12602827 (P.T.A.B. Aug. 24, 2016)

Ex Parte Berrino et al

Patent Trial and Appeal BoardAug 24, 2016

12602827 (P.T.A.B. Aug. 24, 2016)

UNITED STA TES p A TENT AND TRADEMARK OFFICE APPLICATION NO. FILING DATE FIRST NAMED INVENTOR 12/602,827 05/03/2010 Liberato Berrino 20311 7590 08/26/2016 LUCAS & MERCANTI, LLP 30 BROAD STREET 21st FLOOR NEW YORK, NY 10004 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. 1108.1065 9110 EXAMINER FINN, MEGHAN R ART UNIT PAPER NUMBER 1629 NOTIFICATION DATE DELIVERY MODE 08/26/2016 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): info@lmiplaw.com PTOL-90A (Rev. 04/07) UNITED STATES PATENT AND TRADEMARK OFFICE BEFORE THE PATENT TRIAL AND APPEAL BOARD Ex parte LIBERA TO BERRINO, ANTONIO CASCINO, MARILENA CIPOLLARO, AMALIA FORTE, FRANCESCO ROSSI, GIUSEPPE BIANCHI, and PATRIZIA FERRARI1 Appeal2014-008522 Application 12/602,827 Technology Center 1600 Before DONALD E. ADAMS, JEFFREY N. FREDMAN, and JOHN G. NEW, Administrative Patent Judges. NEW, Administrative Patent Judge. DECISION ON APPEAL 1 Appellants state the real party-in-interest is Sigma-Tau Industrie Farmaceutiche Riunite S.P.A. App. Br. 3. Appeal2014-008522 Application 12/602,827 SU~vHvfARY Appellants file this appeal under 35 U.S.C. Â§ 134(a) from the Examiner's Final Rejection of claims 1 and 3 which stand rejected as unpatentable under 35 U.S.C. Â§ 103 (a) as being obvious over the combination of A. Forte et al., PST 2238 Treatment Affects Gene Expression in Arteriotomy-Injured Milan Hypertensive Rat Strain Carotids, 23 (suppl. 2) JOURNAL OF HYPERTENSION 5244 (2005) ("Forte I"), Mariko Harada- Shiba, Gene Transfer and Target Diseases, NON-VIRAL GENE THERAPY (K. Taira et al., eds.) (Springer 2005) ("Harada-Shiba"), and Rohit Khurana et al., Gene Therapy for Cardiovascular Disease: A Case for Cautious Optimism, 38 HYPERTENSION 1210-16 (2001) ("Khurana"). We have jurisdiction under 35 U.S.C. Â§ 6(b). We AFFIRM. NATURE OF THE CLAIMED INVENTION Appellants' invention is directed to a compound of formula (I) for preparing a medicament for the prevention and/or treatment of obstructive vascular lesions following vascular surgery and for the prevention and/or treatment of diseases due to organ fibrosis. Abstract. 2 Appeal2014-008522 Application 12/602,827 REPRESENTATIVE CLAHv1 Independent claim 1 is representative of the claims on appeal and recites: 1. A method for the treatment of restenosis, said method comprising administering to a mammal in need thereof a compound of formula (I) wherein: the symbol --- represents a single bond; Y is OR4 and --- in position 3 is a single bond which can have an alpha or beta configuration; R is an unsubstituted or substituted 3-furyl; R1 is hydrogen; methyl; ethyl or n-propyl substituted by OH orNRsR6â€¢ ' R2 is hydrogen; R3 is hydrogen; R4 is hydrogen, methyl; or C2-C6 alkyl wherein the alkyl can be unsubstituted or substituted by a quaternary ammonium group or OR7- or NR8R9; Rs, R6 are independently hydrogen; methyl or Rs and R6 taken together with the nitrogen atom form an unsubstituted or substituted saturated or unsaturated penta- or hexa- 3 Appeal2014-008522 Application 12/602,827 rnonoheterocyclic nng, optionally containing another heteroatom chosen from oxygen or sulfur or nitrogen; R7 is hydrogen or methyl; R 8, R9 are independently hydrogen; methyl; or C2-C6 alkyl wherein the alkyl can be unsubstituted or substituted by one NR10R11 , or R8 and R9 taken together with the nitrogen atom form an unsubstituted penta- or hexa-monoheterocyclic ring; R 10, R11 are independently hydrogen, C1-C6 alkyl, or R 10 and R11 , taken together with the nitrogen atom form a saturated penta- or hexa-monoheterocyclic ring, App. Br. 11-12. ISSUES AND ANALYSES We agree with, and explicitly adopt, the Examiner's findings and conclusion that the appealed claims are prima facie obvious over the cited prior art references. We address the arguments raised by Appellants on appeal below. Issue Appellants argue the Examiner erred because the combined cited prior art fails to teach or suggest the limitations of the claims on appeal. App. Br. 9. Analysis Appellants argue Forte I provides only for variations of gene expression in MHS rats following arteriotomy: Appellants assert Forte I is silent with respect to using PST2238 for the treatment of stenosis induced by 4 Appeal2014-008522 Application 12/602,827 arteriotorny. App. Br. 9. According to Appellants, Forte I teaches data that suggest early molecular events involved in arteriotomy-induced stenosis are influenced mainly by hypertension and not by the genetic background shared by the MHS rats employed in the study. Id. Therefore, argue Appellants, in the absence of additional experiments involving MHS rats (i.e., normotensive rats with wild-type genetic backgrounds) a skilled person would not arrive at the conclusion that genetic background has no role in the evolution of gene expression. Id. at 9-10. Rather, Appellants argue, the only plausible conclusion is that PST2238 has some effects on gene expression at an early stage when given to rats which are genetically modified. Id. at 10. Furthermore, Appellants point to Forte I's conclusion "that stenosis was more influenced by hypertension than by genetic background" and argue this conclusion is not supported by the experiments conducted and/or any data. App. Br. 10 (quoting Forte I 5244). To arrive at such a conclusion, Appellants argue, the same experiment should have been conducted on wild-type rats, and a person of ordinary skill in the art would have therefore been forced to conduct undue experimentation. Id. Appellants next argue that Mariko fails to cure the deficiencies of Forte I. App. Br. 10. Appellants point out that Mariko is a chapter in a volume entitled "Non-viral Gene Therapy" and assert that a skilled person in gene therapy is necessarily not a skilled person in medicinal chemistry. Id. Consequently, Appellants contend, to arrive at Appellants' claimed invention, a skilled person could not learn from Mariko the type of molecules required to solve the technical problem of restenosis, nor would 5 Appeal2014-008522 Application 12/602,827 this person have ever sought this kind of prior art after learning the teachings of Forte I. Id. Appellants argue Mariko teaches antisense approaches and overexpression of negative regulators of cell growth, both approaches being anti-proliferative in nature. App. Br. 10. However, Appellants argue, the compounds of their claimed invention do not target proliferation, therefore Mariko would never be considered by a person skilled in the art interested in treating restenosis. Id. Appellants argue further that Khurana is also directed to the field of gene therapy. App. Br. 11. Appellants also contend Khurana is cautious with respect to the expectation of positive results using gene therapy. Id. Appellants point out the only positive results mentioned in Khurana are those of the PREVENT trial that involved transfection with antisense nucleotides aimed at E2F transcription factor; other antisense constructs demonstrated various degrees of efficacy. Id. (citing Khurana 1213). Appellants contend all the experiments taught by Khurana have led to an apoptosis-mediated approach to the regression of intimal disease and, consequently, a person skilled in the art would not have been motivated to use molecules having a mechanism of action different from those taught in Khurana (i.e., not directed to favor apoptosis). Id. (citing, e.g., Khurana 1213). Appellants point to an additional prior art reference they have submitted, viz.: Shahin Assadnia et al., Strain Differences in Neointimal Hyperplasia in the Rat, 84 CIRC. RES. 1252-57 (1999) ("Assadnia"). App. Br. 11-12. According to Appellants, Assadnia teaches, contrary to the teachings of Forte I, that genetic background is highly involved in 6 Appeal2014-008522 Application 12/602,827 progression of stenosis. Id. at 12. Appellants disagree with the Examiner's finding that Assadnia does not teach anything about the influence of the genetic background, arguing that Assadnia teaches analysis of intima growth differences between spontaneously hypertensive and normotensive rats following injury to the left iliac artery. Id. (citing Assadnia Abstr.). Appellants contend Assadnia further teaches that patients with certain allelic combinations will be susceptible to such a complication, whereas patients with different alleles of the crucial genes will be resistant to restenosis. Id. (citing, e.g., Assadnia 1257). Consequently, Appellants argue, unlike the allegedly unsupported conclusion of Forte I, a person skilled in the art would have concluded from the teachings of Assadnia that genetic factors do have an important role in the development of restenosis. Id. The Examiner responds that Forte I teaches the effect of PST2238 on gene expression in MHS rats, which is necessarily directly measuring the effect of a pharmaceutical compound on the expression of genes that are known to be involved in stenosis progression. Ans. 6. The Examiner finds Forte I is not silent with respect to using PST2238 for treatment of stenosis, rather, it teaches treatment of MHS rats with PST2238 induces a change in the expression of genes involved in stenosis progression, in particular delaying and/or lowering activation of transcription factors. Id. at 6-7 (citing Forte I 5244). The Examiner finds that, although Forte I does not explicitly recite the word "treatment," a person of ordinary skill would understand that the focus of the reference is based on measuring the effect of PST2238 in reducing the expression of stenosis-related genes in rat model. Ans. 7. The Examiner finds this teaching demonstrates that PST2238 has a beneficial effect in 7 Appeal2014-008522 Application 12/602,827 reducing the progression of stenosis, at least in a mammalian model. Id. The Examiner therefore disagrees with Appellants' argument that Forte I is silent with respect to "treatment"; the Examiner finds treatment of stenosis is an obvious goal of studying the effect of a pharmaceutical active agent (i.e., PST2238) already known in the art to lower blood pressure in an animal model for stenosis/restenosis. Id. The Examiner further finds Appellants' argument with respect to wild-type, normotensive rats does not invalidate Forte I's conclusions. App. Br. 10. The Examiner finds Forte I teaches comparing the effects of hypertension and the genetic background solely of MHS rats. Id. The Examiner finds the conclusions of Forte I are directly supported by the data showing that the PST 223 8 lowered levels of gene expression, such as c- myc, and not others such as apoptosis-related genes. Id. (citing Forte I 5244). With respect to Mariko, the Examiner finds there is no requirement that a person be a skilled artisan in both medicinal chemistry and gene therapy areas to render the teachings relevant or the invention obvious. Ans. 11. The Examiner finds Forte I teaches both the relationship between PST2238 administration and gene expression and is therefore directed towards both gene therapy and medicinal chemistry. Id. The Examiner finds Forte I is thus directed to persons of ordinary skill in the art in both areas. Id. The Examiner finds a person of ordinary skill would be motivated to look to Mariko because the teachings of Forte I does not provide much background beyond the effects of PST223 8 upon the downregulation of stenosis-related genes. Id. at 11-12. The Examiner finds a person of ordinary skill would be motivated to look for other references directed to the 8 Appeal2014-008522 Application 12/602,827 expression of c-rnyc (and other) stenosis-related genes and treatment of restenosis which are subjects to which both the Mariko and Khurana references are directed. Id. at 12. The Examiner finds, by way of example, that Khurana teaches upregulation of inactivating genes (including c-myc) as a treatment for inhibiting restenosis in animal models. Id. (citing Khurana, 1213). We are not persuaded by Appellants' arguments. As an initial matter, we are not persuaded by Appellants' argument that a person of ordinary skill would have been forced to conduct undue experimentation in wild-type rats to arrive at the conclusions of Forte I. See App. Br. 10. "Undue experimentation" is part of the test for determining whether a claim is enabled by the specification. See Nat 'l Recovery Techs., Inc. v. Magnetic Separation Sys., Inc., 166 F.3d 1190, 1196 (Fed. Cir. 1999) ("The scope of enablement, in tum, is that which is disclosed in the specification plus the scope of what would be known to one of ordinary skill in the art without undue experimentation"). The proper test for obviousness, rather, "is what the combined teachings of the references would have suggested to those of ordinary skill in the art." In re Keller, 642 F.2d 413, 425 (C.C.P.A. 1981). Moreover, we find Forte I is enabling to the extent that it teaches administration of PST2238 to an animal with an induced stenosis and a risk (due to hypertension) of developing restenosis. See Forte I 5244. The main thrust of Appellants' arguments with respect to Forte I is that Forte I does not teach the portion of claim 1 reciting: "A method for the treatment of restenosis, said method comprising administering to a mammal in need thereof a compound of formula (I)" and specifically, that neither Forte I, nor the other cited prior art, teaches the "treatment of restenosis." 9 Appeal2014-008522 Application 12/602,827 See App. Br. 9. However, the "treatment of restenosis" is part of the language of the preamble to the claims, and such language is generally not limiting upon the claim "where a patentee defines a structurally complete invention in the claim body and uses the preamble only to state a purpose or intended use for the invention." Rowe v. Dror, 112 F.3d 473, 478 (Fed. Cir. 1997)). See In re Montgomery, 677 F.3d 1375, 13801381 (Fed. Cir 2012) (We are skeptical that a proper interpretation of the claims would include an efficacy requirement. In Bristol-Myers Squibb Co. v. Ben Venue Laboratories, Inc., we construed a similar method-of- treatment claim-involving ' [a] method for reducing hematologic toxicity' by administering taxol to a cancer patient-and held that it "merely express[ ed] a purpose of reducing hematologic toxicity" rather than requiring a particular result.) Such a construction is even more appropriate here in the examination context, where we apply the "broadest reasonable interpretation consistent with the specification." In re Am. Acad. of Sci. Tech Ctr., 367 F.3d at 1364"). In the appeal at bar, the body of the claim recites: "administering to a mammal in need thereof a compound of formula (I)" and the subsequent limitations further define the physical scope of formula (I). Appellants do not dispute the Examiner's finding that Forte I teaches administration of PST2238 (i.e., l 7B-(3-furyl)-5B-androstane-3a, 14B, l 7a-triol, a selected embodiment of formula (I)) to a mammal in need of treatment for steno sis. See Final Act. 3. Nor do Appellants dispute the Examiner's finding that Forte I teaches hypertension is a risk factor for restenosis. Id. at 4; see also Forte I 5244 ("Hypertension, diabetes and hypercholesterolemia are recognized as risk factors for restenosis occurrence in patients"). 10 Appeal2014-008522 Application 12/602,827 Furthermore, we agree with the Examiner that Forte teaches administration of PST223 8 to animals with an induced stenosis and which are at risk (due to hypertension) of restenosis. We agree that a person of ordinary skill in the art would therefore realize from the teachings of Forte I that the purpose of the study was to determine the effects of administration of PST2238 on events (i.e., downregulation of genes) that are known in the art to promote restenosis in a mammal at risk of restenosis, and therefore in need of the treatment. We consequently find that, because the preambular language of claim 1 does not limit the scope of the claim, and because Forte I teaches the remaining limitations of claim 1 (i.e., administration of formula (I) to a mammal in need thereof), Appellants' arguments are moot. We consequently affirm the Examiner's rejection of claims DECISION The Examiner's rejection of claims 1 and 3 as unpatentable under 35 U.S.C. Â§ 103(a) is affirmed. No time period for taking any subsequent action in connection with this appeal may be extended under 37 C.F.R. Â§ l.136(a). AFFIRMED 11