Ex Parte RANGES et al

Patent Trial and Appeal BoardMay 20, 2016

12619913 (P.T.A.B. May. 20, 2016)

UNITED STA TES p A TENT AND TRADEMARK OFFICE APPLICATION NO. FILING DATE FIRST NAMED INVENTOR 12/619,913 11/17/2009 23599 7590 05/24/2016 MILLEN, WHITE, ZELANO & BRANIGAN, P,C 2200 CLARENDON BL VD. SUITE 1400 ARLINGTON, VA 22201 Gerald RANGES 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. BA YER-0002-D02 9542 EXAMINER KANTAMNENI, SHOBHA ART UNIT PAPER NUMBER 1627 NOTIFICATION DATE DELIVERY MODE 05/24/2016 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): docketing@mwzb.com PTOL-90A (Rev. 04/07) UNITED STATES PATENT AND TRADEMARK OFFICE BEFORE THE PATENT TRIAL AND APPEAL BOARD Ex parte GERALD RANGES, WILLIAM SCOTT, MICHAEL BOMBARA, DEBORAH RAUNER, ANIKO REDMAN, ROGER SMITH, HOLGER PAULSEN, DAVID GUNN, JINSHAN CHEN, and JOEL RENICK1 Appeal2013-003060 Application 12/619,913 Technology Center 1600 Before JEFFREY N. FRED MAN, ULRIKE W. JENKS, and CHRISTOPHER G. PAULRAJ, 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 method of treating p38-mediated disease with aryl urea compounds. The Examiner rejects the claims for lack of enablement, obviousness, and on the grounds of nonstatutory obviousness-type double patenting. We have jurisdiction under 35 U.S.C. Â§ 6(b ). We AFFIRM. 1 According to Appellants, the Real Party in Interest is Bayer Healthcare LLC. (Br. 1.) Appeal2013-003060 Application 12/619,913 STATEMENT OF THE CASE Claims 1-16 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 method for the treatment of a disease, other than cancer, mediated by p3 8, comprising administering a pharmaceutical composition comprising a pharmaceutically acceptable carrier and a compound of Formula I I wherein A is optionally substituted C6-12-aryl or Cs-12-heteroaryl; R1 is Hor C1_4-alkyl; R2 and R3 are each independently halogen, -COOR1, -CN, - CONR7R8, or-CH2NHR9; R5 is C3_5-alkyl; R6 is C1-6-alkyl; R7 is hydrogen; R 8 is methyl; R9 is hydrogen, methyl or -CO-R10; and R 10 is hydrogen or methyl optionally substituted by NR62 or COOR6. 2 Appeal2013-003060 Application 12/619,913 The following grounds of rejection are before us for review: I. claims 1-16 under 35 U.S.C. Â§ 112, first paragraph as failing to meet the enablement requirement; II. claims 1-3, 5, 7-11 under 35 U.S.C. Â§ 103(a) as unpatentable over Widdowson; 2 and III. claims 1-16 are rejected under the judicially created doctrine of nonstatutory obviousness-type double patenting. I Issue: Enablement The Examiner's position is that the Specification "while being enabling for [a] method of treating a specific disease mediated by p38, does not reasonably provide enablement for treating any disease mediated by p3 8 by administering a pharmaceutical composition comprising a compound of Formula I." (Ans. 4.) "The specification does not provide sufficient information that all diseases are treatable with pharmaceutical composition comprising compound of Formula I described in the method claims." (Id. at 5.) The Examiner finds that "[t]he claims would reasonably encompass any disease mediated by p3 8 which could be the treatment of unknown diseases." (Id. at 6.) "[T]he treatment of any disease using inhibitors of p38 is highly unpredictable with regard to therapeutic effects." (Id. at 8.) Appellants contend that the Examiner has not established that "there are 'reasons or evidence' to doubt the objective enablement." (Br. 3.) Appellants contend that "the use of p3 8 inhibitors to treat various indications 2 Katherine Lousia Widdowson et al., US 5,886,044, issued Mar. 23, 1999 ("Widdowson"). We note that the Examiner consistently refers this reference as "Louisa" (Ans. 10). 3 Appeal2013-003060 Application 12/619,913 is established as noted in the background section of the application, and would be well understood by one of skill in the art." (Id. at 5.) The issue is: Does the preponderance of evidence of record support the Examiner's conclusion that the claims are not enabled? Findings of Fact Breadth of the claims FF 1. Claim 1 is directed to "[a] method for the treatment of a disease, other than cancer, mediated by p3 8, comprising administering a pharmaceutical composition comprising a pharmaceutically acceptable carrier and a compound of Formula I." FF2. The Examiner finds that "[t]he claims would reasonably encompass any disease mediated by p3 8 which could be the treatment of unknown diseases." (Ans. 6 (emphasis removed).) Presence of Working Examples FF3. The Specification provides "[t]he in vivo inhibitory properties of selected compounds were determined using a murine LPS induced TNFa production in vivo model. BALB/c mice ... in groups often were treated with either vehicle or compound by the route noted .... TNF a levels in sera were measured using a commercial murine TNF ELISA kit." (Spec. 76-76; see Ans. 6 and 14.) Amount of Direction or Guidance Presented FF4. The Examiner finds that "[a]ll of the guidance given by the specification is the in vitro inhibitory properties of the compounds using a p3 8 kinase assay, and in vivo inhibitory properties of selected compounds using a murine LPS induced TNF alpha production in vivo model." (Ans. 6 (emphasis removed).) 4 Appeal2013-003060 Application 12/619,913 State of the Prior Art FF5. The Examiner finds that "the state of the art with regard to treating any disease mediated by p3 8 generally is underdeveloped. In particular, there is no known compound which is effective against all diseases." (Ans. 7 (emphasis removed).) Unpredictability of the Art FF6. The Specification explains that "[ s ]everal patents have appeared claiming polyarylimidazoles and/or compounds containing polyarylimidazoles as inhibitors of p38 .... It has been reported that arylimidazoles complex to the ferric form of cytochrome P450cam ... , causing concern that these compounds may display structure-related toxicity." (Spec. 6; see Ans. 8 ("these compounds may display structure-related toxicity .... Thus the treatment of any disease using inhibitors of p3 8 is highly unpredictable with regard to therapeutic effects").) Quantity of Experimentation FF7. As explained by the Examiner, the quantity of experimentation required to practice the claimed invention is high. First you start out by envisioning the compound, then you choose appropriate carrier, then you decide the route of administration and need to select the appropriate animal model. Once all that is complete "[ o ]ne would then need to test the combination in the model system to determine whether or not the combination is effective for inhibiting TNFapha, and then need to determine if the composition inhibits p38." (Ans. 8.) If unsuccessful, further testing is required after modifications to both compound and assay (id.). "[I]t would be necessary for one to 5 Appeal2013-003060 Application 12/619,913 conduct the preceding experimentation for each type of disease because there is no known drug effective for treating all types of diseases." (Id. at 9.) FF8. The Examiner finds: Since every disease and disorder has its unique chemical pathway of expression, diagnosis and treatment of individual diseases and condition cannot be predicted a priori but must be determined from case to case by painstaking experimental study and when the above factors are weighed together, one of ordinary skill in the art would be burdened with undue "painstaking experimentation study" to determine which compounds of Formula I treats which diseases/ conditions." (Ans. 9.) Principle of Law Factors to be considered in determining whether a disclosure would require undue experimentation ... include (1) the quantity of experimentation necessary, (2) the amount of direction or guidance presented, (3) the presence or absence of working examples, (4) the nature of the invention, (5) the state of the prior art, ( 6) the relative skill of those in the art, (7) the predictability or unpredictability of the art, and (8) the breadth of the claims. In re Wands, 858 F.2d 731, 737 (Fed. Cir. 1988). In order for a medical treatment claim to satisfy the enablement requirement of Section 112, one of ordinary skill in the art must be able to effectively use the claimed treatment method in order to achieve the desired therapeutic result. See, e.g., In re '318 Patent Infringement Litig., 583 F.3d 1317, 1325-27 (Fed. Cir. 2009); Rasmusson v. SmithKline Beecham Corp., 413 F.3d 1318, 1322-25 (Fed. Cir. 2005). When the claims are directed to a treatment using a particular drug, "[ w ]hat is necessary to satisfy the how-to- use requirement ofÂ§ 112 is the disclosure of some activity coupled with 6 Appeal2013-003060 Application 12/619,913 knowledge as to the use of this activity." In re Cortright, 165 F.3d 1353, 13 60 (Fed. Cir. 1999) (citation omitted). Analysis Appellants contend that there is no "'reasons or evidence' to doubt the objective enablement" of the claims (Br. 3), as "the use of p38 inhibitors to treat various indications is established as noted in the background section of the application." (Br. 5.) We are not persuaded. As we balance the Wands factors, the breadth of claim 1 that is directed to the treatment of any p3 8 mediated disease (FF 1 and FF2), the lack of working examples for treating any non-cancer disease that is mediated by p38 (FF3), the lack of specific guidance on how to treat any and all diseases when all the guidance is limited to testing the effect of compounds on the production of TNFa (FF4), the underdeveloped state of the art with respect to showing that there are compounds effective for all diseases (FF5) and the unpredictability and quantity of experimentation (FF6-FF8) combined with a high level of skill supports a finding of lack of enablement with respect to the method of claim 1. We additionally highlight some of the Examiner's reasons for finding a lack of enablement. The Examiner's position is that "[ t ]here are no working examples [in the Specification] for the treatment of a disease using pharmaceutical compositions comprising compounds of Formula (I)." (Ans. 6.) The Examiner recognizes that the Specification teaches the effect of the compounds on the production of TNFa in an animal model (FF3). However, this particular animal model tests the use of the compounds for only a short period of time in the animal and only asks what the effect of the compound is on TNFa production. Additionally, the assay itself does not establish if 7 Appeal2013-003060 Application 12/619,913 there is any benefit to the animal over time as the animals are sacrificed 90 minutes after supplying the compound to the animal (FF3). Although the experiments disclosed in the Specification can be used to test whether the compounds have an effect on the production of TNFa, they do not establish that they can treat any particular p3 8-mediated disease. Furthermore, the background section of the Specification recognizes that some inhibitors of p38, for example polyarylimidazoles, have been shown to be toxic (FF6). Additionally, as pointed out by the Examiner, Appellants "have not specifically described the compounds tested in the p38 assay or LPS induced TNFa production mouse model, [and] they have not correlated the structure of the compounds tested with their relative activity in said assays and they have not tested the compounds in any specific assay, for example specific rheumatoid arthritis assay or any other assays for specific diseases." (Ans. 15.) Accordingly, the experiments disclosed in the Specification are not sufficient to establish that the compounds within the scope of the claims can treat any p38-mediated disease. The Examiner cites Graninger3 and Herlaar4 to support the position that, at the time of filing the present Specification, the prior art recognized that the ability to "treat[] disease by the inhibition of p38 is still exploratory, and other mechanisms are also involved .... Note all these references state that p38-mediated diseases/disorders in general are at best in the early experimental stage and needs further exploratory studies." 3 Graninger and Smolen, One-year inhibition of tumor necrosis factor-a: a major success or a larger puzzle? 13 Current Opinion in Rheumatology 209--213 (2001). 4 Herlaar and Brown, p38 MAPK signalling cascades in inflammatory disease, 5. Mol. Med. Today 439-447 (1999). 8 Appeal2013-003060 Application 12/619,913 (Ans. 13.) Herlaar teaches that "[t]he pyridinyl imidazoles have shown potent inhibitory effects on cytokine production both in vitro and in vivo" and suggest that they may have use in the treatment of inflammatory conditions. (Herlaar 446.) Graninger teaches "the effects of therapeutic TNF blockade on the biology of the disease. The fact that inflammation is not completely halted [in rheumatoid arthritis] and destruction is ongoing in some patients suggests that other mechanisms may also be involved." (Graninger, Abstract.) We agree with the Examiner, that the literature does not provide sufficient evidence that the use of a compound that blocks TNF would also be expected to inhibit a disease mediated by p38. Indeed, Graninger tells us that the assay disclosed in the Specification is insufficient to establish a correlation that an inhibitor of TNF production can be extrapolated to include inhibition of all p38 (see Graninger, Abstract "inflammation is not completely halted"). The preponderance of evidence of record supports the Examiner's conclusion that the Specification fails to provide an enabling disclosure commensurate with the scope of claim 1. Claim 2-16 were not separately argued and fall with claim 1. 3 7 C.F .R. Â§ 41.3 7 ( c )( 1 )(iv). 9 Appeal2013-003060 Application 12/619,913 II. Issue: Obviousness over Widdowson Does the preponderance of evidence of record support the Examiner's conclusion that formula III of Widdowson renders obvious a method of treating a disease using a compound as represented by the claimed formula I? Findings of Fact FF9. Widdowson formula III wherein X is oxygen or sulfur; R is any functional moiety having an ionizable hydrogen and a pKa of 10 or less; R 1 is independently selected from hydrogen; halogen .... Y is independently selected from ... halogen; ... cyano; ... C1-10 alkyl; ... C(O)NRiRs [(Ri and Rs can be hydrogen); C(O)OR12 [(R12 can be hydrogen)]. .. ; n is an integer having a value of 1 to 3; or a pharmaceutically acceptable salt thereof. (Widdowson col. 13, 1. 11 to col. 14, 1. 8) FFlO. Widdowson teaches "[c]ompounds of Formula (III) are also useful for treating a chemokine mediated disease, wherein the chemokine is one which binds to an IL-8 a or B receptor and which method comprises administering an effective amount of a compound of Formula (III) or a pharmaceutically acceptable salt thereof." (Widdowson col. 13, 11. 6-10) 10 Appeal2013-003060 Application 12/619,913 Principle of Law [I]f an examiner considers that he has found prior art close enough to the claimed invention to give one skilled in the relevant chemical art the motivation to make close relatives (homologs, analogs, isomers, etc.) of the prior art compound(s), then there arises what has been called a presumption of obviousness or a prima facie case of obviousness. In re Dillion, 919 F.2d 688, 696 (1990), citing In re Henze, 181 F.2d 196 (CCPA 1950); In re Hass, 141F.2d122, 127, 130 (CCPA 1944). [S]tructural similarity between claimed and prior art subject matter, proved by combining references or otherwise, where the prior art gives reason or motivation to make the claimed compositions, creates a prima facie case of obviousness, and that the burden (and opportunity) then falls on an applicant to rebut that prima facie case. Id. at 692. Analysis The Examiner's position is that "Widdowson clearly teaches the presently claimed thienyl ring. . . . [and explains that] formula III taught by ... Widdowson is a subgenus of instant formula I." (Ans. 17.) The Examiner acknowledges that Widdowson "does not specifically teach the exact position of substitution on the thienyl ring, such as 3, 5 substituted thienyl ring." (Ans. 17 .) Appellants contend "that mere encompassment in a generic formula, without more, is insufficient to render obvious a species or subgenus claimed therein." (Br. 7, citing In re Jones, 21USPQ2d 1941 (Fed. Cir 1992) in support.) The question is, how much picking and choosing would be required to arrive at the claimed subject matter given Widdowson's disclosure? 11 Appeal2013-003060 Application 12/619,913 The Specification explains that cytokines whose production is affected by p38 "include, but are not limited to TNFa, IL-1 and IL-8." (Spec. 7.) Widdowson teaches that compounds falling within the general formula III are active as "treating a chemokine mediated disease, wherein the chemokine is one which binds to an IL-8 a or B receptor" (FFlO). As recognized by the Examiner, Widdowson does not teach the production of a compound with "the exact position of substitution on the thienyl ring, such as 3, 5 substituted thienyl ring." (Ans. 17; FF9.) The similarity between Widdowson's Formula III and the present claim 1 are shown below. Widdowson's disclosure: x '~N- H H Widdowson discloses that X in formula III can be either sulfur or oxygen. (FF9) Claim 1 formula I: H Widdowson requires a selection between and oxygen and a sulfur group. Both structures, however, can be readily envisioned. 12 Appeal2013-003060 Application 12/619,913 Widdowson's disclosure: R (Rl1)m Claim 1 unit A: "R is any functional moiety having A is optionally substituted C6--12-aryl an ionizable hydrogen and a pKa of or CS--12-heteroaryl. (Claim 1) The 10 or less." (FF9.) Such ionizable C6--12-aryl can optionally be hydrogen "groups include, but are substituted with an-OH. (Claim 3.) not limited to, hydroxy, carboxylic acid, thiol, ... More preferably R is OH, SH, or NHS(0)2Rb." (Widdowson col. 4, 11. 6-14 (emphasis added).) "R1 is independently selected from hydrogen; halogen" among others. (FF9.) Accordingly, Widdowson encompasses structures having a C6 aryl that is substituted with an-OH moiety. Thus, Widdowson's structures encompass the structures of "A" as claimed. 13 Appeal2013-003060 Application 12/619,913 Widdowson's disclosure: (Yiâ€¢Yl s "n is an integer having a value of 1 to 3" (FF9.) "Y is independently selected from ... halogen; ... cyano; ... C1-10 alkyl; ... C(O)NR4Rs [(~ andRs can be hydrogen); C(O)OR12 [(R12 can be hydrogen)]." (Widdowson col. 13, 11. 50.) R2 and R3 are each independently halogen, -COOR1, -CN, -CONR7Rs (R7 and Rs can be hydrogen), or - CH2NHR9; Rs is C3--s-alkyl; Widdowson discloses the same substitutions for Y as represented by R2, R3, and Rs of the present claim with the exception of the CH2NHR9 substituent which does not appear disclosed as a potential Y substituent in Widdowson. As recognized by the Examiner, Widdowson "does not specifically teach the exact position of substitution on the thienyl ring, such as 3, 5 substituted thienyl ring." (Ans. 17.) We note however, that the thienyl ring of Widdowson can accept at most three substituents because there are only three open positions on the thienyl ring, "n is an integer having a value of 1 to 3" (Widdowson col. 13, 1. 63). Thus, picking and choosing a position for a Y substituent in the thienyl ring of Widdowson does not present an infinite number of possibilities, and if you are to add two substituents the available options to choose from are even less. As noted in Arkley, "picking and choosing may be entirely proper in the making of a 103, obviousness rejection, where the applicant must be afforded an 14 Appeal2013-003060 Application 12/619,913 opportunity to rebut with objective evidence any inference of obviousness which may arise from the similarity of the subject matter which he claims to the prior art." In re Arkley, 455 F.2d 586, 587-588 (CCPA 1972). Additionally, we find that the list of substituents for Y in Widdowson is not so great as to make it impossible to envision all members of the subgenus. We note that the compounds of Formula III in Widdowson are active at "treating a chemokine mediated disease, wherein the chemokine is one which binds to an IL-8 a or B receptor" (FFlO). "[B]ecause structurally similar compounds will have similar properties, and thus would have same or substantially similar beneficial therapeutic effects. It is pointed out that if the claimed invention and the structurally similar prior art species share any useful property, that will generally be sufficient to motivate an artisan of ordinary skill to make the claimed species. In fact, similar properties may normally be presumed when compounds are very close in structure." (Ans. 18, citing Dillon, 919 F.2d at 693, and MPEP 2144.) We recognize, but are not persuaded by, Appellants' contention that "mere encompassment in a generic formula, without more, is insufficient to render obvious a species or subgenus claimed therein." (Br. 7). We find that the Examiner has reasonably established that the compounds of Formula III of Widdowson are sufficiently close in structure to the claimed compound and are disclosed in Widdowson to effect a similar target, namely IL-8 a target identified in the Specification as being affected by p3 8 (see Spec. 6-7), to have met the burden of establishing a prima facie case. Having considered all of Appellants' arguments and having found them to be unpersuasive, we affirm the Examiner's rejection of claim 1 as described above in conjunction with the reasons of record (see Ans. 10-11, 15 Appeal2013-003060 Application 12/619,913 16-18). Claim 2, 3, 5, and 7-11 have not been separately argued and fall with claim 1. III. Issue: Obviousness-Type Double Patenting Does the preponderance of the evidence of record support the Examiner's conclusion that the recitation of "a pharmaceutical composition comprising a pharmaceutically acceptable carrier" in conjunction with the compound of formula I as recited in the present claims are obvious in light of the claims in Ranges? Findings of Fact FF 11. Claim 1 of Ranges reads, in pertinent part, as follows: A method for the treatment of a disease, other than cancer, mediated by p38, comprising administering a compound of Formula I 0 II A....._ A /B N N ! I H H wherein, .... (Ranges, claim 1.) Analysis Appellants contend that rejection is conclusory and "without more, do[ es] not establish motivation necessary to support a finding of obviousness." (Br. 7 .) The Examiner's position is that the Ranges claims are written in open claim format and encompass additional ingredients such as pharmaceutical 16 Appeal2013-003060 Application 12/619,913 carriers. (Ans. 12.) Because Ranges' claims "do[] not exclude other ingredients as in the pharmaceutical composition of [the] instant invention, ... the instant claims and the method of treating a disease comprising administering pharmaceutical composition claimed in ... [Ranges] are substantially overlapping" (id.), and thereby obvious. Furthermore, the Examiner explains that "water is pharmaceutically acceptable carrier" and that the instant compounds "with the urea linkage would readily absorb moisture" and therefore the pharmaceutical composition for the purpose of administering treatment is obvious (see Ans. 18). We agree with the Examiner's position that one of ordinary skill in the art would have recognized that formulating the compounds as claimed in Ranges with a pharmaceutical carrier, such as water, would be obvious for the purpose of administering the compound to a patient. On the record before us, we conclude the Examiner did not err in rejecting claim 1 on the ground of nonstatutroy obviousness-type double patenting over the claims of Ranges. Claims 2-16 have not been separately argued and fall with claim 1. 17 Appeal2013-003060 Application 12/619,913 SUMMARY We affirm the rejection of claims 1-16 under 35 U.S.C. Â§ 112, first paragraph as failing to meet the enablement requirement. We affirm the rejection of claims 1-3, 5, 7-11under35 U.S.C. Â§ 103(a) as unpatentable over Widdowson. We affirm the rejection of claims 1-16 are rejected under the judicially created doctrine of nonstatutory obviousness-type double patenting. 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. Â§ 1.136(a). AFFIRMED 18