11851643 (P.T.A.B. Dec. 12, 2013)

Ex Parte Binyamin et al

Patent Trial and Appeal BoardDec 12, 2013

11851643 (P.T.A.B. Dec. 12, 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. 11/851,643 09/07/2007 Gary Binyamin 32164-708.201 9684 21971 7590 12/12/2013 WILSON, SONSINI, GOODRICH & ROSATI 650 PAGE MILL ROAD PALO ALTO, CA 94304-1050 EXAMINER WOZNICKI, JACQUELINE ART UNIT PAPER NUMBER 3774 MAIL DATE DELIVERY MODE 12/12/2013 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 GARY BINYAMIN and EITAN KONSTANTINO1 __________ Appeal 2011-013714 Application 11/851,643 Technology Center 3700 __________ Before DONALD E. ADAMS, ERIC GRIMES, and JEFFREY N. FREDMAN, Administrative Patent Judges. GRIMES, Administrative Patent Judge. DECISION ON APPEAL This is an appeal under 35 U.S.C. § 134 involving claims to a stent, which have been rejected for obviousness. We have jurisdiction under 35 U.S.C. § 6(b). We affirm. 1 Appellants identify the Real Party in Interest as TriReme Medical, Inc. (Appeal Br. 3). Appeal 2011-013714 Application 11/851,643 2 STATEMENT OF THE CASE Claims 1-5, 7, 27, and 28 are on appeal. Claim 1 is the only independent claim and reads as follows: 1. A bifurcated stent comprising: a main stent body adapted for placement in a body lumen adjacent to a branch lumen, said main stent body having an abluminal surface and a luminal surface; and a first type of an anti-proliferative or anti-thrombogenic coating over at least a portion of the luminal surface and a second type of coating to promote healing or endothelialization over at least a portion of the abluminal surface. The Examiner has rejected claims 1-5, 7, and 27 under 35 U.S.C. § 103(a) as obvious based on Grotheim2 and Llanos3 (Answer 44). The Examiner has rejected claim 28 as obvious based on Grotheim, Llanos, and Vardi5 (Answer 6). The Examiner finds that Grotheim discloses a bifurcated stent having an anti-proliferative or anti-thrombogenic coating on a portion of its surface, and a coating to promote healing or endothelialization on a portion of its surface but does not disclose the coatings being on the luminal and abluminal surfaces (id. at 4-5). The Examiner finds that “Llanos discloses it 2 Grotheim et al., US 2007/0208415 A1, Sept. 6, 2007. 3 Llanos et al., US 2005/0004663 A1, Jan. 6, 2005. 4 The Examiner did not rely on Llanos in the Office Action mailed Aug. 2, 2010. Appellants treated the rejection in the Answer as a new ground of rejection and addressed it on the merits in their Reply Brief. Appellants also argued that the Examiner entered a new ground without complying with the MPEP, but that is an issue that can be reviewed only by way of petition, not appeal. 5 Vardi et al., US 6,599,316 B2, July 29, 2003. Appeal 2011-013714 Application 11/851,643 3 is known that drug combinations are used on both surfaces to treat and effectively control cellular responses” (id. at 5). The Examiner interprets the claims as “not requir[ing] different coatings on the luminal and abluminal surfaces;” i.e., “the claims do not prevent layers of coatings . . . or one coating with both an anti-thrombogenic and an endothelialization agent present in at least two layers” (id. at 8). Appellants contend that “a plain reading of the claim language is that the coating on the abluminal surface is indeed different than the coating on the luminal surface. This is supported by the specification at paras [0014], and [0041]” (Reply Br. 8). Appellants contend that “[n]owhere does Grotheim teach or suggest different coatings on abluminal and luminal surfaces” (Appeal Br. 6) and that Llanos does not make up for that deficiency (Reply Br. 7). The issue presented is whether the claim language requires a stent having different coatings on the luminal and abluminal surfaces. Findings of Fact 1. The Specification describes “various methods for coating the struts of the stent” (Spec. 13, ¶ 42). 2. The Specification states that “the abluminal surface 42 of strut 40 may have at least two layers 46 and 48 applied thereto. . . . [B]oth layers 46 and 48 may be active and/or may contain a desired therapeutic or other agent.” (id. at 13, ¶ 43.) 3. The Specification states that “a polymeric carrier or therapeutic agent 50 may be deposited in a well 52 or other reservoir formed in a strut Appeal 2011-013714 Application 11/851,643 4 56. Optionally, . . . the well 52 may be covered with a membrane or layer 58 which controls release of therapeutic agent from the well.” (Id. at 13, ¶ 44.) 4. Grotheim discloses “a medical device such as a stent for use in a bifurcated body lumen having a main branch and a side branch” (Grotheim 1, ¶ 13). 5. Grotheim discloses that “[t]he medical device further includes a coating including at least one therapeutic agent. The coating may be selectively disposed on the medical device surface.” (Id. at 1, ¶ 16.) 6. Grotheim discloses that “therapeutic agents include, but are not limited to, anti-thrombogenic agents, anti-proliferative agents, . . . [and] vascular cell growth promoters” (id. at 4, ¶ 66). 7. Grotheim discloses that “coating layers of different coating mixtures may be applied to the stent surface” (id. at 4, ¶ 88). 8. Llanos discloses “[t]he use of a heparin barrier coating for controlling drug release in drug eluting medical devices” (Llanos 4, ¶ 36). 9. Llanos discloses that “the entire inner and outer surface of the stent 100 may be coated with drug/drug combinations in therapeutic dosage amounts” (id. at 11, ¶ 144). 10. Llanos discloses that “a heparin coating may be utilized as a barrier for controlling the elution rate of a therapeutic agent . . . from a medical device, such as a stent” (id. at 50, ¶ 467). 11. Llanos discloses that “heparin may be affixed to one or both surfaces of a stent (luminal and abluminal) as a therapeutic agent to act as both an anti-coagulant and an anti-proliferative. In this exemplary Appeal 2011-013714 Application 11/851,643 5 embodiment; however, heparin . . . also act[s] as a diffusion barrier for other therapeutic agents formulated in the coating.” (Id.) 12. Llanos discloses that “any number of medical devices with any number of therapeutic agents may be treated with a heparin coating to function as a barrier or diffusion coating to control the elution of another therapeutic agent” (id.). Principles of Law During proceedings at the USPTO, “claims are given their broadest reasonable interpretation consistent with the specification.” In re Hyatt, 211 F.3d 1367, 1372 (Fed. Cir. 2000). See also In re Zletz, 893 F.2d 319, 321 (Fed. Cir. 1989) (“[D]uring patent prosecution when claims can be amended, ambiguities should be recognized, scope and breadth of language explored, and clarification imposed.”). Analysis The claims are directed to a stent having “a first type of an anti- proliferative or anti-thrombogenic coating over at least a portion of the luminal surface and a second type of coating to promote healing or endothelialization over at least a portion of the abluminal surface” (claim 1). The claim does not require the coatings on the luminal and abluminal surfaces to be different, and does not require the luminal and abluminal surfaces to have only a single coating layer or a coating containing a single active agent. The Specification states that “methods of coating the struts of the stent” (FF 1) include providing it with “at least two layers . . . contain[ing] a Appeal 2011-013714 Application 11/851,643 6 desired therapeutic” (FF 2) or depositing a therapeutic agent “covered with a membrane or layer 58 which controls release of therapeutic agent” (FF 3). We agree with the Examiner that the broadest reasonable interpretation of the claims, in light of the Specification, includes a stent having the same coating on the luminal and abluminal surfaces; specifically, a coating having two layers, one containing an anti-proliferative or anti-thrombogenic agent and one containing an agent that promotes healing or endothelialization. Grotheim discloses a bifurcated stent that includes a coating that includes at least one therapeutic agent, such as an anti-thrombogenic agent, an anti-proliferative agent, and/or a vascular cell growth promoter (FFs 5, 6). Llanos discloses a heparin barrier coating for controlling release of a therapeutic agent from a stent (FFs 8, 9). Llano discloses that heparin is an anti-coagulant (i.e., anti-thrombogenic) and anti-proliferative agent and also acts as a diffusion barrier (FF 11) for “any number of other therapeutic agents” (FF 12). We agree with the Examiner that it would have been obvious to modify Grotheim’s stent – which Grotheim suggests coating with a vascular cell growth promoter – by adding an outer heparin coating to act as an anti-coagulant and to provide controlled release of the vascular cell growth promoter. Appellants argue that Grotheim alone does not provide a reason to make the claimed stent without the use of hindsight (App. Br. 4-7, Reply Br. 5-6) but this argument does not address what would have been obvious to a person of ordinary skill in the art based on the collective disclosures of Grotheim and Llanos. Appeal 2011-013714 Application 11/851,643 7 Appellants also argue that the claims require a different coating on the abluminal and luminal surfaces (Reply Br. 8) and that Llanos does not teach or suggest different coatings on the two surfaces of Grotheim’s stent (id. at 7). Appellants point to the Specification’s paragraphs 14 and 41 as support for their interpretation of the claim language (id. at 8). This argument is also unpersuasive because, as discussed above, the Specification’s paragraphs 42-44 support interpreting claim 1 to read on a stent having the same coating on both surfaces, where the coating includes a first layer of an anti-thrombogenic or anti-proliferative agent and a second layer of an agent that promotes healing or endothelialization. Paragraphs 14 and 41 of the Specification do not support a narrower interpretation of the claim language because those paragraphs refer to a stent having different therapeutic agents on the main body of the stent and on the crown of the stent (the part that extends into a branching blood vessel; Spec. 12, ¶ 40), not to different coatings on the luminal and abluminal surfaces. Conclusion of Law The claim language does not require a stent having different coatings on the luminal and abluminal surfaces. The rejection of claim 1 as obvious based on Grotheim and Llanos is affirmed. Claims 2-5, 7, and 27 have not been argued separately and therefore fall with claim 1. 37 C.F.R. § 41.37(c)(1)(vii). Appellants have waived any arguments directed specifically to the rejection of claim 28 as obvious based on Grotheim, Llanos, and Vardi (see App. Br. 7, Reply Br. 8). Therefore, we also affirm the rejection of claim 28. See Hyatt v. Dudas, 551 F.3d 1307, 1314 (Fed. Cir. 2008). Appeal 2011-013714 Application 11/851,643 8 SUMMARY We affirm both of the rejections on appeal. 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 lp