Ex Parte Cantor et al

Patent Trial and Appeal BoardApr 29, 2016

12820280 (P.T.A.B. Apr. 29, 2016)

UNITED STA TES p A TENT AND TRADEMARK OFFICE APPLICATION NO. FILING DATE 12/820,280 06/22/2010 32692 7590 05/03/2016 3M INNOVATIVE PROPERTIES COMPANY PO BOX 33427 ST. PAUL, MN 55133-3427 FIRST NAMED INVENTOR Adam S. Cantor 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. 56032US040 1886 EXAMINER GHALI, ISIS AD ART UNIT PAPER NUMBER 1611 NOTIFICATION DATE DELIVERY MODE 05/03/2016 ELECTRONIC 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. Notice of the Office communication was sent electronically on above-indicated "Notification Date" to the following e-mail address( es): LegalUSDocketing@mmm.com PTOL-90A (Rev. 04/07) UNITED STATES PATENT AND TRADEMARK OFFICE BEFORE THE PATENT TRIAL AND APPEAL BOARD Ex parte ADAM S. CANTOR, TERRANCE W. OCHELTREE, and CYNTHIA A. ROBLES 1 Appeal2013-002877 Application 12/820,280 Technology Center 1600 Before TONI R. SCHEINER, LORA M. GREEN, and ULRIKE W. JENKS, Administrative Patent Judges. JENKS, Administrative Patent Judge. DECISION ON APPEAL This is an appeal under 35 U.S.C. Â§ 134 involving claims directed to a transdermal fentanyl drug delivery device. The Examiner rejects the claims as obvious. We have jurisdiction under 35 U.S.C. Â§ 6(b). We AFFIRM. 1 According to Appellants, the Real Party in Interest is are 3M Company and 3M Innovative Properties Company. (Br. 1.) Appeal2013-002877 Application 12/820,280 STATEMENT OF THE CASE According to the Specification, Oral absorption [of fentanyl] is low presumably due to a high hepatic clearance by first-pass metabolism .... Transdermal administration of fentanyl can overcome the drawbacks of frequent dosing needed with the aforementioned route[] of administration ... [because it can] avoid the peaks and valleys obtained with pulsatile delivery. (Spec. 2: 7-13.) Additionally, the Specification explains that "[t]he device should be designed to make it difficult to accidentally deliver higher dosages than the intended amount (i.e., avoid dose dumping)." (Spec. 2: 29-30.) Claims 1-10 are on appeal, and can be found in the Claims Appendix of the Appeal Brief. Claim 1 is representative of the claims on appeal, and reads as follows: 1. A transdermal drug delivery composition consisting of: (a) a copolymer comprising the reaction product of: (i) one or more A monomers selected from the group consisting of alkyl acrylates containing 4 to 12 carbon atoms in the alkyl group and alkyl methacrylates containing 4 to 12 carbon atoms in the alkyl group; and (ii) one or more ethylenically unsaturated B monomers copolymerizable with the A monomer; (b) about 8% to about 30% by weight fentanyl based on the total weight of the composition; and, optionally, ( c) a component selected from the group consisting of delivery enhancing adjuvants, tackifiers, plasticizers, and combinations thereof, wherein the composition is free of undissolved fentanyl. Claim 10, the only other independent claim lists a specific selection for monomers A and B. 2 Appeal2013-002877 Application 12/820,280 Appellants request review of the Examiner's rejection2 of claims 1-10 over Garbe3 in view of Payne.4 As Appellants do not argue the claims separately, we focus our analysis on claim 1, and claims 2-10 stand or fall with that claim. 37 C.F.R. Â§ 41.37 (c)(l)(iv). The Examiner finds that "Garbe teaches a transdermal drug delivery device comprising a backing and a matrix comprising a copolymer, a softener and a drug. . . . Example on page 19 [of Garbe] teaches copolymer comprising 55% isooctyl acrylate, 40% hydroxyethyl acrylate and 5% polymethylmethacrylate, as claimed." (Final Act. 7; Ans. 5.) The Examiner recognizes that "Garbe teaches the claimed copolymer and teaches 0.01 to about 30 percent by weight of active agent, and suggested fentanyl, however, the reference does not exemplify fentanyl." (Ans. 6.) The Examiner relies on Payne solely for "teaching and showing desirability to deliver fentanyl transdermally, versus other routes." (Id. at 14.) The Examiner concludes that "[a]bsent any evidence to the contrary, and based 2 In the Final Action mailed April 27, 2012 the Examiner also rejected claims 1-10 on the ground of non-statutory obviousness-type double patenting. The U.S. Patent and Trademark Office mailed a notice of abandonment on November 23, 2012, for U.S. Application No. 09/965,640, the application upon which this provisional nonstatutory obviousness-type double patenting rejection is based. As the application that forms the basis of this rejection has been abandoned, the contentions presented by Appellants and the Examiner regarding this rejection are moot. Accordingly, we dismiss the appeal with respect to this rejection. 3 Garbe et al., WO 96/08229, published Mar. 21, 1996. 4 Payne et al., Quality of life and cancer pain: satisfaction and side effects with transdermalfentanyl versus oral morphine, 16 J. Clin. Oncol. 1588-93 (1998) (Abstract only). 3 Appeal2013-002877 Application 12/820,280 upon the teachings of the prior art, there would have been a reasonable expectation of success in practicing the instantly claimed invention" based on the teachings of Garbe." (Id. at 7-8.) The issue is: Does the preponderance of evidence of record support the Examiner's conclusion that the combination of references would have suggested formulating fentanyl into the transdermal delivery system of Garbe? Findings of Fact We adopt the Examiner's findings and analysis concerning the scope and content of the prior art. The following facts are repeated for reference convemence. FF 1. Garbe teaches a transdermal drug delivery device, comprising: ( 1) a backing; (2) a matrix adhered to one side of the backing and comprising (a) a copolymer comprising (i) one or more A monomers selected from the group consisting of alkyl acrylates containing 4 to 10 carbon atoms in the alkyl group and alkyl methacrylates containing 4 to 10 carbon atoms in the alkyl group; and (ii) optionally one or more ethylenically unsaturated B monomers copolymerizable with the A monomer; and (iii) a macromonomer, preferably a substantially linear macromonomer, copolymerizable with the A and B monomers defined above and having a molecular weight in the range 500-500,000; (b) a softener dissolved in the copolymer; and, ( c) if the softener is not therapeutically effective, a therapeutically effective amount of a drug. (Garbe 2: 5-19.) 4 Appeal2013-002877 Application 12/820,280 FF2. Garbe teaches the preparation containing isooctyl acrylate, hydroxyethyl acrylate, and polymethylmethacrylate macromonomer (Garbe 19: 1-19; see Ans. 5 (Garbe teaches "copolymer comprising 55% isooctyl acrylate, 40% hydroxyethyl acrylate and 5% polymethylmethacrylate").) FF3. Garbe teaches that suitable drugs include fentanyl. (Garbe 12: 28.) FF4. Garbe teaches that "certain drug substances function as softeners, including nicotine." (Id. at 9: 12-13.) FF5. Garbe teaches that the "transdermal drug delivery device that allows dissolution of drug and relatively heavy loading with oily excipients, maintains contact with the skin, and can be removed cleanly from the skin. The pressure sensitive skin adhesives of the invention provide these advantages and in addition adhere to the skin." (Id. at 3: 11-15.) FF6. Garbe teaches that a drug is present in a transdermal device of the invention in an amount of about 0.01 to about 30 percent by weight based on the total weight of the matrix. In a preferred embodiment the drug is substantially fully dissolved, and the matrix is substantially free of solid undissolved drug. (Id. at 13: 16-20.) Principle of Law "The combination of familiar elements according to known methods is likely to be obvious when it does no more than yield predictable results." KSR Int'! Co. v. Teleflex Inc., 550 U.S. 398, 416 (2007). "If the claim extends to what is obvious, it is invalid underÂ§ 103." Id. at 419 (2007). 5 Appeal2013-002877 Application 12/820,280 Analysis The Examiner rejects claim 1 as obvious based on the combination of Garbe and Payne (Final Act. 5-10; Ans. 4--7). We adopt the Examiner's findings of fact, reasoning regarding the scope and content of the prior art, and responses to argument (see Final Act. 10-16; see also Ans. 8-15), and agree that the claims are rendered obvious by Garbe and Payne. We address Appellants' arguments below. Appellants contend that "[ f]entanyl and nicotine ... are entirely different from the standpoint of transdermal delivery," citing Naik5 in support (Br. 3). "Given the known solubility issues associated with fentanyl, a person of ordinary skill, based upon Garbe, would not have expected amounts of about 8 to about 30% fentanyl to be incorporated without undissolved fentanyl." (Br. 4.) We are not persuaded. Garbe teaches a transdermal delivery system and suggests fentanyl as one of the drugs for use in the system (FF1-FF6). We find nothing in Naik that suggests a composition containing 8-30% fentanyl would not be soluble. We agree with the Examiner that merely demonstrating that fentanyl and nicotine have different pharmacochemical and pharmacokinetic properties does not indicate that they "cannot be delivered transdermally using the same polymer. It is known that different drugs have different solubility and it is known that fentanyl can be delivered transdermally." (Ans. 12.) As further pointed out by the Examiner, "Garbe teaches formulation comprising copolymer suitable to deliver different drugs having different properties including [different] solubility." (Ans. 12.) We 5 Naik et al., Transdermal drug delivery: overcoming the skin's barrier function, 3 PSTT 318-326 (2000). 6 Appeal2013-002877 Application 12/820,280 agree with the Examiner that Garbe teaches a transdermal drug delivery device that allows for the dissolution of the drug (FF5) so that the matrix is substantially free of solid undissolved drug (FF6). The Examiner explains that the dissolution of the drug "it is not only suitable for highly soluble drugs, but also less soluble drugs, since the formulation assists in drug dissolution. In other words, the drug does not need to be soluble, rather the copolymer will dissolute [sic] the drug." (Ans. 12.) The Examiner looks to the teaching of Payne for the use of a transdermal delivery system containing fentanyl for the purpose of pain management. Concluding that one of ordinary skill in the art would have been motivated to formulate Garbe' s transdermal device with fentanyl, as already suggested by Garbe itself (FF2), "because Payne teaches that transdermal fentanyl patches satisfy patients in need of pain management." (Final Act. 9.) We recognize, but are not persuaded by, Appellants argument that nicotine and fentanyl have different pharmacokinetic properties. Naik lists the various drugs that have "acceptable (but rather confined) parameter ranges for currently marketed transdermal agents. The net result is that although there are many transdermal candidates (i.e. drugs that would benefit from this mode of delivery), only a limited number possess the ideal physicochemical properties" and fentanyl as well as nicotine are listed by Naik as meeting these narrow limitations (Naik 320-321 ). Thus, there is nothing in Naik to dissuade the ordinary artisan from using fentanyl in a transdermal patch as already suggest by Garbe (FF3). 7 Appeal2013-002877 Application 12/820,280 Appellants contend that reliance on Payne "is irrelevant because its fentanyl patch has an entirely different architecture [see Venkatramann6] from the patch that is the subject of Applicant's claims." (Br. 4.) We are not persuaded. The Examiner looks to Payne solely to establish that administering fentanyl via a transdermal route is desirable "because transdermal fentanyl patches provide lower frequency and reduced impact of side effects." (Final Act. 9, 15 ("Payne is relied upon for ... solely teaching and showing desirability to deliver fentanyl transdermally, versus other routes, to alleviate pain").) Knowing that the transdermal route of fentanyl administration produces less side effects provides motivation to also formulate Garbe's transdermal delivery composition with fentanyl, as already suggested by Garbe (FF2), with a reasonable expectation of success (Final Act. 9). We do not agree with Appellants position that Payne's teaching is irrelevant just because the Duragesic depot patch, a liquid reservoir patch is "structurally distinct from monolithic acrylate copolymer patches." (Br. 5.) We conclude that the evidence cited by the Examiner supports a prima facie case of obviousness with respect to claim 1, and Appellants have not provided sufficient rebuttal evidence or evidence of secondary considerations that outweighs the evidence supporting the prima facie case. As Appellants do not argue the claims separately, claims 2-10 fall with claim 1. 37 C.F.R. Â§ 41.37 (c)(l)(iv). 6 Venkatraman et al., US 2004/0213832 Al, published Oct. 28, 2004. 8 Appeal2013-002877 Application 12/820,280 SUMMARY We affirm the rejection of claim 1under35 U.S.C. Â§ 103(a) over Garbe in view of Payne. Claims 2-10 were not separately argued and fall with claim 1. No time period for taking any subsequent action in connection with this appeal may be extended under 37 C.F.R. Â§ 1.136(a). AFFIRMED 9