11125297 (B.P.A.I. Sep. 29, 2010)

Ex Parte LI et al

Board of Patent Appeals and InterferencesSep 29, 2010

11125297 (B.P.A.I. Sep. 29, 2010)

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. 11/125,297 05/09/2005 Jamie Li 04-0074US1 9843 27774 7590 09/29/2010 MAYER & WILLIAMS PC 251 NORTH AVENUE WEST 2ND FLOOR WESTFIELD, NJ 07090 EXAMINER FRAZIER, BARBARA S ART UNIT PAPER NUMBER 1611 MAIL DATE DELIVERY MODE 09/29/2010 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 BOARD OF PATENT APPEALS AND INTERFERENCES __________ Ex parte JAMIE LI and MICHAEL MADDEN __________ Appeal 2010-007219 Application 11/125,297 Technology Center 1600 __________ Before CAROL A. SPIEGEL, TONI R. SCHEINER, and DONALD E. ADAMS, Administrative Patent Judges. SCHEINER, Administrative Patent Judge. DECISION ON APPEAL1 This is an appeal under 35 U.S.C. § 134 involving claims to an injectable bulking composition. The claims have been rejected as obvious. We have jurisdiction under 35 U.S.C. § 6(b). 1 The two-month time period for filing an appeal or commencing a civil action, as recited in 37 C.F.R. § 1.304, or for filing a request for rehearing, as recited in 37 C.F.R. § 41.52, begins to run from the “MAIL DATE” (paper delivery mode) or the “NOTIFICATION DATE” (electronic delivery mode) shown on the PTOL-90A cover letter attached to this decision. Appeal 2010-007219 Application 11/125,297 2 STATEMENT OF THE CASE “The present invention relates to injectable bulking compositions for medical and cosmetic applications” (Spec. ¶ 1), for example, “the treatment [of] urinary incontinence . . . and aesthetic shaping (e.g., treatment of skin contour deficiencies)” (id. at ¶ 14). Claims 1-3, 5, 8-11, and 16-20 are pending and on appeal.2 Claims 1 and 20 are representative: 1. An injectable bulking composition comprising: (a) fibers that are configured to prevent migration of the fibers to locations in the body remote from the injection site, and (b) a carrier in an amount effective to render the composition injectable. 20. The injectable bulking composition of claim 1, wherein said fibers have surface features that stimulate host tissue response so as to prevent migration. The Examiner rejected claims 1-3, 5, 8-11, and 16-19 under 35 U.S.C. § 103(a) as unpatentable over Bucay-Couto.3 The Examiner also rejected claims 1 and 20 under 35 U.S.C. § 103(a) as unpatentable over Hunter.4 We reverse. 2 Claims 4, 6, 7, 12-15, 21, and 22 are also pending, but have been withdrawn from consideration (App. Br. 2). 3 Patent Application US 2005/0064008 A1 of Weenna Bucay-Couto et al., published March 24, 2005. 4 U.S. Patent 7,166,570 B2, issued January 23, 2007 to William L. Hunter et al. Appeal 2010-007219 Application 11/125,297 3 FINDINGS OF FACT The Invention 1. All of the claims on appeal are directed to bulking compositions comprising (a) fibers, and (b) a carrier in an amount effective to render the composition injectable. 2. A bulking composition is used to add volume (i.e., bulk) to an area of a subject’s body in need of augmentation (Spec. ¶¶ 1-5). 3. According to the Specification, “[a]s used herein, a ‘fiber’ is an elongated particle having a length that is at least 10 times longer than the greatest width of the particle . . . For instance, in the case of a cylindrical fiber, the length is at least 10 times the diameter” (Spec. ¶ 15). 4. The Specification teaches that “[t]he carrier typically includes one or more liquid species, for example, water, one or more liquid organic species (e.g., glycerin or other alcohols), or a mixture of water and one or more liquid organic species” (Spec. ¶ 24). 5. The Specification also teaches that “surface characteristics that stimulate host tissue response to lock the fibers in position include surface features, such as roughness and microscopic patterns, as well as coatings of therapeutic agents” (Spec. ¶ 23). Bucay-Couto 6. Bucay-Couto discloses an injectable solid or semi-solid dosage form “for chemoablation of tissue, such as prostate tissue.” The dosage forms comprise, as integral components, a biodisintegrable binder (e.g., a polymer) and a chemical ablation agent (e.g., a salt), wherein the ablation agent causes “necrosis (death) or shrinkage of nearby tissue upon injection or insertion of the formulation into the tissue” (Bucay-Couto ¶¶ 1, 6, 14, 15). Appeal 2010-007219 Application 11/125,297 4 7. Bucay-Couto’s biodisintegrable binder is one that, “once injected or inserted into tissue such as the prostate, undergoes dissolution, degradation, resorption and/or other disintegration processes . . . typically [undergoing] . . . a 50-100% reduction in weight after residing in the tissue for a period of 4 days” (Bucay-Couto ¶ 21). 8. According to Bucay-Couto, the solid or semi-solid dosage forms “result . . . in improved dosage retention in the tissue (e.g., there is little to no back-leakage into the injection tract), thereby improving delivery efficiency of the ablation agents and/or minimizing . . . nonspecific tissue damage” (Bucay-Couto ¶ 14). 9. Bucay-Couto’s dosage forms are made, e.g., by dissolving a polymer (i.e., the biodisintegrable binder) in a saturated salt solution (i.e., the ablation agent), and extruding the resultant paste through a needle into ethanol to form a rod/filament which is dried and cut to a desired length (Bucay-Couto Example 1, ¶ 53). 10. Bucay-Couto teaches: Because they are solid or semisolid in consistency, the dosage forms . . . can be provided in an essentially unlimited variety of shapes (e.g., spheres, cylinders, irregular shapes including beads of various shapes) and sizes, ranging from microparticles to pellets . . . As a more specific example, cylindrical pellets can be provided, which have an outside diameter ranging from 1 to 3 mm and a length ranging from 3 to 10 mm. (Bucay-Couto ¶ 36.) Appeal 2010-007219 Application 11/125,297 5 Hunter 11. Hunter discloses a “long-lasting and biocompatible approach for anchoring implantable medical devices into or onto biological tissue” (Hunter, col. 2, ll. 57-58). 12. Hunter provides “drug-coated or drug-impregnated implants and medical devices . . . which induce adhesion or fibrosis in the surrounding tissue, or facilitate ‘anchoring’ of the device/implant in situ” (Hunter, col. 2, l. 66 to col. 3, l. 2). 13. The implants and devices are coated, impregnated, or in contact with “a fibrosis-inducing agent or a composition comprising a fibrosis- inducing agent” (Hunter, col. 3, ll. 43-44). Exemplary fibrosis-inducing agents include . . . talcum powder, metallic beryllium and oxides thereof, copper, silk, silica, crystalline silicates, talc, quartz dust, and ethanol; . . . fibronectin, collagen, fibrin, or fibrinogen; . . . polylysine, poly(ethylene-co-vinylacetate), chitosan, N-carboxybutyl- chitosan, and RGD proteins; vinyl chloride . . . cyanoacrylates and crosslinked poly(ethylene glycol)-methylated collagen; . . . TGFβ, PDGF, VEGF, bFGF, TNFα, NGF, GM-CSF, IGF-a, IL- 1, IL-8, IL-6, . . . CTGF; BMP . . . and bleomycin or an analogue or derivative thereof. (Id. at 4, ll. 48-63.) 14. Hunter discloses that the “the agent may be present in a composition along with a polymer,” which may be biodegradable or not (Hunter col. 4, ll. 35-39), or with a “bulking agent” or a sealant” (id. at 4, ll. 44, 47). 15. Hunter teaches that the silk “may be in any suitable form that allows the silk to be joined with the medical implant, e.g., the silk may be in thread or powder” form (Hunter, col. 9, ll. 16-17, 65-68). Appeal 2010-007219 Application 11/125,297 6 16. Hunter also describes therapeutic methods involving injecting “a composition comprising a fibrosis-inducing agent” into a vein, an artery, a fallopian tube, a damaged joint, an intervertebral disc space, etc. (Hunter, col. 5, ll. 16-60). OBVIOUSNESS Obviousness over Bucay-Couto Claims 1-3, 5, 8-11, and 16-19 stand rejected as unpatentable over Bucay-Couto. The Examiner finds that Bucay-Couto discloses “solid or semi-solid therapeutic formulations comprising a biodisintegrable binder and an ablation agent which is injectable, and whereby retention at the site of injection . . . is improved, thereby improving delivery efficiency” (Ans. 4). According to the Examiner, “[t]he carrier may be a liquid such as a sodium chloride solution . . . or the biodisintegrable binder, such as cellulose, may also act as the carrier” (id.). The Examiner acknowledges that Bucay-Couto doesn’t “specifically teach that the biodisintegrable polymers are ‘fibers’ according to Applicant’s definition in the specification” (Ans. 4), but concludes that “one skilled in the art would be motivated to select cylindrical pellets having dimensions according to Applicant’s definition of ‘fiber’ . . . by routine experimentation, in order to optimize the retention at the site of injection to improve delivery efficiency, as taught by Bucay-Couto” (id. at 5), especially as “the biodisintegrable polymers of Bucay-Couto et al. ‘can be provided in an essentially unlimited variety of shapes’” (id.). Appeal 2010-007219 Application 11/125,297 7 Appellants contend that “the ‘injectable bulking composition’ of the claim preamble does not merely state a purpose or an intended use of the invention, but rather, discloses a fundamental characteristic of the claimed invention that is properly construed as a limitation of the claim” (Reply Br. 4). Appellants contend “[t]here is simply no suggestion or motivation, either in the Bucay-Couto reference itself or in the knowledge generally available to one of ordinary skill in the art” (App. Br. 5 (emphasis omitted), “to take the tissue-ablating formulations of Bucay-Couto et al., which very purpose is to ‘result[ ] in necrosis (death) and shrinkage of nearby tissue upon injection . . . and modify such formulations to create a bulking composition that, instead of killing or shrinking nearby tissue, is an ‘augmentative material’” (id. at 5-6). Appellants further contend that “a ‘fiber’ would not be recognized by one of ordinary skill in the art as a type of ‘dosage form’” (App. Br. 7), thus, “one of ordinary skill in the art would not find that the variety of dosage forms described in Bucay-Couto et al., ‘spheres, cylinders, [beads of] irregular shapes . . . and sizes, ranging from microparticles to pellets’” would suggest fibers (id.). Nevertheless, the Examiner asserts that Bucay-Couto’s dosage forms are “capable of use as bulking compositions” (Ans. 8) because they are “retained at the site of injection or insertion . . . [and] last[ ] for at least several days, . . . [and] provide[ ] an increased mass or ‘bulk’ at the site of injection” (id. at 9). As the Examiner sees it, “the question is not one of modifying the formulation of Bucay-Couto . . . , but rather of selecting a shape of ‘fiber’, as defined by Appellants, from what is already disclosed by Bucay-Couto” (id. at 10). Appeal 2010-007219 Application 11/125,297 8 Given these conflicting positions, the principle issue raised by this rejection is whether the Examiner’s interpretation of Bucay-Couto’s chemoablation dosage formulation as a “bulking composition” is reasonable in the first place, given the evidence of record. On this basic point, Appellants have the better position. Bucay- Couto’s chemoablative dosage form contains an ablative agent as an integral component, the express purpose of which is to shrink tissue, not to augment it. Even if the dosage form is retained at the injection site for a period of days, there is nothing to suggest that it adds bulk to the tissue because the tissue around it is being ablated. Moreover, the shapes, e.g., cylinders, disclosed by Bucay-Couto refer to the overall shape of the dosage form, which is an integral mixture of a biodisintegrable polymer and an ablative agent (e.g., Example 1, wherein the polymer is dissolved in a saturated salt solution) (FF9). Even if the ablative agent is considered to be the “carrier” required by the claims on appeal, there’s no suggestion in the reference that the biodisintegrable polymer itself, which is blended with the carrier in an intimate mixture, is in the form of a fiber, nor has the Examiner explained why it would have been obvious to modify the shape of the polymer itself within the solid or semi-solid dosage form. On this record, we are constrained to reverse the rejection of claims 1-3, 5, 8-11, and 16-19 as unpatentable over Bucay-Couto. Appeal 2010-007219 Application 11/125,297 9 Obviousness over Hunter Claims 1 and 20 stand rejected as unpatentable over Hunter. Claim 20 depends from claim 1 and requires that the “fibers have surface features that stimulate host tissue response so as to prevent . . . migration” of the fibers. The Examiner finds that Hunter discloses “a composition comprising a fibrosis-inducing agent and a bulking agent” (Ans. 7); and that the “fibrosis-inducing agent may be growth factors” (id.); that “the therapeutic agent may [be] formulated with a polymeric carrier” (id.); and that “[t]he compositions may be injected” (id.). The Examiner also notes that Hunter teaches that “fibrosis-inducing agents . . . such as silk . . . may be in the form of strands and/or threads” (id.). The Examiner acknowledges that Hunter doesn’t “specifically teach that the bulking agent and/or growth factors are ‘fibers’” (Ans. 7). However, the Examiner concludes that “it would have been obvious . . . to form an injectable bulking composition comprising fibers and a carrier, thus arriving at the claimed invention” (Ans. 7-8), “in order to optimize the promotion of fibrosis” (id. at 8), because Hunter “fairly teach[es] and suggest[s] other fibrosis-inducing agents in the form of strands and/or threads, such as silk” and Hunter’s compositions are “injectable and capable of use as bulking compositions” (id.). Appellants contend that Hunter “teaches joining or otherwise attaching raw silk threads to the surface of a medical implant in order to promote[ ] adhesion between the implant and tissue” (App. Br. 9), and “does not utilize fibers within an injectable bulking composition as required by the present invention” (id.). Appellants further contend there is “no suggestion or motivation, either in the Hunter et al. reference itself or in the knowledge Appeal 2010-007219 Application 11/125,297 10 generally available to one of ordinary skill in the art, to modify the reference or to combine reference teachings” (id. at 8 (emphases omitted)). Given these conflicting positions, the issue raised by this rejection is whether the Examiner has established that one of ordinary skill in the art would have had a reason to include a fibrous fibrosis-inducing agent in an injectable composition, given Hunter’s disclosure. Again, Appellants have the better position. The Examiner has drawn from disparate embodiments to assemble the components required by the claims, without a reasoned explanation as to why one of ordinary skill in the art would have combined those particular elements. It is true that Hunter teaches that a composition comprising a fibrosis-inducing agent can be injected into veins, etc., and also teaches that silk fibers are fibrosis-inducing agents. But the Examiner has not explained why, out of the fifty or so predominantly particulate fibrosis-inducing agents listed (FF13), one would have selected silk, possibly the only fiber listed, to inject into a vein, when Hunter specifically discusses silk fibers only as an attachment or coating for an implanted device (FF15) (which is what Hunter is primarily directed to, in any case). On this record, we are constrained to reverse the rejection of claims 1 and 20 as unpatentable over Hunter. Appeal 2010-007219 Application 11/125,297 11 SUMMARY The rejection of claims 1-3, 5, 8-11, and 16-19 under 35 U.S.C. § 103(a) as unpatentable over Bucay-Couto is reversed. The rejection of claims 1 and 20 under 35 U.S.C. § 103(a) as unpatentable over Hunter is reversed. REVERSED alw MAYER & WILLIAMS PC 251 NORTH AVENUE WEST 2ND FLOOR WESTFIELD, NJ 07090