Ex Parte Leveugle

Patent Trial and Appeal BoardDec 21, 2012

10470519 (P.T.A.B. Dec. 21, 2012)

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. 10/470,519 02/04/2004 Beatrice Leveugle 2483QPI-1 8433 22442 7590 12/21/2012 Sheridan Ross PC 1560 Broadway Suite 1200 Denver, CO 80202 EXAMINER RAMACHANDRAN, UMAMAHESWARI ART UNIT PAPER NUMBER 1627 MAIL DATE DELIVERY MODE 12/21/2012 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 BEATRICE LEVEUGLE __________ Appeal 2011-011754 Application 10/470,519 Technology Center 1600 __________ Before ERIC GRIMES, FRANCISCO C. PRATS, and STEPHEN WALSH, Administrative Patent Judges. GRIMES, Administrative Patent Judge. DECISION ON APPEAL This is an appeal under 35 U.S.C. § 134 involving claims to methods of treating cancer. The Examiner has rejected the claims as obvious. We have jurisdiction under 35 U.S.C. § 6(b). We affirm but designate the affirmances as new grounds of rejection. STATEMENT OF THE CASE The Specification discloses “photodynamic therapy (PDT) and sonodynamic therapy (SDT) … for the treatment of cancer. These therapies involve systemic or topical administration of a sensitizer, followed by its Appeal 2011-011754 Application 10/470,519 2 activation by light of a specific wavelength (PDT), or activation by sound of a specific frequency (SDT).” (Spec. 2:18-22.) Claims 1, 2, 3, 5, 8, 13 and 14 are on appeal. Claim 1, the only independent claim, reads as follows: 1. A method of potentiating activity of an administered immunotherapeutic agent in cancer therapy comprising a) administering a composition comprising a hypocrellin derivative consisting of a compound selected from the group consisting of butylaminatedhypocrellin B; 2-(N,N-dimethylamino)-propylamine- hypocrellin B; ethanolaminated hypocrellin B; and 1,12-Bis[2- (acetyloxy)propyl]-2,4,6,7,9,11-hexamethoxy-3,10-perylenedione, compounds of the formulae and and wherein R1, R2, R3, R4 are OCH3 or NHCH2Ar (Ar are phenyl or pyridyl group), NHCH(CH2)n (wherein -CH(CH2) are alicyclic groups and n=3,4,5,6), said hypocrellin derivative being a sonosensitizer and/or a photosensitizer, and b) activating the hypocrellin derivative, wherein said activation is effected by light or sound or by light and sound; and Appeal 2011-011754 Application 10/470,519 3 c) separately administering the immunotherapeutic agent comprising an antibody that is not conjugated to the hypocrellin derivative of step a) after administering the hypocrellin composition of step a) and activating the hypocrellin in step b). The claims stand rejected under 35 U.S.C. § 103(a) as follows: • Claims 1, 3, 5, 8 and 13 in view of Fanslow1 and Wu;2 • Claim 2 in view of Fanslow, Wu and Iger;3 and • Claim 14 in view of Fanslow, Wu and Eccles.4 I. Issue The Examiner has rejected claims 1, 3, 5, 8 and 13 as obvious in view of Fanslow and Wu, and has rejected claim 2 as obvious in view of Fanslow, Wu, and Iger. We will consider the rejections together since Appellant has waived any argument based on Iger (Appeal Br. 14-15). The Examiner finds that Fanslow discloses treating cancer with a “CD40 binding protein in conjunction with photodynamic therapy [PDT],” where the CD40 binding protein can be an antibody to CD40 (Answer 5). The Examiner finds that Fanslow discloses that “combining PDT with … a CD40 binding protein should significantly enhance the in vivo anti-tumor immune response” (id.). The Examiner finds that Fanslow’s Example 2 1 Fanslow III et al., US 2002/0041864 A1, Apr. 11, 2002. 2 Wu et al., New potential photodynamic therapeutic anti-cancer agents: synthesis and characterization of demethoxy amino-substituted hypocrellins, 15 ANTI-CANCER DRUG DESIGN 287-293 (2000). 3 Iger, WO 98/52610, Nov. 26, 1998. 4 Eccles, Monoclonal antibodies targeting cancer: ‘magic bullets’ or just the trigger?, 3 BREAST CANCER RESEARCH 86-90 (2001). Appeal 2011-011754 Application 10/470,519 4 discloses the “administration of a photosensitizing compound followed by activation” by light and subsequent administration of a CD40 binding protein (id.). The Examiner finds that Fanslow does not teach hypocrellin compounds (id. at 6), but Wu discloses “demethoxy amino-substituted hypocrellins … [having] photodynamic therapy advantages over commonly used photofrins” (id.). The Examiner finds that Wu discloses that its “compound 3 exhibited much greater phototoxicity than the[ ] parent hypocrellins and … qualifies as a better photodynamic therapeutic agent” (id.). The Examiner concludes that it “would have been obvious to one of ordinary skill in the art … to administer hypocrellin as a photosensitizer in Fanslow’s method of treating tumors … because the claimed hypocrellin compounds are taught by Wu as photosensitizing compounds for treating cancer” (id.). Appellant contends that Fanslow’s Example 1 teaches away from the claimed invention and Fanslow’s Example 2 is a prophetic example (Appeal Br. 11-13). Appellant also argues that Wu only tested one demethoxy amino-substituted hypocrellin and that Wu “does not teach one of skill in the art that all demethoxy amino-substituted hypocrellins will demonstrate much greater phototoxicity than the parent hypocrellins A and B” (id. at 13-14). The issue presented is: Does the evidence of record support the Examiner’s conclusion that the cited references would have made obvious the method of potentiating the activity of an administered immuno- therapeutic agent in cancer therapy that is defined by claim 1? Appeal 2011-011754 Application 10/470,519 5 Findings of Fact 1. Fanslow discloses that “[p]hotodynamic therapy (PDT) is a treatment for cancer that involves the use of a photosensitizer and light” (Fanslow 1, ¶ 0002). 2. Fanslow discloses that cancerous cells “retain the photosensitizer more readily than normal tissues. Subsequent exposure of the cells to wavelength-specific light induces a photochemical reaction that causes oxidative damage to numerous cellular components and cell death.” (Id.) 3. Fanslow discloses a “method for inducing a memory cytotoxic T lymphocyte (CTL) response in a tumor-bearing subject comprising administering a therapeutically effective amount of a CD40 binding protein to said subject in combination with photodynamic therapy” (id. at 1, ¶ 0008). 4. Fanslow discloses that a “variety of CD40 binding proteins may be employed …, including, for example, an antibody that binds CD40” or CD40 ligand (id. at 1, ¶ 0011). 5. Fanslow discloses that the “particular photosensitizer employed is not crucial to the present invention.… A preferred photosensitizer employed is Photofrin®.” (Id. at 4, ¶ 0044.) 6. Fanslow discloses that “[c]ombining PDT with administration of a CD40 binding protein should significantly enhance the in vivo anti-tumor immune response” (id. at 6, ¶ 0064). 7. Fanslow’s Example 2 is a prophetic example that describes the administration of a CD40 binding protein to tumor-bearing subjects after PDT, and states that the combination “enhances anti-tumor treatment” (id. at 6, ¶ 0065). Appeal 2011-011754 Application 10/470,519 6 8. Wu discloses “potential photodynamic therapeutic anti-cancer agents” (Wu 287, title). 9. Wu discloses that hypocrellin A (HA) and hypocrellin B (HB) exhibit “several advantages over the presently used photodynamic therapeutic (PDT) agent photofrin” (id. at 287, left col.). 10. Wu discloses that “as in the case of photofrin, hypocrellins do not exhibit absorptivity at >600 nm sufficiently strong for photodynamic therapy, and this has limited their PDT applications to date” (id. at 287, left– right col.). 11. Wu discloses “demethoxy amino-substituted hypocrellin derivatives (AHDs) which demonstrate significantly enhanced red absorptivity (>600 nm) and strong active oxygen … generating properties” (id. at 287, right col.). 12. Wu’s compound 3 is shown below: Wu discloses that compound 3 is “2-butylamino demethoxy HB,” and “3 consists of two tautomers – a ketone form (3a) and an enol form (3b)” (id. at 289, right col.). 13. Wu discloses that “[c]ompound 3 exhibited much greater phototoxicity than their parent hypocrellins … which qualifies 3 as a better Appeal 2011-011754 Application 10/470,519 7 photodynamic therapeutic anti-cancer agent than the parent hypocrellins” (id. at 292, right col.). Analysis Claim 1 is directed to a method comprising administering a composition comprising one of a set of specified hypocrellin derivatives, activating the hypocrellin derivative by light or sound, and then administering an immunotherapeutic antibody. Fanslow discloses treating cancer using a combination of photodynamic therapy (PDT) and administration of a CD40 binding protein, such as an antibody that binds CD40. Fanslow discloses that a preferred photosensitizer is Photofrin® and that the combination therapy should significantly enhance the anti-tumor immune response. Wu discloses that hypocrellins A and B have advantages over photofrin in PDT but none of the three compounds exhibit sufficient absorptivity at >600 nm. Wu discloses hypocrellin derivatives with enhanced absorptivity at wavelengths >600 nm and strong active oxygen generating properties. Wu discloses that its compound 3 (2-butylamino demethoxy hypocrellin B) exhibited much greater phototoxicity than hypocrellins A and B and is therefore a better PDT agent. In view of these disclosures, it would have been obvious to one of ordinary skill in the art to modify Fanslow’s method of administering PDT followed by anti-CD40 antibody by using Wu’s compound 3 as a photosensitizer because Wu Appeal 2011-011754 Application 10/470,519 8 suggests that compound 3 would have advantages over photofrin in anti- cancer therapy.5 Appellant argues that Fanslow’s Example 1 teaches away from using an antibody because it “shows that the administration of an antibody in combination with photodynamic therapy results in no change in the effect of PDT (see, control rat [I]gG), or an elimination of the effect of PDT (anti- CD40 ligand antibody). Thus … the antibodies used therein in combination with PDT do not improve the anti-tumor immune response.” (Appeal Br. 12). This argument is not persuasive. As discussed above, Fanslow expressly suggests the use of PDT in combination with an antibody that binds and activates CD40. As Appellant acknowledges (Appeal Br. 12), the antibodies used in Fanslow’s Example 1 were a rat IgG used as a negative control, which was not expected to bind to anything, and an antibody that binds CD40 ligand, thus inhibiting activation of CD40. These antibodies are different from the anti-CD40 antibody that Fanslow suggests combining with PDT for cancer treatment. Appellant also argues that Fanslow’s Example 2 is a prophetic example (Appeal Br. 11). Appellant argues that although Fanslow “recites the steps of an anti-cancer treatment combining PDT with immunotherapy in 55 Wu’s compound 3 (2-butylamino demethoxy hypocrellin B) corresponds to the second formula recited in claim 1, where R1, R2, and R4 are OCH3 and R3 is NHCH(CH2)n where n=3. Cf. Spec. 13:1-2 (“A hypocrellin derivative of the present invention also includes 2-butylamino-2-demethoxy- hypocrellin B (2-BA-2-DMHB)”) and 9:2-3 (“2-BA-2-DMHB is where R1, R2, R3 are OCH3, and R4 is NH(CH2)3CH3”). Appeal 2011-011754 Application 10/470,519 9 Example 2, there is no indication that such combined therapy was in any way successful or even promising” (id. at 13). Appellant argues that the procedures in Fanslow’s Example 2 “are merely a wish list of experimental protocols that could be utilized.… Such wish list is certainly insufficient to support an inference that one of skill in the art would regard such therapy as useful or efficacious.” (Id.) This argument is also unpersuasive. Fanslow expressly discloses that “[c]ombining PDT with administration of a CD40 binding protein should significantly enhance the in vivo anti-tumor immune response” (FF 6) and that a CD40 binding antibody is a suitable CD40 binding protein (FF 4). “[A] presumption arises that both the claimed and unclaimed disclosures in a prior art patent are enabled.” Amgen, Inc. v. Hoechst Marion Roussel, Inc., 314 F.3d 1313, 1355 (Fed. Cir. 2003). Appellant has not provided any evidence that Fanslow does not enable providing an anti-tumor treatment using PDT therapy in combination with anti-CD40 antibodies. Nor has Appellant provided evidence or sound reasoning to show that a skilled worker would not have expected Fanslow’s treatment method to be effective, notwithstanding the fact that Fanslow did not actually carry out the treatment in vivo. See In re Kumar, 418 F.3d 1361, 1368 (Fed. Cir. 2005) (Patent applicants bear the burden of “presenting sufficient reason or authority or evidence, on the facts of the case, to show that the prior art method would not produce or would not be expected to produce the claimed subject matter.”). Appellant also argues that Wu only tested one demethoxy amino- substituted hypocrellin and “does not teach … that all demethoxy amino- Appeal 2011-011754 Application 10/470,519 10 substituted hypocrellins will demonstrate much greater phototoxicity than the parent hypocrellins A and B” (Appeal Br. 13-14). This argument is not persuasive since the Wu’s compound 3 is within the scope of claim 1 and is disclosed to have greater phototoxicity than the parent hypocrellins. Appellant argues that the Examiner erred in finding that Wu’s compound 3 is the same as the compound recited in dependent claim 8 (Appeal Br. 14), and Wu “does not teach one of skill in the art that all demethoxy amino-substituted hypocrellins will demonstrate much greater phototoxicity than the parent hypocrellins A and B” (id.). In response to Appellant’s arguments, the Examiner acknowledged that Wu’s compound 3 is not the same as the compound recited in claim 8 (Answer 12-13). Specifically, claim 8 requires that R1, R2, and R3 are OCH3 and R4 is NH(CH2)3CH3, but in Wu’s compound 3, R1, R2, and R4 are OCH3 and R3 is NH(CH2)3CH3. The Examiner concludes, however, that the compound of claim 8 would have been obvious based on the hypocrellin derivatives disclosed by Wu, because Wu “teaches butyl amino demethoxy compounds of Hyp A [HA] and Hyp B [HA] … as photodynamic therapeutic anti-cancer agents” (id. at 13). We agree with the Examiner's reasoning and conclusion set forth in the Answer (pages 13-14). That is, the compound recited in claim 8 is the same as Wu’s compound 3 except with the R3 and R4 substituents switched around, and the Examiner concludes that the compound of claim 8 would have been obvious based on Wu’s very similar compound. Appellant has provided no evidence or sound reasoning to support a contrary conclusion. Simply pointing out a difference between a claimed compound and the prior Appeal 2011-011754 Application 10/470,519 11 art is not a sufficient basis for concluding that the claimed compound would not have been obvious based on the prior art. Thus, we affirm the rejection of claims 1 and 8 as obvious in view of Fanslow and Wu. Claims 3, 5, and 13 were not argued separately and therefore fall with claim 1. 37 C.F.R. § 41.37(c)(1)(vii). We also affirm the rejection of claim 2 as obvious in view of Fanslow, Wu and Iger, since Appellant has waived any argument based on Iger (Appeal Br. 14-15). Conclusion of Law The evidence of record supports the Examiner’s conclusion that the cited references would have made obvious the claimed method of potentiating the activity of an administered immunotherapeutic agent in cancer therapy. II. Issue The Examiner has rejected claim 14 as obvious in view of Fanslow, Wu, and Eccles. Claim 14 is directed to the method of claim 1, “wherein the antibody is a tumor specific antibody” (Appeal Br. 18 (Claims Appendix)). The Examiner relies on Fanslow and Wu as discussed above (Answer 8). The Examiner finds that Eccles discusses “monoclonal antibodies approved for cancer therapy clinical trials to specifically target the cancer cells, for example, … herceptin for metastatic breast cancer” (id. at 9). The Examiner concludes that it “would have been obvious to one having ordinary skill in the art … to administer a tumor specific antibody in treating Appeal 2011-011754 Application 10/470,519 12 cancer after PDT therapy because with tumor specific antibodies, specific tumors or cancers can be effectively targeted as taught by Eccles” (id.). Appellant contends that Eccles does not disclose or suggest that “there is a known mechanism of action or biological reason to expect that the antibodies described would be effective in combination with PDT therapy” (Appeal Br. 15). The issue with respect to this rejection is: Does the evidence of record support the Examiner’s conclusion that the cited references would have made obvious the use of Eccles’ anti-tumor antibodies in the therapy method suggested by Fanslow and Wu? Additional Findings of Fact 14. Eccles discloses that Herceptin® [anti-(c-erbB-2/HER-2)] has received regulatory approval for treatment of metastatic breast cancer (Eccles 86). 15. Fanslow discloses that “the combination of a CD40 binding protein and PDT may be supplemented by the use of additional active agents” (Fanslow 5, ¶0055). 16. Fanslow discloses that its combination treatment “may be used in conjunction with other therapies appropriate for afflicted subjects, including chemotherapy, radiation therapy, and immunotherapy” (id. at 6, ¶0060). Analysis Fanslow and Wu are discussed above. Eccles discloses that Herceptin® [anti-(c-erbB-2/HER-2)] has been approved by the FDA for the treatment of metastatic breast cancer. In view of this disclosure, it would Appeal 2011-011754 Application 10/470,519 13 have been obvious to modify the PDT therapy method suggested by Fanslow and Wu (i.e., PDT therapy with a CD40 binding agent) to include treatment with the Herceptin® antibody disclosed by Eccles in the treatment for metastatic breast cancer because Fanslow expressly suggests combining its treatment method with immunotherapy. Appellant contends that “Eccles would not teach one of skill in the art that there is a known mechanism of action or biological reason to expect that the antibodies described would be effective in combination with PDT therapy” (Appeal Br. 15). This argument is not persuasive. Eccles discloses that the anti-tumor antibody Herceptin® has been approved for the treatment of metastatic breast cancer. Fanslow and Wu disclose that PDT therapy has been shown to be effective in targeting cancer cells. Even if the exact mechanism of action for anti-tumor antibodies has not been established, one of ordinary skill in the art would expect that combining two successful treatment methods would improve the effect compared to either method used alone. Appellant has not pointed to anything in Eccles to suggest that the treatment with Herceptin would interfere with Fanslow’s treatment method or vice versa. Conclusion of Law The evidence of record supports the Examiner’s conclusion that the cited references would have made obvious the use of Eccles’ anti-tumor antibodies in the therapy method suggested by Fanslow and Wu. Appeal 2011-011754 Application 10/470,519 14 SUMMARY We affirm the rejections under 35 U.S.C. § 103(a) of claims 1, 3, 5, 8, and 13 in view of Fanslow and Wu, claim 2 in view of Fanslow, Wu, and Iger, and claim 14 in view of Fanslow, Wu, and Eccles. However, since our reasoning differs from, or at least expands significantly on, the Examiner’s reasoning, we designate the affirmances as new grounds of rejection in order to provide Appellant a fair opportunity to respond. TIME PERIOD FOR RESPONSE This decision contains a new ground of rejection pursuant to 37 CFR § 41.50(b) (effective September 13, 2004, 69 Fed. Reg. 49960 (August 12, 2004), 1286 Off. Gaz. Pat. Office 21 (September 7, 2004)). 37 CFR § 41.50(b) provides “[a] new ground of rejection pursuant to this paragraph shall not be considered final for judicial review. 37 CFR § 41.50(b) also provides that the Appellant, WITHIN TWO MONTHS FROM THE DATE OF THE DECISION, must exercise one of the following two options with respect to the new ground of rejection to avoid termination of the appeal as to the rejected claims: (1) Reopen prosecution. Submit an appropriate amendment of the claims so rejected or new evidence relating to the claims so rejected, or both, and have the matter reconsidered by the examiner, in which event the proceeding will be remanded to the examiner …. (2) Request rehearing. Request that the proceeding be reheard under § 41.52 by the Board upon the same record …. AFFIRMED/37 C.F.R. § 41.50(b) Appeal 2011-011754 Application 10/470,519 15 lp