-23” (id. at 7). We agree with Appellants that the Examiner has not provided an adequate basis for concluding that practicing the method defined by claims 19-23 would require undue experimentation. As Appellants pointed out, the claims are not directed to a vaccine against HIV or a method of vaccinating against HIV. Claim 19 is directed to a “method for increasing the potency of a vaccine directed toward a pathogen of interest in a subject” (claim 1), “wherein the pathogen is HIV” (claim 19). Thus, the claims do not require generating an immune response that provides complete protection, or any specific degree of protection, from HIV infection, only that the potency of an HIV vaccine is increased relative to vaccination with an HIV antigen alone. The Examiner acknowledges that the “specification contains examples showing the immunogenicity of the HIV gag protein” (Answer 7). Appellants state that “paragraphs [0015] and [0070] and Figure 2 of the pending specification ‘demonstrate that T cell responses can be further improved by priming with Ii-Key peptides’ and ‘revealed IFN-gamma responses that were approximately two-fold stronger that [sic] either of the DNA vaccine regimes’” (Appeal Br. 6). The Examiner does not dispute this characterization of the Specification’s data. In short, the nonenablement rejection is based upon a requirement to obtain results – clinically effective protection from HIV infection – that are Appeal 2012-000374 Application 11/582,596 6 not required by the claims on appeal. The Examiner has not provided evidence or persuasive technical reasoning to show that a person of ordinary skill in the art would have expected that practicing the method defined by claim 19, to produce the results recited in the claim, would have required undue experimentation. II. Issue The Examiner has rejected claims 1, 2, 4, 6, and 7 as anticipated by Humphreys ‘594 (Answer 8), and has rejected claims 1, 2, 4, 6, 7, and 10-18 as anticipated by Humphreys ‘947 (Answer 11). Humphreys ‘947 is a continuation-in-part of Humphreys ‘594 (Humphreys ‘947, front page), the Examiner relies on the same disclosures in both references in rejecting claim 1, and Appellants present the same argument in response to both rejections. We will therefore address them together. The Examiner finds that both Humphreys references disclose hybrid peptides comprising the LRMK core motif from the Ii-Key peptide, coupled to an MHC class II epitope (Answer 9, 12). The Examiner also finds that both Humphreys references state “that ‘this invention relates to the use of Ii- Key/antigenic epitope hybrids to enhance protective immune responses to a subsequently administered DNA vaccine or against an attenuated pathogen vaccine’” (id. at 10, 13). The Examiner concludes that both Humphreys references teach “that priming the immune system with the Ii-key/antigen hybrid peptide followed by administration of the antigen (e.g., protein antigen or DNA encoding the antigen) will result in an enhanced immune response” (id.). Appeal 2012-000374 Application 11/582,596 7 Appellants contend that neither Humphreys reference provides sufficient guidance to enable a person of ordinary skill in the art to practice the instantly claimed invention “without the teachings of the presently pending application” (Appeal Br. 8, 11). The issue with respect to this rejection is: Have Appellants shown that the Humphreys references are not enabling for increasing the potency of a vaccine directed to a pathogen? Findings of Fact 1. Both Humphreys references disclose “an antigen presentation enhancing hybrid polypeptide which includes three elements”: (1) “an N-terminal element consisting essentially of 4-16 residues of the mammalian Ii-Key peptide,” (2) a polypeptide that binds to the antigenic peptide binding site of an MHC class II molecule, and (3) “a chemical structure covalently linking the N-terminal element . . . to the MHC Class II-presented epitope.” (Humphreys ‘594, ¶ 7; Humphreys ‘947, ¶ 8.) 2. Both Humphreys references disclose that “modified Ii key peptides which retain antigen presentation enhancing activity will function in the enhancing hybrid of the present invention. . . . Examples of modified versions of Ii key peptide which are known to retain high activity are LRMK,” among others. (Humphreys ‘594, ¶ 28; Humphreys ‘947, ¶ 29.) 3. Both Humphreys references disclose “the use of Ii-Key/antigenic epitope hybrids to enhance protective immune responses to a subsequently administered DNA vaccine or against an attenuated infectious pathogen vaccine. Such adjuvant vaccine preparations can be referred to as PreVaccinesTM.” (Humphreys ‘594, ¶ 114; Humphreys ‘947, ¶ 115.) Appeal 2012-000374 Application 11/582,596 8 4. Both Humphreys references disclose that, [i]n the case of smallpox vaccination, Ii-Key antigenic epitope hybrids are used to elicit a Th1 response to one or more MHC Class II-presented epitopes of the gp42 extracellular envelope protein coded by the B5R viral gene of vaccinia. Individuals so vaccinated will have an anamnestic response which is more rapid and of higher potency in terms of antibody titers . . . to challenge by cDNA vaccines for the B5R gene. (Humphreys ‘594, ¶ 114; Humphreys ‘947, ¶ 115.) Analysis Both Humphreys references disclose a method meeting all of the limitations of claim 1. The disclosed method includes providing a vaccine comprising a pathogen protein or DNA (FF3, FF4), providing an Ii-Key hybrid peptide comprising the LRMK residues of Ii-Key (FF2) and an MHC Class II epitope from the pathogen’s protein (FF4), priming the immune system with the hybrid protein (FF3), and administering the vaccine under conditions that boost the immune response of the subject to the vaccine (FF4). Appellants argue, however, that “one of skill in the art would not have been able at the time of filing to practice the present invention without undue experimentation in view of the cited Humphreys publication[s] without the teachings of the presently pending application” (Appeal Br. 8, 11). Appellants do not identify any specific teachings in the present Specification that would provide the guidance allegedly missing from the Humphreys references. Instead, Appellants present an analysis of the Humphreys references based on the factors of In re Wands, 858 F.2d 731, 737 (Fed. Cir. 1988) (Appeal Br. 9-13). Appeal 2012-000374 Application 11/582,596 9 Appellants’ argument is not persuasive. “[A] prior art publication cited by an Examiner is presumptively enabling barring any showing to the contrary by a patent applicant.” In re Antor Media Corp., 689 F.3d 1282, 1288 (Fed. Cir. 2012). “As long as an examiner makes a proper prima facie case of anticipation by giving adequate notice under § 132, the burden shifts to the applicant to submit rebuttal evidence of nonenablement.” Id. at 1289. Appellants’ Wands analysis of the Humphreys references is not supported by citation to evidence showing that the references do not provide adequate guidance to enable one skilled in the art to enhance the potency of a vaccine by carrying out the steps recited in claim 1, which are the same steps recited in both Humphreys references. Appellants’ unsupported attorney argument is not “rebuttal evidence of nonenablement,” In re Antor Media Corp., 689 F.3d at 1289, and therefore is inadequate to show that the Humphreys references are not enabling for the method of claim 1. Appellants also argue that the Humphreys references do not specify “whether the MHC Class II epitope contained within the Ii-Key construct is necessarily the same epitope encoded by the DNA vaccine. . . . [T]he subject application specifically requires that the Ii-Key MHC Class II epitope is the same as the MHC Class II epitope contained within the vaccine protein.” (Appeal Br. 9, 12.) This argument is also unpersuasive. Both Humphreys references expressly describe a method of priming a subject’s immune system using an Ii-Key hybrid protein comprising the gp42 envelope protein encoded by the B5R viral gene, which produces a response of “higher potency in terms of antibody titers . . . to challenge by cDNA vaccines for the B5R gene” (FF4). Appeal 2012-000374 Application 11/582,596 10 The references therefore describe a method that includes the disputed limitation. Conclusion of Law Appellants have not shown that the Humphreys references are not enabling for increasing the potency of a vaccine directed to a pathogen. We affirm the rejection of claim 1 as anticipated by both Humphreys ‘594 and Humphreys ‘947. Claims 2, 4, 6, 7, and 10-18 were not argued separately and therefore fall with claim 1. 37 C.F.R. § 41.37(c)(1)(vii). III. Issue The Examiner has rejected claims 3, 8-18, 22, and 23 as obvious based on Humphreys ‘594, Kotsopoulou, Kallinteris, Humphreys (PharmaDD), and Hackett (Answer 14); and has rejected claims 3, 8, 9, 22, and 23 as obvious based on Humphreys ‘947 and Kotsopoulou (Answer 17- 18). The claims subject to each rejection have not been argued separately and therefore stand or fall together. 37 C.F.R. § 41.37(c)(1)(vii). We select claim 8 as representative of the claims subject to each of the § 103 rejections. Claim 8 is directed to the method of claim 1, where the subject treated is a bird. The Examiner finds that “it is well within the purview of one of ordinary skill in the art to choose a subject in need of immunization (e.g., humans, birds, etc.)” (Answer 17, 18), and therefore the additional limitation of claim 8 would have been obvious to a person of ordinary skill in the art. Appellants argue that the Examiner Appeal 2012-000374 Application 11/582,596 11 has not shown why one of skill in the art would have combined these techniques without the benefit of the teachings of the present invention or how one of skill in the art would have predicted the success of the pending invention based solely in the identification of these disparate techniques without the benefit of the teachings of the present invention. (Appeal Br. 14, 17.) Appellants have not, however, provided evidence or sound technical reasons why a person of ordinary skill in the art would not have considered it obvious to practice the method disclosed by the Humphreys references on a subject that was a bird. We note that both Humphreys references describe their methods as applicable to a wide variety of diseases: “an infectious disease caused or associated with infection by a bacterium, a virus, a parasite, a fungus, a rickettsia, or other infectious agent” (Humphreys ‘594, ¶ 76; Humphreys ‘947, ¶ 77). In addition, Humphreys (PharmaDD) describes H5N1 influenza as a virus with “serious pandemic potential” and refers to it as “bird flu” (Humphreys (PharmaDD), at 4). The evidence of record thus supports the Examiner’s conclusion that it would have been obvious to practice the method disclosed by Humphreys ‘594 and Humphreys ‘947 on a subject that was a bird, for example in order to limit the spread of H5N1 bird flu. SUMMARY We reverse the rejection of claims 19-23 for lack of enablement. We affirm the rejection of claims 1, 2, 4, 6, and 7 as anticipated by Humphreys ‘594, and the rejection of claims 1, 2, 4, 6, 7, and 10-18 as anticipated by Humphreys ‘947. Appeal 2012-000374 Application 11/582,596 12 We affirm the rejection of claim 8 under 35 U.S.C. § 103(a) as obvious based on the combination of Humphreys ‘594, Kotsopoulou, Kallinteris, Humphreys (PharmaDD), and Hackett. Claims 3, 9-18, 22, and 23 fall with claim 8 because they were not argued separately. 37 C.F.R. § 41.37(c)(1)(vii). We affirm the rejection of claim 8 under 35 U.S.C. § 103(a) as obvious based on Humphreys ‘947 and Kotsopoulou. Claims 3, 9, 22, and 23 fall with claim 8 because they were not argued separately. 37 C.F.R. § 41.37(c)(1)(vii). 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 lp