15013469 (P.T.A.B. Dec. 10, 2018)

Ex Parte Simard

Patent Trial and Appeal BoardDec 10, 2018

15013469 (P.T.A.B. Dec. 10, 2018)

UNITED STA TES p A TENT AND TRADEMARK OFFICE APPLICATION NO. FILING DATE 15/013,469 02/02/2016 88684 7590 12/12/2018 XBiotech, Inc. 5425 Park Central Court Suite 111 Naples, FL 34109 FIRST NAMED INVENTOR John Simard 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. 5407-0244 8433 EXAMINER DENT, ALANA HARRIS ART UNIT PAPER NUMBER 1643 NOTIFICATION DATE DELIVERY MODE 12/12/2018 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): sakptomail@iplawpro.com PTOL-90A (Rev. 04/07) UNITED STATES PATENT AND TRADEMARK OFFICE BEFORE THE PATENT TRIAL AND APPEAL BOARD Ex parte JOHN SIMARD Appeal2017-010206 Application 15/013 ,469 Technology Center 1600 Before JEFFREY N. FREDMAN, ROBERT A. POLLOCK, and JACQUELINE T. HARLOW, Administrative Patent Judges. FREDMAN, Administrative Patent Judge. DECISION ON APPEAL This is an appeal 1,2,3 under 35 U.S.C. Â§ 134 involving claims to a method of reducing the formation of new metastases by administration of anti-human IL-1 a antibodies. The Examiner rejected the claims as anticipated and as obvious. We have jurisdiction under 35 U.S.C. Â§ 6(b). We affirm. 1 Appellant identifies the Real Party in Interest as XBiotech, Inc. (see Br. 3). 2 We have considered and refer to the Specification of Feb. 2, 2016 ("Spec."); Final Office Action of Sept. 8, 2016 ("Final Act."); Appeal Brief of Jan. 31, 2017 ("Br."); and Examiner's Answer of May 4, 2017 ("Ans."). 3 This appeal is related to Appeal 2013-002616 which affirmed the rejections in parent application US 12/302,066 (see Br. 4). Appeal2017-010206 Application 15/013,469 Statement of the Case Background "[A]nti-IL-la antibody can inhibit metastatic potential of tumors through interruption of the physiological role tumor-derived IL- I a plays in tumor metastasis. Moreover, because IL- I a is expressed by tumors, an antibody targeting IL- I a can cause direct tumor cytotoxicity through antibody directed cellular cytotoxicity" (Spec. ,r 6). The Claims Claims 1--4 are on appeal. Independent claim 1 is representative and is reproduced below: 1. A method of reducing the formation of new metastases comprising human cancer cells in a subject harboring said human cancer cells, the method comprising a step of administering to the subject an amount of anti-human IL- I a antibodies effective to reduce the development of new metastases in the subject, wherein the formation of new metastases in the subject is reduced. Br. 13 (Claims Appendix). The Issues A. The Examiner rejected claims 1 and 4 under 35 U.S.C. Â§ I02(b) as anticipated by Garrone '085 4 (Final Act. 3--4). B. The Examiner rejected claims 1 and 4 under 35 U.S.C. Â§ I02(b) as anticipated by Garrone '7665 (Final Act. 6-7). C. The Examiner rejected claims 1, 3, and 4 under 35 U.S.C. Â§ I02(b) as anticipated by Witte6 (Final Act. 4--5). 4 Garrone et al., US 5,959,085, issued Sept. 28, 1999. 5 Garrone et al., EP O 659 766 Al, published June 28, 1995. 2 Appeal2017-010206 Application 15/013,469 D. The Examiner rejected claims 1--4 under 35 U.S.C. Â§ I03(a) as obvious over Garrone '085, Witte, and Varnum 7 (Final Act. 7-9). E. The Examiner rejected claims 1--4 under 35 U.S.C. Â§ I03(a) as obvious over Garrone '766, Witte, and Varnum (Final Act. 10-12). A. &B. 35 USCÂ§ 102(b) over Garrone '085 and Garrone '766 Because the disclosures of Garrone '085 and Garrone '766 are similar, if not identical, we will consider these anticipation rejections together. The Examiner finds that Garrone '085 "discloses human monoclonal antibodies (HuMabs ), such as IL- I a for the treatment of tumors, see abstract; and column 11, lines 66 and 67" (Final Act. 4). The Examiner finds Garrone '766 teaches "human monoclonal antibodies against human cytokine, human interleukin alpha, see abstract. This antibody may be useful in tumor treatment, see page 8, last sentence of last full paragraph. This disclosure reads on treating new metastases because tumors comprise human cancer cells" (Final Act. 6-7). The issue with respect to this rejection is: Does the evidence of record support the Examiner's conclusion that Garrone '085 and Garrone '766 anticipate claims 1 and 4? Findings of Fact 1. Garrone '085 teaches that the "HuMAbs and fragments of the present invention may be used therapeutically to treat existing symptoms 6 Witte et al., US 2003/0026806 Al, published Feb. 6, 2003. 7 Varnum et al., US 2004/0097712 Al, published May 20, 2004. 3 Appeal2017-010206 Application 15/013,469 associated with the antigen of interest. For example, IL-la" (Garrone '085 11 :26-28; cf Garrone '766 8:34--35). 2. Garrone '085 teaches that "IL- I a has been reported to act as an autocrine growth stimulator for human thyroid and gastric carcinoma cells [Ito et al., Cancer Res., 53:4102-4106 (1993)], as well as adult T cell leukemias [Shirakawa et al., Cancer Res., 49:1143-1147 (1989)]. Thus, an anti-IL-la HuMAb of the invention may be useful in the treatment of tumors" (Garrone '085 11:62---67; cf Garrone '766 8:53-56). 3. Garrone '085 teaches "an antibody fragment such as an Fab, F(ab')2, Fv, single-chain binding protein, or any other binding polypeptide which contains one or more complementarity determining regions (CDRs)" (Garrone '085 9:10-14; cf Garrone '766 7:9-11). 4. Garrone '085 exemplifies the "ability of human monoclonal antibody X3 to inhibit the binding of radio labeled human IL- I a to IL- I receptors" and finds that "the antibody X3 blocks in a dose-dependent manner the binding of radio labeled human IL- I a on EL4 cells" ( Garrone '085 20:38-58; cf Garrone '766 15:51-16:4). 5. Garrone '085 teaches that the "concentration of the HuMAb or fragment of the invention in the pharmaceutical compositions may vary, e.g., from about 0.1 Âµg/ml to about 1 mg/ml ... The dose will be adjusted in a conventional manner by the skilled artisan to levels appropriate to achieve the desired result in vivo" (Garrone '085 12:39-47; cf Garrone '766 9:20- 24). 6. Garrone '085 teaches that "biological activity of human IL-I was measured by its ability to stimulate IL-2 production by the murine 4 Appeal2017-010206 Application 15/013,469 thymoma subline EL4-6.1" (Garrone '085 21:25-27; cf Garrone '766 16:25-26). 7. Garrone '085 teaches that the "proliferation of IL-2-dependent CTLL cells is proportional to the concentration of IL-2 produced by EL4 cells in the first step of culture" (Garrone '085 21:30-33; cf Garrone '766 16:28-29). 8. Garrone '085 teaches that the "human monoclonal antibody X3 specifically inhibits human IL-I a-induced IL-2 production by EL4 cells" (Garrone '085 21:64---65; cf Garrone '766 16:46-47). Principles of Law "The protocol of giving claims their broadest reasonable interpretation during examination does not include giving claims a legally incorrect interpretation. This protocol is solely an examination expedient, not a rule of claim construction." In re Skvorecz, 580 F.3d 1262, 1267 (Fed. Cir. 2009). Analysis Appellant contends the "sections of Garrone relied upon for this rejection do not expressly teach that' ... the formation of new metastases in the subject is reduced.' ... Accordingly, Garrone fails to expressly teach claim 1" (Br. 6-7). Appellant also contends Garrone "does not make clear that administering an anti-IL- I a antibody would inevitably result in the reduction of the development of new metastases in the subject" (id. at 7). The Examiner, in response, cites our discussion from the parent application Appeal 2013-002616, but does not specifically address the changes in claim 1 relative to the claims at issue in the previous case, 5 Appeal2017-010206 Application 15/013,469 specifically the addition of the clause "wherein the formation of new metastases in the subject is reduced." We therefore begin with claim interpretation. In our Decision in Appeal 2013-002616, there was no "wherein" clause, but simply a method of administering a particular dose of anti-human IL-I a antibodies. The "wherein" clause is reasonably assigned patentable weight consistent with Griffin, a case where the Federal Circuit addressed a claim to a "method for diagnosing an increased risk for thrombosis" comprising two steps of "obtaining" nucleic acids and "assaying" for point mutations and a final clause "wherein the presence of said point mutation in said test nucleic acid indicates an increased risk for thrombosis." Griffin v. Bertina, 285 F.3d 1029, 1031 (Fed. Cir. 2002). Griffin found that "the Board did not err in giving limiting effect to the 'wherein' clauses" because they give "meaning and purpose to the manipulative steps." Id. at 1033. Similarly here, the "wherein" clause limits the patient population to cancer patients who have cancers capable of metastasis, a subset of all cancer patients. The Examiner provides no specific explicit teaching or other evidence that either Garrone reference discloses treatment to a limited subset of cancer patients who are subject to metastasis. We also agree with Appellant that neither Garrone reference inherently addresses this limitation regarding the patient population of cancer patients subject to metastasis. Perricone distinguished inherency with regard to different patient populations, specifically between the topical application of a lotion to skin generally to prevent sunburn, and the topical application of a lotion to treat sunburned skin. Perricone v. Medicis Pharm. Corp., 432 F.3d 1368, 1378 (Fed. Cir. 2005). In Perricone, when treatment 6 Appeal2017-010206 Application 15/013,469 was applicable to any person with skin, inherency applied because everyone had skin, but Perricone found that when the patient population was limited to patients with sunburn the "issue is not ... whether [ the prior art] lotion if applied to skin sunburn would inherently treat that damage, but whether [the prior art] discloses the application of its composition to skin sunburn. It does not." Id. The same analysis applies here. There may be a general teaching in the Garrone references to treat cancer patients with anti-human IL-I a antibodies, and if those same patients also happened to be at risk of new metastases, the treatment might also necessarily result in reducing metastasis, analogous to the skin treatment at issue in Perricone. However, the Examiner has not established that all cancer patients are at risk of metastasis. In the same manner that not everyone who applies lotion to their skin will necessarily have sunburn, not all cancer patients will necessarily be at risk of new metastases. In re Oelrich, 666 F.2d 578, 581 (C.C.P.A. 1981) ("Inherency, however, may not be established by probabilities or possibilities. The mere fact that a certain thing may result from a given set of circumstances is not sufficient."). Conclusion of Law The evidence of record does not support the Examiner's conclusion that Garrone '085 and Garrone '766 anticipate claims 1 and 4. C. 35 USCÂ§ 102(b) over Witte The Examiner finds "Witte discloses IL- I a monoclonal and polyclonal antibodies and implementing these IL- I selective binding agents 7 Appeal2017-010206 Application 15/013,469 in a method of treating IL- I mediated diseases such a tumor metastasis" (Final Act. 5). The issue with respect to this rejection is: Does the evidence of record support the Examiner's conclusion that Witte anticipates claims 1, 3, and4? Findings of Fact 9. Witte teaches "humanized, fully human, single chain and/or bispecific antibodies. Antibody fragments include those portions of an anti- IL-1 antibody which bind to an epitope on an IL-I polypeptide" (Witt ,r 97). 10. Witte teaches that the "term 'IL-I' means that the text applies to IL-la or IL-I~" (Witte 48). 11. Witte teaches a "list of acute and chronic IL-1-mediated- diseases includes but is not limited to the following ... cancer, such as multiple myeloma and myelogenous (e.g., AML and CML) and other leukemias, as well as tumor metastasis" (Witte ,r,r 178, 188). 12. Witte teaches that "IL-I antagonist antibodies or antigen binding domains of the invention are administered in a therapeutically or prophylactically effective amount to prevent and/or treat loss of bone associated with metastatic bone disease" (Witt ,r 240). 13. Witte teaches that a "'therapeutically or prophylactically effective amount' of an IL-I antagonist antibody is that amount which affects a parameter of an IL- I mediated disease ... Typically, a clinician will administer the composition until a dosage is reached that achieves the desired effect" (Witte ,r,r 240-241 ). 8 Appeal2017-010206 Application 15/013,469 Analysis Appellant contends "Witte nowhere unequivocally states that tumor metastasis is a condition associated specifically with elevated IL- I a. According to Witte' s definitions, tumor metastasis could be only associated with elevated levels of IL- I a in bodily fluids or tissue, or in the supernatant of a culture of cells or tissues excised from a subject" (Br. 9). Appellant further contends Witte "does not make clear that administering an anti-IL-la antibody would inevitably result in the reduction of the development of new metastases in the subject, or even that IL- I a is involved in the formation of new metastases" (id.). The Examiner responds that the "antibodies of Witte and Appellant are one and the same, hence the treatment it provides result in the same therapeutic effect. Products of identical chemical composition cannot have mutually exclusive properties" (Ans. 8). The Examiner also finds that "when the species is clearly named, the species claim is anticipated no matter how many other species are additionally named" (Ans. 8, citing Ex parte A, 17 USPQ 1716 (BPAI 1990)). We rely upon our claim interpretation of the "wherein" clause as discussed above. We agree with the Examiner because Witte specifically teaches "IL- I antagonist antibodies ... are administered in a therapeutically or prophylactically effective amount to prevent and/or treat loss of bone associated with metastatic bone disease" (FF 12). Witte teaches "'IL-I' means that the text applies to IL- I a or IL- I W' (FF 10). Thus, Witte teaches administration of antibodies to either of only two different IL- I types, IL- I a or IL- I~' to patients to prevent or treat sequelae of metastatic bone disease (FF 10, 12). We think the Examiner reasonably interprets Witte's teaching 9 Appeal2017-010206 Application 15/013,469 to "prevent" metastatic bone disease as an express teaching to reduce formation of new metastases. Regarding inherency, we agree with the Examiner that Witte teaches treatment of a patient population that inherently are at risk of new metastases (FF 11-12). Thus, applying the Perricone analysis discussed above, Witte singles out the patient population at issue in claim 1, patients at risk of new metastases, and directly suggests treatment of those patients with the same anti IL- I a antibody composition as that required by claim 1 "to prevent and/or treat loss of bone associated with metastatic bone disease" (FF 12). "Using the same composition claimed ... in the same manner claimed ... naturally results in the same claimed ... benefits." Perricone, 432 F.3d at 1380. We therefore agree with the Examiner that Witte both expressly and inherently anticipates the rejected claims. Conclusion of Law The evidence of record supports the Examiner's conclusion that Witte anticipates claims 1, 3, and 4. D.&E. 35 USCÂ§ 103(a) over either Garrone '085 or Garrone '766, Witte, and Varnum Because the disclosures of Garrone '085 and Garrone '766 are similar, if not identical, we will consider these two obviousness rejections together. The Examiner finds "Garrone ['085] teaches HuMabs, such as IL-la for the treatment of tumors, see abstract; and column 11, lines 66 and 67. This disclosure reads on treating new metastases because these malignant growths comprise human cancer cells" (Final Act. 9). The Examiner 10 Appeal2017-010206 Application 15/013,469 acknowledges that Garrone '085 does not teach "that are polyclonal and the cancer affects the breast or prostate" (id.). The Examiner finds Witte teaches "IL- I polyclonal antibodies and implementing IL- I selective binding agents in a method of treating IL- I mediated diseases such a tumor metastasis" (Final Act. 9). The Examiner finds Varnum teaches "treating IL- I mediated diseases, such as prostate cancer, breast cancer and other malignancies with metastatic potential" (id.). The Examiner finds it obvious to "combine the teachings of all the references to manufacture IL- I a polyclonal antibodies and treat breast or prostate metastatic cancer with all types of antibodies cited herein" (id.). The issue with respect to this rejection is: Does the evidence of record support the Examiner's conclusion that Garrone '085 and Garrone '7 66, along with Witte and Varnum render claims 1--4 obvious? Findings of Fact 14. Varnum teaches that anti-IL- I RI antibodies, alone or in combination with other cytokine inhibitors or other active agents as described above, can be used to treat various forms of cancer, including acute myelogenous leukemia, chronic myelogenous leukemia leukemia, Epstein-Barr virus-positive nasopharyngeal carcinoma, glioma, colon, stomach, prostate, renal cell, cervical and ovarian cancers, lung cancer (SCLC and NSCLC), including cancer-associated cachexia, fatigue, asthenia, paraneoplastic syndrome of cachexia and hypercalcemia. Solid tumors, including sarcoma, osteosarcoma, and carcinoma, such as adenocarcinoma ( for example, breast cancer) and squamous cell carcinoma are also treatable. Additional treatable cancers include esophogeal cancer, gastric cancer, gall bladder carcinoma, leukemia, including acute myelogenous leukemia, chronic myelogenous leukemia, myeloid leukemia, chronic or acute 11 Appeal2017-010206 Application 15/013,469 lymphoblastic leukemia and hairy cell leukemia. Other malignancies with invasive metastatic potential, including multiple myeloma, can be treated with the subject compounds, compositions and combination therapies. (Varnum ,r 240). 15. Varnum teaches the "combination of an IL- I receptor antibody and RANKL inhibitors ... is useful for ... anti-tumor therapy aimed at preventing metastasis to bone" (Varnum ,r 230). Principles of Law [D]uring patent prosecution, an examiner is entitled to reject claims as anticipated by a prior art publication or patent without conducting an inquiry into whether or not that prior art reference is enabling. As long as an examiner makes a proper prima facie case of anticipation by giving adequate notice underÂ§ 132, the burden shifts to the applicant to submit rebuttal evidence of nonenablement. In re Antor Media Corp., 689 F.3d 1282, 1289 (Fed. Cir. 2012). However, "[o]nce an applicant makes a non-frivolous argument that cited prior art is not enabling[], the examiner must address that challenge." In re Morsa, 713 F.3d 104, 110 (Fed. Cir. 2013). Analysis We adopt the Examiner's findings of fact and reasoning regarding the scope and content of the prior art (Final Act. 7-12; FF 1-15) and agree that the claims are obvious over Garrone, Witte, and Varnum. We address Appellant's arguments below. Appellant contends "the examiner does not clearly state the differences between Witte and Varnum over claims 1-4, nor does it clearly resolve the level of ordinary skill in the pertinent art" (Br. 12). 12 Appeal2017-010206 Application 15/013,469 We do not find these arguments persuasive because the Examiner specifically identifies the portions of the cited prior art relied upon and explains why the claims would have been obvious, moreover, Appellant fails to explain how the level of ordinary skill in the art should be resolved or how such resolution would affect the outcome of this inquiry. (see Final Act 7-12). Appellant contends Varnum also fails to expressly or inherently teach that anti- IL- I a antibodies can be used to reduce the formation of new metastases. Varnum paragraph [0240] relates to anti-IL- lRlantibodies - not anti-IL-la antibodies. And like Garonne and Witte, Varnum does not describe any actual experiments that would have suggested to the skilled artisan that anti- IL- I a antibodies could actually be used to reduce the formation of new metastases. (Br. 10). We find this argument unpersuasive because a "specification need not contain a working example if the invention is otherwise disclosed in such a manner that one skilled in the art will be able to practice it without an undue amount of experimentation." In re Borkowski, 422 F.2d 904, 908 (CCPA 1970). Here, the prior art evidences that the method may be performed without undue experimentation, and no evidence is presented in rebuttal. Specifically, Witte evidences that IL- I mediates tumor metastasis (FF 11 ), and that IL- I antagonist antibodies are useful in prevention and treatment of metastatic bone disease (FF 12). Witte specifically teaches dosages for treatment (FF 13) and anti-IL-I a antibodies (FF 9-10). In addition, Varnum supports Witte by suggesting that anti-IL-la antibodies are useful in treatment of "malignancies with invasive metastatic 13 Appeal2017-010206 Application 15/013,469 potential" (FF 14) and that the "combination of an IL- I receptor antibody and RANKL inhibitors ... is useful for ... anti-tumor therapy aimed at preventing metastasis to bone" (FF 15). Thus, Witte and Varnum both suggest treatment and prevention of metastases using anti-IL- I a antibodies (FF 9--15). Moreover, Garrone provides examples showing the efficacy of the human anti-IL-la antibody in vitro (FF 4, 6-8), demonstrates the expected association with human cancers for the antibody (FF 2), and provides human dosing information (FF 5). Therefore, we agree with the Examiner that the ordinary artisan, informed by Garrone, Witte and Varnum of anti-IL- I a antibodies, including Garrone's evidence that these antibodies have biological activity (FF 4, 6), would provide the ordinary artisan with a reasonable expectation of success in reducing metastases formation. "Obviousness does not require absolute predictability of success ... all that is required is a reasonable expectation of success." In re Kubin, 561 F.3d 1351, 1360 (Fed. Cir. 2009) (citing In re O'Farrell, 853 F.2d 894, 903-904 (Fed. Cir. 1988)). Moreover, the explicit guidance to prevent metastases (FF 12, 15) using anti-IL-la antibodies (FF 2, 10) demonstrates that the "prior art gives direction as to what parameters are critical and which of many possible choices may be successful." 0 'Farrell, 853 F.2d at 894. Conclusion of Law The evidence of record supports the Examiner's conclusion that Garrone '085 and Garrone '766, along with Witte and Varnum render claims 1--4 obvious. 14 Appeal2017-010206 Application 15/013,469 SUMMARY In summary, we reverse the rejection of claims 1 and 4 under 35 U.S.C. Â§ 102(b) as anticipated by Garrone '085. We reverse the rejection of claims 1 and 4 under 35 U.S.C. Â§ 102(b) as anticipated by Garrone '7 66. We affirm the rejection of claims 1, 3, and 4 under 35 U.S.C. Â§ 102(b) as anticipated by Witte. We affirm the rejection of claims 1--4 under 35 U.S.C. Â§ 103(a) as obvious over Garrone '085, Witte, and Varnum. We affirm the rejection of claims 1--4 under 35 U.S.C. Â§ 103(a) as obvious over Garrone '766, Witte, and Varnum. No time period for taking any subsequent action in connection with this appeal may be extended under 37 C.F.R. Â§ 1.136(a). AFFIRMED 15