13392570 (P.T.A.B. Aug. 30, 2016)

Ex Parte Farries et al

Patent Trial and Appeal BoardAug 30, 2016

13392570 (P.T.A.B. Aug. 30, 2016)

UNITED STA TES p A TENT AND TRADEMARK OFFICE APPLICATION NO. FILING DATE FIRST NAMED INVENTOR 13/392,570 03/12/2012 Timothy Parries 22925 7590 09/01/2016 PHARMACEUTICAL PATENT ATTORNEYS, LLC 55 MADISON A VENUE 4THFLOOR MORRISTOWN, NJ 07960-7397 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. Ark- GB0916997 1063 EXAMINER HAMMELL, NEIL P ART UNIT PAPER NUMBER 1636 NOTIFICATION DATE DELIVERY MODE 09/01/2016 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@LicensingLaw.net administration@LicensingLaw.net PTOL-90A (Rev. 04/07) UNITED STATES PATENT AND TRADEMARK OFFICE BEFORE THE PATENT TRIAL AND APPEAL BOARD Ex parte TIMOTHY F ARRIES and DAVID ECKLAND 1 Appeal2015-001484 Application 13/392,570 Technology Center 1600 Before JEFFREY N. FREDMAN, RYAN H. FLAX, and DEVON ZASTROW NEWMAN, Administrative Patent Judges. NEWMAN, Administrative Patent Judge. DECISION ON APPEAL This is an appeal under 35 U.S.C. Â§ 134 involving claims 19-46 to gene therapies for cancer, which have been rejected as anticipated, obvious and nonenabled. We have jurisdiction under 35 U.S.C. Â§ 6(b ). We reverse. STATEMENT OF THE CASE Background "Malignant glioma is a cancerous tumour that is confined to the brain and only rarely spreads further." (Spec. 1: 10-11 ). "The current standard 1 Appellants identify the Real Party in Interest as Fin Vector Vision Therapies Ltd. (App. Br. iv). Appeal2015-001484 Application 13/392,570 therapy involves surgically removing the solid tumour mass and initiating radiotherapy and/or chemotherapy." (Id. at 1:11-13). "Currently most available cancer medicines are generally very toxic and many do not readily reach the brain tumour." (Id. at 1:15-16). "The present invention is based on a study, which shows that locally administered antigens in combination with a pre-existing immunoresponsiveness to those antigens, enhances the efficacy of an adenoviral-based gene therapy treatment for glioma." (Id. at 2:28-31). The Issues A. Claims 19-24 are rejected under 35 U.S.C. Â§ 102(b) as being anticipated by Yla-Herttuala. 2 B. Claim 25 is rejected under 35 U.S.C. Â§ 103(a) as being unpatentable over Yla-Herttuala and Ulasov. 3 C. Claims 33-38 are rejected under 35 U.S.C. Â§ 103(a) as being unpatentable over Yla-Herttuala and King. 4 D. Claim 39 is rejected under 35 U.S.C. Â§ 103(a) as being unpatentable over Yla-Herttuala, King, and Ulasov. 2 U.S. Pat. No. 6,579,855 Bl, issued June 17, 2003. 3 IV Ulasov et al., Combination of adenoviral virotherapy and temozolomide chemotherapy eradicates malignant glioma through autophagic and apoptotic cell death in vivo, 100 BRITISH JOURNAL OF CANCER 1154--1164 (2009). 4 Gwendalyn D. King et al., High-Capacity Adenovirus Vector-Mediated Anti-Glioma Gene Therapy in the Presence of Systemic Antiadenovirus Immunity, 82 JOURNAL OF VIROLOGY 4680-4684 (2008). 2 Appeal2015-001484 Application 13/392,570 E. Claims 19--39 are rejected under 35 U.S.C. Â§ 112, first paragraph, as nonenabled. Anticipation ISSUE Does the preponderance of evidence of record support the Examiner's finding that Yla-Herttuala discloses the invention of claims 19--24? FACTUAL FINDINGS (FF) FF 1. The Specification teaches that In a preferred embodiment, stimulation of the immune system is used to increase the immunoresponsiveness of the patient that is to be administered vector antigens to enhance the therapeutic efficacy of the gene therapy adenoviral vector. This immunostimulation may be achieved by either nonspecific activation of immune reactions or by stimulation specifically relating to the therapy by the immunogens (or antigens) of the gene therapy vector, or the tumour. (Spec. 4:3-9). FF 2. Yla-Herttuala teaches that patients "underwent craniotomy and tumour resection" after which the "diagnosis of malignant glioma was confirmed .... " (Yla-Herttuala 3:17-30). FF 3 Yla-Herttuala teaches that "[a]fter tumour resection, HSVtk retrovirus packaging cells were injected into the wall of the tumour cavity" of patients. (Id. at 3:30-34). FF 4 Yla-Herttuala teaches that "[a]nti-virus antibodies were measured before and two weeks after the gene transfer." (Id. at 4:9--10). 3 Appeal2015-001484 Application 13/392,570 FF 5 Yla-Herttuala teaches an increase in adenovirus antibodies in 3 of 7 Adv/tk-treated patients. (Id. at 5:48-50). These patients had a measurable antivirus titer as opposed to the remaining four, who had no measurable titer. (Id. at Table 1 ). Based on these data, we find that not all the patients studied in Yla-Herttuala had measurable baseline antiviral immunity prior to administration of the viral vector; therefore, confirmation of measurable level of immunity was not required to proceed to viral vector administration. ANALYSIS Appellants' independent claim 19 is reproduced below: 19. In a method of treating cancer in a human by partial or complete resection of tumor from said human, the improvement comprising: a. Determining the level of immunity against a viral vector, b. Confirming said human has a measurable level of immunity against said vector, and c. Administering to said human said viral vector. The Examiner finds that Yla-Herttuala teaches "resecting malignant gliomas from human patients," "determining and confirming a measurable level of immunity against a viral vector," and "administering the viral vector to the patients." (Ans. 2). As Yla-Herttuala performs the step of measuring antibodies both before and after administration of the viral vector, rather than exclusively before administration (FF 3--4), the Examiner's rejection requires that the steps of claim 19 be performed out of the order they are written: 4 Appeal2015-001484 Application 13/392,570 Applicants acknowledge that Yla-Herttuala determined and confirmed a measurable level of immunity in 3 out of the 7 Adv/tk-treated patients []. Therefore, it is clear that Yla- Herttuala determined and confirmed a measurable level of immunity against the vector. As discussed above, the claims do not require that this determination and confirmation occurs before the administration of the viral vector. (Final Act. 15). Appellants argue that Yla-Herrtuala cannot anticipate because the steps of claim 19 are limited to the "specific order there specified" by the prosecution history, the physical nature of the steps, and the literal claim language. (App. Br. 4--5). We find that the broadest reasonable interpretation of claim 19 requires that continuing the method to step "c," that is, administering the viral vector, first requires confirmation at step "b" that the patient has a measurable level of immunity against the vector; otherwise the method does not continue to step "c." See In re Am. A cad. of Science Tech Center, 367 F.3d 1359, 1364 (Fed. Cir. 2004) ("The Patent and Trademark Office ('PTO') determines the scope of claims in patent applications not solely on the basis of the claim language, but upon giving claims their broadest reasonable construction 'in light of the specification as it would be interpreted by one of ordinary skill in the art."'). While Yla-Herttula does disclose measuring antibodies before and after injecting HSVtk retrovirus, it is not disputed that Yla-Herttuala does not disclose that one must first confirm measurable immunity before then administering an injection. (see, e.g., Final Act. 17). Because the process 5 Appeal2015-001484 Application 13/392,570 disclosed by Yla-Herttuala does not so restrict its viral vector administration step, it does not disclose the claimed method. We are persuaded by Appellants' argument that the language of claim 19 mandates that the steps be implemented in the sequence as written. (App. Br. 7). In particular, we find the claim terms "said human" and "said vector/said viral vector" would lack antecedent basis if not read in the order claim 19 is written. In addition, this interpretation is consistent with the Specification, which states that "stimulation of the immune system is used to increase the immunoresponsiveness of the patent that is to be administered vector antigens to enhance the therapeutic efficacy of the gene therapy adenoviral vector." (FF 1, emphasis added). In order for vector antigens to be administered after immunoresponsiveness is increased, claim 19 must be performed in the order as written. Accordingly, we find Yla-Herttuala does not anticipate claim 19 because Yla-Herttuala does not perform the steps of the claimed method in the same way as recited in claim 19. See Net MoneyIN, Inc. v. VeriSign, Inc., 545 F.3d 1359, 1371 (Fed. Cir. 2008). ("[U]nless a [prior art] reference discloses within the four comers of the document not only all of the limitations claimed but also all of the limitations arranged or combined in the same way as recited in the claim, it cannot be said to prove prior invention of the thing claimed and, thus, cannot anticipate under 35 U.S.C. Â§ 102. ") We do not find it necessary to reach Appellants' other arguments on this issue. 5 5 Although we do not reach Appellants' other arguments, we note multiple occasions where Appellants' counsel disparages the Examiner (See, e.g., Reply 6 Appeal2015-001484 Application 13/392,570 Obviousness ISSUE Does the preponderance of evidence on this record support the Examiner's finding that Yla-Herttula and Ulasov render obvious the invention of claim 25? ANALYSIS Based on the combination of Yla-Herttuala and Ulasov, the Examiner concludes that, at the time Appellants' invention was made, it would have been obvious to "have modified the method of Yla-Herttuala by further administering temozolaminde ... for the advantage of treating the glioma." (Ans. 3). The Examiner, however, has not established that Ulasov makes up Br. 3, 7). We remind Appellants of the requirement to conduct all business with the Office with decorum and courtesy. Applicants and their attorneys or agents are required to conduct their business with the United States Patent and Trademark Office with decorum and courtesy. Papers presented in violation of this requirement will be submitted to the Director and will not be entered. A notice of the non-entry of the paper will be provided. Complaints against examiners and other employees must be made in correspondence separate from other papers. 37 C.F.R. Â§ 1.3 ("Business to be conducted with decorum and courtesy"). We find comments such as those do not represent Appellants' best interests, arguably violate at least the spirit of Rule 1.3, and are not helpful in aiding the Board to properly resolve the issues necessary to render a decision on the merits. 7 Appeal2015-001484 Application 13/392,570 for the deficiency of Yla-Herttuala, as discussed above. Accordingly, we find the preponderance of evidence on this record does not support the Examiner's finding on this issue. ISSUE Does the preponderance of evidence on this record support the Examiner's finding that Yla-Herttula and King render obvious the invention of claims 33-38? FACTUAL FINDINGS (FF) FF 6 King teaches that rats were "systemically immunized [] with a first- generation Ad[ enovirus ]" or control saline, then "rat glioma cell line CNS-I" was implanted into their striata. (King 4681 i-f 2). "One week later, groups of animals received an intratumoral injection of Ad- TKL, HC-Ad-TK, Ad-B-galactosidase [], HC-Ad- Bgal, or saline." (Id.) FF 7 King discloses that "only treatment with HC-Ad-TK significantly extended the survival of preimmunized rats." (Id.) ANALYSIS Appellants' independent claim 33 is reproduced below: 33. A method comprising: a. diagnosing cancer in a human, and then b. in any sequence: - performing a partial or complete resection of tumor from said human, and 8 Appeal2015-001484 Application 13/392,570 - determining the level of immunity against a viral vector, and confirming said human has a measurable level of immunity against said vector; and then c. Administering to said human said viral vector. Based on the combination of Yla-Herttula and King, the Examiner concludes that, at the time Appellants' invention was made, it would have been obvious to have modified the method of Yla-Herttuala by determining and confirming whether a patient had a measurable level of immunity against a viral vector prior to administering to the human the viral vector ... because this would have been important to inform whether one should administer a first- generation adenoviral vector or a second-generation high- capacity adenoviral vector. 6 (Ans. 5). The Examiner further states "[t]he claims broadly recite 'viral vector' and therefore encompass any viral vector including first-generation and second-generation adenoviral vectors." (Ans. 16). According to the Examiner The rejection argues that in the event that one determined and confirmed a measurable level of immunity to a viral vector in a human, one would have chosen to administer the second- 6 The Examiner's reference to a "second-generation high capacity adenoviral vector" refers to HC-Ad-TK, which is an adenovirus but is not the same adenovirus that was first injected into the rats in King. (King 4681 i-f 2). It is therefore a second-generation adenovirus with respect to the injected adenovirus. 9 Appeal2015-001484 Application 13/392,570 (Id.). generation HC-Ad-TK viral vector as taught by King because this would have been more likely to be able to effectively treat the glioblastoma. The Examiner finds King teaches that T-cells recognize the expression of viral epitopes from first-generation adenoviral vectors in infected cells leading to T-cell immunity ... and further that the presence of preexisting immune responses against first- generation adenoviral vectors hampers therapeutic transgene expression resulting in diminished clinical efficacy of the treatment .... In contrast, even in the presence of a pre-existing immune response, since second-generation adenoviral vectors do not express viral antigenic epitopes in infected cells, anti- adenovirus immune T cells do not have any adenovirus-derived epitopes that they can recognize on infected cells, and thus transgene expression from such vectors remains stable in infected cells. (Ans. 17, emphasis added). The Examiner further finds "King concludes that the administration of second-generation adenoviral vectors represents a powerful treatment for glioblastomas even in patients who have a preexisting immune response to the adenovirus." (Id.) Appellants argue King "expressly teaches away from using Yla- Herttuala's viral vector in immune incompetent patients." (App. Br. 8). We find the Examiner has not established a prima facie case of obviousness on these references. We have discussed the deficiency of Yla- Herttuala above and find that King does not address that deficiency. 10 Appeal2015-001484 Application 13/392,570 King teaches success through administration of a first-generation viral vector and treatment using a second-generation viral vector. King teaches away from use of a first-generation viral vector as the "said viral vector" to be administered in the last step of claim 33. Rather, King teaches the second generation vector is a "powerful treatment for glioblastomas" and "only treatment with HC-Ad-TK significantly extended the survival of preimmunized rats." (Ans. 1 7; King 4 6 81 i1 2). We find the second generation vector of King cannot be used to perform the method of claim 33 because the recited step of "confirming said human has a measurable level of immunity against said vector" requires that the vector express a viral antigenic epitope, against which the detected immune response is mounted. This "said vector" is the same vector that is later administered to the patient in the final step "[a ]dministering to said human said viral vector." As discussed above regarding construction of the claims at issue, we find the "said viral vector" in the final step of claim 33 must be identical to the first referenced viral vector for the claim to make sense. Nor can the second generation vector disclosed by King be used in the claimed method because it does not express a viral antigenic epitope against which an immune response can be generated and later measured. (Ans. 17). Accordingly, we find King does not remedy the deficiencies of Yla- Herttuala. 11 Appeal2015-001484 Application 13/392,570 ISSUE Does the preponderance of evidence on this record support the Examiner's finding that Yla-Herttula, King, and Ulasov render obvious the invention of claim 39? ANALYSIS Based on the combination of Yla-Herttuala, King, and Ulasov, the Examiner concludes that, at the time Appellants' invention was made, it would have been obvious to "have modified the method of Yla-Herttuala by further administering temozolaminde ... for the advantage of treating the glioma." (Ans. 6). The Examiner has not established that Ulasov remedies the deficiencies in Yla-Herttuala and King for the reasons discussed above. Enablement ISSUE Does the preponderance of evidence on this record support the Examiner's finding that claims 19-46 are not enabled? FACTUAL FINDINGS FF 8 The Specification discloses According to a second aspect, the present invention is a product comprising an immunostimulant and a vector comprising a transgene that promotes death of neoplastic cells, for simultaneous, sequential or separate administration in the treatment of cancer. 12 Appeal2015-001484 Application 13/392,570 According to a third aspect, the present invention is a method of selecting patients for treatment with a product as defined above, comprising determining ex vivo the level of immunity against the vector, in a sample taken from a patient, and selecting the patient for treatment if the level of immunity is above a predetermined level. (Spec. 3:1-14). ANALYSIS The Examiner rejected claims 19-25 and 33-39 because the specification, ... does not reasonably provide enablement for determining the level of immunity against a viral vector that does not comprise a transgene or comprises any transgene and any route of administration of the viral vector. The specification does not enable any person skilled in the art to which it pertains, or with which it is most nearly connected, to practice the invention commensurate in scope with these claims. (Ans. 7). The Examiner finds the Specification "teaches a single example" in which "the viral vector is injected to the brain tumor cavity resulting from the tumor resection." (Id.) The Examiner cites a literature review in support of the Examiner's concern regarding the safety and efficacy of the claimed method (id. at 8-9) and finds that "the specification does not provide a single working example of a human who had an immune response to a viral vector 'induced' and then the administration of the viral vector treated cancer as recited in the preamble." (Id. at 17-18). The Examiner further 13 Appeal2015-001484 Application 13/392,570 finds the claims are "sufficiently broad that they encompass treating cancer by administering just any viral vector." (Id. at 9). Appellants argue the Specification provides an enabling disclosure and that the Examiner "provides no evidence to doubt the objective truth of the inventors' disclosure." (App. Br. 9). Appellants cite to evidence in the record provided by the Examiner that teaches "a viral vector that does not comprise a transgene" and a method for "determining the level of immunity against a viral vector." (Id. at 10). Appellants argue that because "determining immunity against viral vector given by 'any route of administration' is known," their Specification need not teach it. (Id. at 11 ). While we share the Examiner's concern that methods of treating patients must be made safe, the scope of our review on this issue concerns only whether Appellants have enabled the claimed methods. Considerations about safety are entertained by the Food and Drug Administration (FDA), not the Patent and Trademark Office. See In re Brana, 51F.3d1560, 1567 (Fed. Cir. 1995). We are not persuaded by the Examiner's concern that one of skill in the art could not measure immunity relative to the vector. The Specification describes a method of inducing an immune response using a viral vector (FF 1, FF 8) and data reflecting success in measuring the immune response. (Spec, Tables 1-2). Subsequent steps of the claimed methods either represent techniques known to one of ordinary skill in the art, such as "[a]dministering to said human said viral vector" or adding a medication such as temozolamide, or narrow the claims by specifying the type of vector 14 Appeal2015-001484 Application 13/392,570 (e.g., transgene), type of cancer (e.g., glioma) or further describe a method step (e.g., administering to the cavity created by resection of said tumor). We do not find the teachings of King helpful on the issue of the scope of enablement as that reference focused on success obtained using a second generation vector to which there was no detected immunity due to a lack of expressed epitopes, as discussed above. With regard to general scope of the claims, we find the invention is constrained by the claim language and the Specification in that an immune response must be detected in the subject prior to administration of the viral vector, as discussed above. Therefore, we find the claims are adequately enabled within the provided scope. See AK Steel Corp. v. Sollac, 344 F.3d 1234, 1244 (Fed. Cir. 2003) (citation omitted). ("[A]s part of the quid pro quo of the patent bargain, the applicant's specification must enable one of ordinary skill in the art to practice the full scope of the claimed invention. That is not to say that the specification itself must necessarily describe how to make and use every possible variant of the claimed invention, for the artisan's knowledge of the prior art and routine experimentation can often fill gaps, interpolate between embodiments, and perhaps even extrapolate beyond the disclosed embodiments, depending upon the predictability of the art.") In any event, "[i]t is well settled that patent applicants are not required to disclose every species encompassed by their claims, even in an unpredictable art." In re Angstadt, 537 F.2d 498, 502---03 (CCPA 1976). Although the disclosure must provide enablement commensurate with the scope of the claims, "[t ]he enablement requirement is met if the description 15 Appeal2015-001484 Application 13/392,570 enables any mode of making and using the invention." Johns Hopkins Univ. v. Cellpro Inc., 152 F.3d 1342, 1361 (Fed. Cir. 1998) (quoting Engel Indus., Inc. v. Locliformer Co., 946 F.2d 1528, 1533 (Fed. Cir. 1991)). We find Appellants have sufficiently described a method of making and using the invention and that one of skill in the art could, guided by the Specification, apply ordinary skill to practice the claimed invention without undue experimentation. Accordingly, the preponderance of evidence does not support the Examiner's rejection on this issue. Conclusion of Law The preponderance of the evidence relied upon by the Examiner fails to support a finding of anticipation, obviousness or lack of enablement. SUMMARY The rejection of claims 19--24 under 35 U.S.C. Â§ 102(b) as being anticipated by Yla-Herttuala is reversed. The rejection of claim 25 under 35 U.S.C. Â§ 103(a) as unpatentable over Yla-Herttuala and Ulasov is reversed. The rejection of claims 33-38 under 35 U.S.C. Â§ 103(a) as unpatentable over Yla-Herttuala and King is reversed. The rejection of claim 39 under 35 U.S.C. Â§ 103(a) as unpatentable over Yla-Herttuala, King, and Ulasov is reversed. The rejection of claims 19--39 under 35 U.S.C. Â§ 112, first paragraph, as nonenabled is reversed. REVERSED 16