11958090 (P.T.A.B. Mar. 17, 2016)

Ex Parte Ruane et al

Patent Trial and Appeal BoardMar 17, 2016

11958090 (P.T.A.B. Mar. 17, 2016)

UNITED STA TES p A TENT AND TRADEMARK OFFICE APPLICATION NO. FILING DATE 111958,090 12/17/2007 48004 7590 03/17/2016 EGL/Cook - Indianapolis BRINKS GILSON & LIONE CAPITAL CENTER, SUITE 1100 201 NORTH ILLINOIS STREET INDIANAPOLIS, IN 46204-4220 FIRST NAMED INVENTOR Patrick H. Ruane 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. 12730-328 (PA-6079-RFB) 1499 EXAMINER SHARMA, YASHITA ART UNIT PAPER NUMBER 3774 MAILDATE DELIVERY MODE 03/17/2016 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 parte1 PA TRICK H. RUANE, PRISCILLA REYES, BLAYNE A. ROEDER, and AMY M. VIBBERT Appeal2012-000553 Application 11/958,090 Technology Center 3700 Before DONALD E. ADAMS, ERICA A. FRANKLIN, and SUSAN L. C. MITCHELL, Administrative Patent Judges. Opinion for the Board filed by Administrative Patent Judge MITCHELL. Opinion Concurring filed by Administrative Patent Judge ADAMS. DECISION ON APPEAL Appellants appeal under 35 U.S.C. Â§ 134 from the Examiner's decision finally rejecting claims 10-17. We have jurisdiction over the appeal under 35 U.S.C. Â§ 6(b). We reverse, 1 Appellants identify the Real Party in Interest as MED Institute, Inc. App. Br. 1. Appeal2012-000553 Application 11/958,090 STATEMENT OF THE CASE The Specification is directed to implantable medical devices adapted to release a therapeutic agent. Spec. i-f 2. Claims 10-1 7 are on appeal, and are set forth in a Claims Appendix to the Appeal Brief. App. Br. 26-27. Claim 10, the sole independent claim at issue, is illustrative and reads as follows (emphasis added): 10. A coated tubular stent graft having an abluminal surface with a surface area and a luminal surface defining a drainage lumen, the coated stent graft comprising: a graft material attached to a radially expandable support frame to form at least a portion of both the luminal surface and the abluminal surface of the coated tubular stent graft and a coating including a glycol polymer on the portion of the graft material forming the abluminal surface, the graft material containing about 5 - 100 micrograms of a taxane therapeutic agent per mm2 of the surface area of the abluminal surface and a polyurethane polymer comprising a polymer including polydimethylsiloxane and a polyurethane, the stent graft having a weight ratio of the taxane therapeutic agent to the glycol of between about 0.10 and 3.50. The Examiner has rejected the claims as follows: I. Claims 10-12, 14, 15, and 17 under 35 U.S.C. Â§ 103(a) as unpatentable over Dimatteo,2 Hunter,3 and Raze;4 2 Kristian Dimatteo and Robert C. Thistle, US 2003/0093141 Al, published May 15, 2003. 3 William L. Hunter et al., US 2004/0260318 Al, published Dec. 23, 2004. 4 Brian Raze and David Tseng, US 2006/0020329 Al, published Jan. 26, 2006. 2 Appeal2012-000553 Application 11/958,090 II. Claim 13 under 35 U.S.C. Â§ 103(a) as unpatentable over Dimatteo, Hunter, Raze, and Shakushiro; 5 and III. Claims 16 and 17 under 35 U.S.C. Â§ 103(a) as unpatentable over Dimatteo, Hunter, Raze and Udipi. 6 Ans. 4--9. I. Obviousness over Dimatteo, Hunter, and Raze Addressing independent claim 10, the Examiner asserts that Dimatteo teaches all the limitations except for "a polyurethane polymer comprising a polymer including polydimethylsiloxane and a polyurethane" and "the stent graft having a weight ratio of the taxane therapeutic agent to the glycol of between about 0.10 and 3.50." Ans. 4--5. The Examiner relies on Raze for teaching a graft "comprising a polyurethane polymer comprising a polymer including polydimethylsiloxane and polyurethane." Id. at 7. The Examiner relies on Hunter for teaching "the stent graft having a weight ratio of the taxane therapeutic agent to the glycol of between about 0.10 and 3.50," stating because Hunter teaches the polymer and drug agent ratio can be controlled by controlling the combination of the two elements (pg. 48, par. 0309), it would have been an obvious matter of design choice to modify the teaching of the Hunter reference, to have a weight ratio of the taxane therapeutic agent to the glycol of between about 0.10 and 3.50, since appellant has not disclosed that having this particular ratio[] of0.10 and 3.50 solves any stated problem or is for any particular purpose and it appears that the device would perform equally well with [ o ]ther designs. 5 Kiyoski Shakushiro et al., US 5,227,043, issued Jul. 13, 1993. 6 Kishore Udipi et al., US 6,918,929 B2, issued Jul. 19, 2005. 3 Appeal2012-000553 Application 11/958,090 Furthermore, absent a teaching as to criticality that a weight ratio of the taxane therapeutic agent to the glycol has to be between about 0.10 and 3.50, this particular arrangement is deemed to have been known by those skilled in the art since the instant specification and evidence of record fail to attribute any significance (novel or unexpected results) to a particular arrangement. Ans. 6 (citing In re Kuhle, 526 F.2d 553, 555 (CCPA 1975)). Appellants counter that the Examiner admits that the combination of references fails to teach or suggest a stent graft having the claimed weight ratio of a taxane therapeutic agent to glycol, and has failed to establish that this claimed ratio is merely a design choice. App. Br. 8, 11-15. According to Appellants, the Specification explains the ratio of taxane therapeutic agent to the glycol is important to successful loading of the stent graft device on the deployment system and successful deployment of the stent graft within the body vessel while maintaining its intended elution rate for optimal therapeutic purposes. Id. at 9-10 (citing Spec. i-f 151 ). Appellants conclude as follows: As Table 13 clearly shows, with stent grafts having the ratio of the claimed invention, large amounts of the therapeutic agent can be loaded into the device for delivery to the treatment sites without undesirable consequences to loading, deployment or elution rates as found with stent grafts having similar amounts of the therapeutic agent but lacking the claimed ratio. Id. at 10 (emphasis omitted). The Examiner responds that the claimed "weight ratio of the taxane therapeutic agent to the glycol of between about 0.10 and 3.50" would be obvious because "Hunter teaches the polymer and drug agent ratio can be controlled by controlling the combination of the two elements." Ans. 10 4 Appeal2012-000553 Application 11/958,090 (citing Hunter, 48 i-f 309). The Examiner further responds that the data contained in Table 13 of Appellants' Specification "does not disclose criticality" of the "very broad range of 'about 0.10-3.50"' as recited in claim 10. Ans. 10. In response, Appellants contend that because none of the cited references recognize that the claimed weight ratio of taxane therapeutic agent to glycol polymer is a result-effective variable, the Examiner has improperly shifted the burden of demonstrating the criticality of the claimed range. Reply Br. 8-9. Specifically, Appellants note that the Examiner has not demonstrated that Hunter, or other prior art references "recognize that the ratio of taxane therapeutic agent to glycol polymer was important in preventing damage to the stent graft to avoid possible loss of the therapeutic agent during deployment and/or alteration of the elution rate of the agent after deployment." Id. We agree with Appellants that the obviousness rejection should be reversed. As correctly expressed by Appellants, the Examiner "has not shown that the claimed weight ratios would be discovered by one of ordinary skill in the art by routine experimentation." Reply Br. 8. "[\V]hile it may ordinarily be the case that the detennination of optimum values for the parnrneters of a prior art process would be at least prima facie obvious, that conclusion depends upon what the prior art discloses with respect to those parameters." in re Sebek, 465 F.2d 904, 907 (CCPA 1972). On this recon..1, the prior art fails to disclose the claimed weight ratio of the taxane therapeutic agent to the glycol~ let alone suggest that this ratio is important to consider when one is interested in preventing physical damage to the stent 5 Appeal2012-000553 Application 11/958,090 graft, resulting in the possible loss of the therapeutic agent during deployment and/or alteration of the agent's elution rate after deployment, i.e) that the ratio of the taxane therapeutic agent to the glycol is a result-etlective variable. Thus, the Exarniner failed to establish an evidentiarv basis to ' v support a conclusion that the claimed ratio would have been obvious. See In re Antonie, 559 F.2d 618, 620 (CCPA 1977) (finding an exception to "the rule that the discovery of an optirnum value of a variable in a known process is nonna11y obvious" when "the parameter optimized was not recognized to be a result-effective variable"). Further, even if the Examiner properly shifted the burden to Appellants to demonstrate the criticality of the claimed range, the Examiner has not demonstrated on this record how Appellants' proffered data fails to do so. Specifically, the Examiner states that "[c]laim 10 requires a very broad range of 'about 0.10-3.50' and the specification does not disclose [the] criticality of such a broad range." Ans. 10. We disagree with the Examiner. Referring to Table 13, the Specification describes the successful deployment of coated stent grafts having a ratio of paclitaxel to polyethylene glycol (PEG) of 0.74--3.28, with grafts at ratios higher than about 3.6 being more difficult to deploy without damage to the graft material. Spec. i-f 151; see also Appeal Br. 9-10. In other words, as Appellants have correctly asserted, the Specification provides a weight-ratio range that encompasses the range recited by claim 10, and further explains the importance or criticality of that range to achieve successful deployment without damaging graft material. 6 Appeal2012-000553 Application 11/958,090 Therefore, for the reasons expressed in the Appeal and Reply Briefs, and as outlined above, we do not sustain the Examiner's rejection of independent claim 10 as obvious over Dimatteo, Hunter and Raze. For the same reasons, we also do not sustain the Examiner's rejection of dependent claims 11, 12, 14, 15 and 17. "[D]ependent claims are nonobvious if the independent claims from which they depend are nonobvious." In re Fritch, 972 F.2d 1260, 1266 (Fed. Cir. 1992). II. Obviousness over Dimatteo, Hunter, Raze, and Shakushiro I Udipi Addressing claim 13, the Examiner finds that Dimatteo, Hunter and Raze teach all the limitations "except for the glycol polymer is poly( ethylene glycol) with a weight average molecular weight in the range from 100 to about 10,000." Ans. 8. To address this deficiency, the Examiner relies on the Shakushiro reference. Id. Addressing claims 16 and 17, the Examiner finds that Dimatteo, Hunter and Raze teach all the limitations except for those that require the graft material to comprise 5-100 milligrams of poly( ethylene glycol), and about 1--40 micrograms poly( ethylene glycol) per mm2 of the abluminal surface area. Ans. 9. The Examiner relies on the Udipi reference to remedy this deficiency. Id. Claims 13, 16 and 17 depend either directly or ultimately from independent claim 10, and neither Shakushiro nor Udipi is relied on by the Examiner for what we find lacking in the Examiner's rejection of claim 10---a teaching for the stent graft to have a weight ratio of the taxane 7 Appeal2012-000553 Application 11/958,090 therapeutic agent to the glycol between about 0.10 and 3.50, or some suggestion that the ratio is a result-effective variable. Accordingly, for the reasons expressed above in our discussion of the rejection of independent claim 10, we also reverse the Examiner's rejections of claims 13, 16 and 17. SUMMARY We reverse the rejection of claims 10-12, 14, 15 and 17 under 35 U.S.C. Â§ 103(a) as unpatentable over Dimatteo, Hunter, and Raze. We reverse the rejection of claim 13 under 35 U.S.C. Â§ 103(a) as unpatentable over Dimatteo, Hunter, Raze, and Shakushiro. We reverse the rejection of claims 16 and 17 under 35 U.S.C. Â§ 103(a) as unpatentable over Dimatteo, Hunter, and Raze, and Udipi. APJ Initials: SLCM EAF PL Initials: kmm REVERSED 8 UNITED STATES PATENT AND TRADEMARK OFFICE BEFORE THE PATENT TRIAL AND APPEAL BOARD Ex parte PA TRICK H. RUANE, PRISCILLA REYES, BLAYNE A. ROEDER, and AMY M. VIBBERT Appeal2012-000553 Application 11/958,090 Technology Center 3700 Before DONALD E. ADAMS, ERICA A. FRANKLIN, and SUSAN L. C. MITCHELL, Administrative Patent Judges. ADAMS, Administrative Patent Judge, concurring. DECISION ON APPEAL 7 This appeal under 35 U.S.C. Â§ 134(a) involves claims 10-17 (see App. Br. 3).8 Examiner entered rejections under 35 U.S.C. Â§ 103(a). This Panel has jurisdiction over the appeal under 35 U.S.C. Â§ 6(b ). 7 Appellants identify the Real Party in Interest as "MED Institute, Inc." (App. Br. 1.) 8 Claims 1-9 and 18-20 stand withdrawn from consideration (App. Br. 3). Appeal2012-000553 Application 11/958,090 STATEMENT OF THE CASE Appellants' "invention relates to medical devices for implantation in a body vessel. More particularly, ... to implantable medical devices adapted to release a therapeutic agent" (Spec. i-f 2). Claim 10 is representative and reproduced in the Claims Appendix of Appellants' Brief. Claims 10-12, 14, 15, and 17 under 35 U.S.C. Â§ 103(a) as unpatentable over Dimatteo,9 Hunter, 10 and Raze. 11 Claim 13 under 35 U.S.C. Â§ 103(a) as unpatentable over Dimatteo, Hunter, Raze, and Shakushiro. 12 Claims 16 and 17 under 35 U.S.C. Â§ 103(a) as unpatentable over Dimatteo, Hunter, Raze and Udipi. 13 ISSUE Does the preponderance of evidence relied upon by Examiner support a conclusion of obviousness? FACTUAL FINDINGS (FF) FF 1. Examiner finds that Dimatteo fails to disclose, inter alia, a coated tubular stent graft, but fails to suggest, inter alia, "a weight ratio of [] taxane therapeutic agent to[] glycol of between about 0.10 and 3.50" (see Ans. 4-- 5). 9 Kristian Dimatteo and Robert C. Thistle, US 2003/0093141 Al, published May 15, 2003. 10 William L. Hunter et al., US 2004/0260318 Al, published Dec. 23, 2004. 11 Brian Raze and David Tseng, US 2006/0020329 Al, published Jan. 26, 2006. 12 Kiyoaki Shakushiro et al., US 5,227,043, issued July 13, 1993. 13 Kishore Udipi et al., US 6,918,929 B2, issued July 19, 2005. 2 Appeal2012-000553 Application 11/958,090 FF 2. Hunter discloses the incorporation of "an anti-scarring agent (e.g., paclitaxel) ... into a carrier[, or stent graft coating,] that includes a polyurethane" (see Hunter i-f 313; Ans. 5). FF 3. Hunter discloses the application of the taxane paclitaxel to a "device surface at a dose of about 0.25 Âµg/mm2 to about 5 Âµg/mm2" (Hunter i-f 385; see generally Ans. 5---6 and 10). FF 4. Hunter discloses that active agents can be imbibed into a surface hybrid polymer layer, or incorporated directly into the hybrid polymer coating solutions. Imbibing drugs into surface polymer layers is an efficient method for evaluating polymer-drug performance in the laboratory, but for commercial production it may be preferred for the polymer and drug to be premixed in the casting mixture. Greater efficacy can be achieved by combining the two elements in the coating mixtures in order to control the ratio of active agent to polymer in the coatings. Such ratios are important parameters to the final properties of the medicated layers, i.e., they allow for better control of active agent concentration and duration of pharmacological activity. (Hunter i-f 309; see Ans. 6 and 10.) FF 5. Examiner finds that Appellants' Specification "disclose[s] the ratios [of] ... 'about 1.34 to 3.28,' and, '0.74-3.28"' and "the criticality of these ranges and the advantages and purposes of these ranges when loading the stent graft with [a] therapeutic agent to prevent undesirable consequences to loading, deployment or elution rates" (Ans. 10 and 12; see Spec. i-f 151). FF 6. Examiner finds that the combination of Dimatteo and Hunter fails to suggest a "graft comprising a polyurethane polymer comprising a polymer including polydimethylsiloxane and a polyurethane" and relies on Raze to make up for this deficiency in the combination of Dimatteo and Hunter (Ans. 7). 3 Appeal2012-000553 Application 11/958,090 FF 7. Examiner finds that the combination of Dimatteo, Hunter, and Raze fails to suggest a "glycol polymer [that] is poly( ethylene glycol) with a weight average molecular weight in the range from 100 to about 10,000" and relies on Shakushiro to make up for this deficiency in the combination of Dimatteo, Hunter, and Raze (Ans. 8 and 13). FF 8. Examiner finds that the combination of Dimatteo, Hunter, and Raze fails to suggest a "graft material [that] comprises a total of 5 - 100 milligrams of[] poly( ethylene glycol) and about 1-40 micrograms poly( ethylene glycol) per mm2 of the abluminal surface area" (Ans. 8-9). FF 9. Udipi discloses [a] drug-polymer coated stent, comprising: a stent framework; and a drug-polymer coating disposed on the stent framework, wherein the drug-poymer coating comprises a styrenic block copolymer grafted with polyethylene glycol; and a bioactive drug dispersed within the drug-polymer coating, wherein the grafted styrenic block copolymer comprises a chain length of the styrenic block copolymer, a chain length of the polyethylene glycol grafts, and a polyethylene glycol based on a predetermined elution rate of the bioactive drug. (Udipi 12:37--44 and 47-51 (claim 30); cf Ans. 9.) FF 10. Udipi discloses that a "polymeric coating includes between 0.5 percent and 50 percent of the bioactive agent of drug by weight" (Udipi 5:26-29; see Ans. 9; see also Ans. 13 ("Udipi is[] relied on for the teaching of the total weight ratio of about 0.1-1.50 since Udipi discloses polyethylene glycol graft including 0.50-50 % or 0.5 total drug by weight or total paclitaxel to total polyethylene glycol weight ratio")). 4 Appeal2012-000553 Application 11/958,090 ANALYSIS The rejection over the combination of Dimatteo, Hunter, and Raze: Based on the combination of Dimatteo, Hunter, and Raze, Examiner concludes that, at the time Appellants' invention was made, it would have been prima facie obvious to modify the teaching of the Hunter reference, to have a weight ratio of the taxane therapeutic agent to the glycol of between about 0.10 and 3.50, since appellant has not disclosed that ... th[ e] particular ratio[] of 0.10 and 3 .50 solves any stated problem or is for any particular purpose and it appears that the device would perform equally well with either [a ratio of0.10 or 3.50]. (Ans. 6.) I am not persuaded. "[R]ejections on obviousness grounds cannot be sustained by mere conclusory statements; instead, there must be some articulated reasoning with some rational underpinning to support the legal conclusion of obviousness." In re Kahn, 441 F.3d 977, 988 (Fed. Cir. 2006). On this record, Examiner recognizes that Appellants' disclosure establishes that the weight ratio of taxane therapeutic agent to glycol on a coated tubular stent provides advantages and "prevents undesirable consequences to loading, deployment or elution rates" (FF 5; see App. Br. 9-10; Reply Br. 5---6). Therefore, I am not persuaded by Examiner's unsupported conclusion that even though the combination of Dimatteo, Hunter, and Raze fails to suggest a "stent graft having a weight ratio of the taxane therapeutic agent to the glycol of between about 0.10 and 3.50," such a range would have been obvious to a person of ordinary skill in this art because Appellants fail to establish that the ratio of polymer-to-drug is critical, or otherwise important (Ans. 6 and 10-11; see App. Br. 10 (the combination of Dimatteo, Hunter, and Raze fails to "suggest a stent graft 5 Appeal2012-000553 Application 11/958,090 having a weight ratio of a taxane therapeutic agent to glycol of between about 0.1 and 3.50")). In addition, I am not persuaded by Examiner's attempt to bridge the evidentiary void on this record by relying on Hunter's generic disclosure that polymer-to-drug "ratios are important parameters to the final properties of the medicated layers, i.e., they allow for better control of active agent concentration and duration of pharmacological activity" (FF 4; see Reply Br. 3). In this regard, while it may be true that "it is not inventive to discover the optimum or workable ranges by routing experimentation" when "the general conditions of a claim are disclosed in the prior art," on this record, Examiner failed to establish an evidentiary basis to support a conclusion that the general conditions (i.e. ratios) were disclosed in the art relied upon by Examiner (see generally App. Br. 14--15; Reply Br. 3--4 and 8-9). See In re Aller, 220 F.2d 454, 456 (CCPA 1955); cf In re Sebek, 465 F.2d 904, 907 (CCP A 1972). Therefore, I am not persuaded by Examiner's unsupported assertion that "[a]ny ratio chosen in Hunter would be 'about' 0.1-3.5 since the about limitation allows for ratios outside of the range to be selected" (Ans. 11 ). In my opinion, the term "about" does not, on this record, open the claimed range so far as to read on any polymer-to-drug ratio that may fall within Hunter's broad disclosure (see FF 4). Lastly, Examiner recognizes that the ratio of polymer-to-drug on the stent graft is important (FF 5). Therefore, I am not persuaded by Examiner's assertion that the combination of Dimatteo, Hunter, and Raze suggests a stent graft as required by Appellants' claimed invention, because Appellants' fail to specifically disclose the importance of a polymer-to-drug ratio of0.10 and 3.50 (see Ans. 6; see also id. at 10-11). 6 Appeal2012-000553 Application 11/958,090 The rejection over the combination ofDimatteo, Hunter, Raze, and Shakushiro: Based on the combination of Dimatteo, Hunter, Raze, and Shakushiro, Examiner concludes that, at the time Appellants' invention was made, it would have been prima facie obvious "to modify the graft" suggested by the combination of Dimatteo, Hunter, and Raze "to include poly( ethylene glycol) with a weight average molecular weight in the range from 100 to about 10,000, for the purpose of a polymer with sufficient molecular weight to allow for proper delivery of therapeutic agents" (Ans. 8). I am not persuaded. Examiner failed to establish an evidentiary basis on this record to support a conclusion that Shakushiro makes up for the foregoing deficiency in the combination of Dimatteo, Hunter, and Raze (FF 7; App. Br. 19). The rejection over the combination of Dimatteo, Hunter, Raze, and Udipi: Based on the combination of Dimatteo, Hunter, Raze, and Udipi, Examiner concludes that, at the time Appellants' invention was made, it would have been prima facie obvious to modify the graft suggested by the combination of Dimatteo, Hunter, and Raze "to include a total of 5 - 100 milligrams of the poly( ethylene glycol) and about 5 - 100 micrograms poly( ethylene glycol)[, or alternatively about 1 - 40 micrograms poly( ethylene glycol),] per mm2 of the abluminal surface area, for the purpose of providing sufficient polymer to allow for proper elution of the drug" (Ans. 9). Examiner fails, however, to identify an evidentiary basis on this record to support Examiner's conclusion (see FF 1-6 and 8-10; see App. Br. 20-21 ). 7 Appeal2012-000553 Application 11/958,090 CONCLUSION OF LAW The preponderance of evidence relied upon by Examiner fails to support a conclusion of obviousness. Therefore, I agree that the rejections of record should be reversed. REVERSED 8