Ex Parte Rudy et alDownload PDFPatent Trial and Appeal BoardNov 15, 201211568506 (P.T.A.B. Nov. 15, 2012) Copy Citation 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. 11/568,506 10/30/2006 Susilo Rudy JCLA22273 5531 23900 7590 11/15/2012 J C PATENTS 4 VENTURE, SUITE 250 IRVINE, CA 92618 EXAMINER SZNAIDMAN, MARCOS L ART UNIT PAPER NUMBER 1628 MAIL DATE DELIVERY MODE 11/15/2012 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 RUDY SUSILO and EBERHARD AMTMANN __________ Appeal 2011-006472 Application 11/568,506 Technology Center 1600 __________ Before ERIC GRIMES, FRANCISCO C. PRATS, and STEPHEN WALSH, Administrative Patent Judges. PRATS, Administrative Patent Judge. DECISION ON APPEAL This appeal under 35 U.S.C. § 134 involves claims to a method of increasing the therapeutic efficacy of the cytostatic anticancer compound temozolomide. The Examiner entered rejections for indefiniteness and obviousness. We have jurisdiction under 35 U.S.C. § 6(b). We affirm. STATEMENT OF THE CASE Claims 9-13 stand rejected and appealed (Ans. 2). Claim 9, the only independent claim, illustrates the appealed subject matter and reads as follows: Appeal 2011-006472 Application 11/568,506 2 Claim 9. A method for increasing the efficacy of cytostatics, comprising administrating an effective amount of 2-methylthiazolidine-2,4-dicarboxylic acid and/or physiologically acceptable salts to a mammal in need thereof. In response to a species election requirement, Appellants elected: (a) temozolomide as the cytostatic compound having increased efficacy, and (b) small cell and non-small cell bronchial carcinoma, i.e. lung cancer, as the species of treated disorder for prosecution on the merits (see Ans. 4; see also Response to Restriction Requirement (entered April 21, 2008)). Therefore, as to the merits of the art rejection, we limit our analysis regarding the claimed process to the elected compound and disorder, and the extent to which the appealed claims read on them. See Ex parte Ohsaka, 2 USPQ2d 1460, 1461 (BPAI 1987). The following rejections are before us for review: (1) Claims 9-13, under 35 U.S.C. 112, second paragraph, as indefinite (Ans. 4); and (2) Claims 9-13, under 35 U.S.C. § 103(a) as obvious over Susilo 1 and Adonizio 2 (Ans. 4-8). As Appellants direct no argument to the Examiner’s indefiniteness rejection, we summarily affirm it. See MPEP § 1205.02 (“If a ground of 1 WO 01/60343 A2 (published August 23, 2001). In discussing the Susilo reference, the Examiner cites to Susilo’s English language counterpart publication, U.S. Patent No. 6,943,185 B2 (issued September 13, 2005). We do the same. 2 Christian S. Adonizio et al., Temozolomide in Non-Small-Cell Lung Cancer: Preliminary Results of a Phase II Trial in Previously Treated Patients, 3 CLINICAL LUNG CANCER 254-258 (2002). Appeal 2011-006472 Application 11/568,506 3 rejection stated by the examiner is not addressed in the appellant’s brief, that ground of rejection will be summarily sustained by the Board.”). OBVIOUSNESS As evidence that the claimed process would have been obvious to an ordinary artisan, the Examiner cited Susilo as teaching that the compound recited in Appellants’ claims as increasing the efficacy of cytostatics, 2-methylthiazolidine-2,4-dicarboxylic acid (2-MTDC), was useful for treating lung cancer, the elected species of treated disorder (Ans. 5). The Examiner cited Adonizio as evidence that temozolomide, the elected species of cytostatic, was also useful for treating lung cancer (id. at 6). Based on these teachings, the Examiner reasoned that, because both of the claimed agents were useful for treating the same disorder, an ordinary artisan would have been prompted to co-administer them to treat that disorder (see id. (citing In re Kerkhoven, 626 F.2d 846, 850 (CCPA 1980)). The Examiner also reasoned that a “further motivation to combine 2-MTDC and Temozolomide is the fact that according to Susilo, 2-MTDC reduces the toxicity of cytostatics (i.e. Temozolomide)” (Ans. 6). As stated in In re Oetiker, 977 F.2d 1443, 1445 (Fed. Cir. 1992): [T]he examiner bears the initial burden . . . of presenting a prima facie case of unpatentability. . . . After evidence or argument is submitted by the applicant in response, patentability is determined on the totality of the record, by a preponderance of evidence with due consideration to persuasiveness of argument. Appellants’ arguments do not persuade us that a preponderance of the evidence fails to support the Examiner’s conclusion that the claimed process would have prima facie obvious to an ordinary artisan, nor are we persuaded Appeal 2011-006472 Application 11/568,506 4 that the evidence of unexpected results advanced by Appellants is sufficient to overcome the Examiner’s prima facie case. In particular, we are not persuaded, as Appellants argue, that Susilo teaches only that 2-MTDC was useful for reducing the side effects of other cytostatic agents. While Susilo describes reducing side effects of cytostatics as “[a]nother promising application” of 2-MTDC (see Susilo, col 2, l. 58 (emphasis added)), Susilo also discloses: Animal tests proved that 2-methyl-thiazolidine-2,4- dicarboxylic acid (2-MTDC) and/or its physiologically tolerable salts can slow down or even stop the advance of cancerous diseases. These studies were conducted in several animal tumor models. Test systems used were the mouse, the rat, and the hamster. The objects of study included . . . pulmonary adenocarcinomas . . . . (Id. at col. 1, ll. 58-66.) Thus, because Susilo teaches that 2-MTDC was useful not only for ameliorating the side effects of cancer-treating cytostatic agents, but also useful in and of itself for treating cancers such as lung cancer, and because Adonizio teaches that temozolomide was also useful for treating lung cancer (see Adonizio, abstract), we agree with the Examiner that an ordinary artisan would have been prompted to co-administer 2-MTDC and temozolomide to treat lung cancer as required by Appellants’ claims. Appellants argue that the claims’ recitation, that the method is “for increasing the efficacy of cytostatics” (App. Br. 9 (claim 9)), provides a manipulative difference between the claims and the method of reducing side effects suggested by Susilo (see id. at 5-6). We are not persuaded. Appeal 2011-006472 Application 11/568,506 5 As noted above, Susilo suggests that 2-MTDC itself is useful as an anticancer therapeutic (see Susilo, col. 1, ll. 58-66). Moreover, while Appellants advance a number of ways a method of increasing the efficacy of a cytostatic might differ from a method of ameliorating the side effects of a cytostatic (see App. Br. 5-6), Appellants point to no specific evidentiary support for those differences. More importantly, Appellants’ claims do not limit the administration of the two drugs to any particular sequence or technique which has been demonstrated as being different than that suggested by the cited references. As to Appellants’ evidence of unexpected results, we acknowledge the Specification’s disclosure that, while 2-MTDC did not influence the growth of the bladder cancer cell line “EJ,” 200 µg/ml 2-MTDC nonetheless reduced the IC50 value of temozolomide against the EJ cells from 1053.36 µg/ml to 96.58 µg/ml (Spec. 15). We also acknowledge, as Appellants argue, that 1000 µg/ml of 2-MTDC decreased the IC50 value of temozolomide against EJ cells 67-fold (id. at 18). We further acknowledge the statement in the Specification that “[t]hese test data prove the unexpected increase of the efficacy of combinations of a cytostatic with 2-methylthiazolidine-2,4-dicarboxylic acid compared to the administration of a single cytostatic and the non existent or low influence on the efficacy of a cytostatic or a cytotoxic or antiangiogenic substance by N-acetylcysteine” (id. at 15). As the Examiner points out, however, “the present species of cancer under examination is lung cancer” (Ans. 13). Thus, the Examiner finds, “Appellants have not set forth any reasoning as to how these results [in a bladder cancer cell line] can be extrapolated to other cancer cell lines Appeal 2011-006472 Application 11/568,506 6 including lung cancer (species under examination) since it is well known that each type of cancer has its own etiology and pathophysiology” (id.). We acknowledge that, although “[e]vidence of secondary considerations must be reasonably commensurate with the scope of the claims[,] . . . . [t]his does not mean that an applicant is required to test every embodiment within the scope of his or her claims.” In re Kao, 639 F.3d 1057, 1068 (Fed. Cir. 2011). Here, nonetheless, Appellants point to no evidence that an ordinary artisan would have extrapolated to lung cancer, the species of disorder under examination, the increased activity against bladder cancer cells of temozolomide in the presence of 2-MTDC. Moreover, the Examiner’s undisputed finding, that the activity of a cytostatic compound against one cancer cell line cannot be extrapolated to another, is supported by the fact that 2-MTDC has essentially no activity against the EJ bladder cancer cell line, but has significant activity against the H4 neuroglioma cell line (see Spec. 15 (“In the human gliomas cells H4, 2-methylthiazolidine-2,4- dicarboxylic acid had a significant cytotoxic effect. An IC50 value of 9.66 µg/ ml was found.”)). Thus, we find that a preponderance of the evidence supports the Examiner’s position that the evidence of unexpected results advanced by Appellants is not commensurate in scope with the claimed subject matter under examination, and is therefore insufficient to rebut the Examiner’s prima facie case of obviousness. Accordingly, we affirm the Examiner’s rejection of claims 9-13 as obvious over Susilo and Adonizio. Appeal 2011-006472 Application 11/568,506 7 SUMMARY We affirm the Examiner’s rejection of claims 9-13 as indefinite. We also affirm the Examiner’s obviousness rejection of claims 9-13 over Susilo and Adonizio. 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 cdc Copy with citationCopy as parenthetical citation
