10310824 (B.P.A.I. Jan. 5, 2009)

Ex Parte Evans et al

Board of Patent Appeals and InterferencesJan 5, 2009

10310824 (B.P.A.I. Jan. 5, 2009)

UNITED STATES PATENT AND TRADEMARK OFFICE ____________ BEFORE THE BOARD OF PATENT APPEALS AND INTERFERENCES ____________ Ex parte ALLAN EVANS AND ROSS MCKINNON ____________ Appeal 2008-6177 Application 10/310,824 Technology Center 1600 ____________ Decided: January 5, 2009 ____________ Before DEMETRA J. MILLS, RICHARD M. LEBOVITZ, and JEFFREY N. FREDMAN, Administrative Patent Judges. LEBOVITZ, Administrative Patent Judge. DECISION ON APPEAL This is a decision on appeal from the Examiner’s final rejection of claims 1-4, 7, 12, 14-19, 69-78, 81, 86, 88-103, 106, 111, and 113-124. Jurisdiction is under 35 U.S.C. § 6(b). We affirm. Appeal 2008-6177 Application 10/310,824 STATEMENT OF THE CASE The claims are drawn to methods of applying a topical formulation of flurbiprofen to the skin for preventing and reducing the occurrence of non- melanoma skin cancer. Claims 1-4, 7, 12, 14-19, 69-78, 81, 86, 88-103, 106, 111, and 113- 124 are pending and stand rejected as follows: 1) Claims 1-4, 7, 12, 14-19, 100-103, 106, 111, and 113-124 under 35 U.S.C. § 112, first paragraph, as not being enabled (Ans. 41); 2) Claims 1-4, 7, 12, 14-19, 69-78, 81, 86, 88-103, 106, 111, and 113- 124 under 35 U.S.C. § 103(a) as obvious in view of Falk (US 6,103,704, Aug. 15, 2000), Brune (US 5,206,029, Apr. 27, 1993), and Nudelman et al. (US 6,110,955, Aug. 29, 2000) (Ans. 3, 72); and 3) Claims 1-4, 7, 12, 14-19, 69-78, 81, 86, 88-103, 106, 111, and 113- 124 under 35 U.S.C. § 103(a) as obvious over Nudelman (Final Rejection 13; Ans. 113). 1 The Examiner’s statement of the rejection on page 4 of the Answer (Jan. 17, 2007) included claims which are not pending. 2 The Examiner’s statement of the rejection on page 7 of the Answer included claims which are not pending and excluded claims which were indicated as rejected on page 3 of the Answer. In the Reply Brief (Section VI), Appellants properly summarized the rejected claims. We also note that the Examiner indicated on page 3 of the Answer that the rejection was also over Falk, alone, but corrected this on page 7 of the Answer. 3 The Examiner’s statement of the rejection on page 11 of the Answer included claims which are not pending and excluded claims which were indicated as rejected on page 13 of the Final Rejection. In the Reply Brief (Section VI), Appellants properly summarized the rejected claims. 2 Appeal 2008-6177 Application 10/310,824 Claims 1, 75, and 100, which are the only independent claims, are representative and read as follows: 1. A method for preventing the occurrence of non-melanoma skin cancers in a patient, comprising: applying a topical formulation to the skin of said patient, said formulation containing a pharmaceutically effective amount of a non- steroidal anti-inflammatory drug, wherein said nonsteroidal anti- inflammatory drug is an arylpropionic acid derivative, and wherein said non- steroidal anti-inflammatory drug is flurbiprofen. 75. A method for reducing the occurrence of non-melanoma skin cancers in a patient, comprising: applying a topical formulation to the skin of said patient, said formulation containing a pharmaceutically effective amount of a non- steroidal anti-inflammatory drug, wherein said non-steroidal anti- inflammatory drug is an arylpropionic acid derivative, and wherein said non- steroidal anti-inflammatory drug is flurbiprofen. 100. A method for preventing non-melanoma skin cancers in a patient, comprising: applying a topical formulation to skin of said patient, said formulation consisting essentially of a pharmaceutically effective amount of a non- steroidal anti-inflammatory drug, and wherein said non-steroidal anti- inflammatory drug is an arylpropionic acid derivative, and wherein said non- steroidal anti-inflammatory drug is flurbiprofen. REJECTION UNDER § 112, FIRST PARAGRAPH Issue Does the Specification enable preventing skin cancer as recited in claims 1 and 100? Principles of Law “[T]o be enabling, the specification . . . must teach those skilled in the art how to make and use the full scope of the claimed invention without 3 Appeal 2008-6177 Application 10/310,824 ‘undue experimentation.’” In re Wright, 999 F.2d 1557, 1561 (Fed. Cir. 1993). When rejecting a claim under the enablement requirement of section 112, the PTO bears an initial burden of setting forth a reasonable explanation as to why it believes that the scope of protection provided by that claim is not adequately enabled by the description of the invention provided in the specification of the application; this includes, of course, providing sufficient reasons for doubting any assertions in the specification as to the scope of enablement. If the PTO meets this burden, the burden then shifts to the applicant to provide suitable proofs indicating that the specification is indeed enabling. In re Wright, 999 F.2d at 1561-1562. Findings of Fact 1. The Specification describes results of using flurbiprofen as a “chemopreventative NSAID” to prevent skin cancer produced by UV exposure (Spec. 16-20). 2. “Hairless mice [“SKH-1”], as used in the experiments detailed herein, have generally been accepted in the art as a good laboratory test model for predicting the therapeutic results of pharmacological treatments upon mammals, including humans” (Spec. 17:2-6). 3. SKH-1 hairless mice exposed to UV-light were treated with topical flurbiprofen (Spec. 18-19). 4. “The development of skin cancer was assessed as the visible appearance of papillomas, which subsequently developed, in a subset of cases, to tumours” (Spec. 20:4-6). 5. “Comparing the data from the animals that received the highest concentration of flurbiprofen with the control group, it was found that there 4 Appeal 2008-6177 Application 10/310,824 was a greater than 80% reduction in the number of animals that developed skin tumours” (Spec. 23:4-8). 6. A declaration under 37 C.R.R. § 1.132 by Dr. Allan Evans (“Evans Dec.”), an inventor of the claimed invention, was provided by Appellants. Dr. Evans stated: In light of my knowledge of this field, I believe that one skilled in this art would accept reliable animal model data that showed a statistically significant reduction in the number or frequency of skin cancer lesions developed after UV exposure as reasonably supporting that a given drug therapy was effective in preventing the development of skin cancer lesions, pre-skin cancerous lesions, and other related conditions. Data showing absolute prevention of later skin cancer lesions, pre- skin cancerous lesions, and other related conditions one hundred percent of the time would not be necessary to establish efficacy of a drug for prevention of non-melanoma skin cancers. Reliable data showing statistically significant reduction in the occurrence of skin cancer lesions in subjects in addition to a statistically significant delay in the development of lesions in subjects would be considered by one skilled in the art to establish effectiveness of the drug in preventing non-melanoma skin cancers as is described and claimed in the patent application. (Evans Dec. ¶ 4.) 7. Dr. Evans also stated in the same declaration: Those skilled in the field of the identification, testing and validation of drugs and drug therapies relating to skin cancer and other related UV induced skin diseases and disorders, however, readily accept studies in SKH-1 hairless mice to be a good predictor of and have a strong correlation to human efficacy. (Evans Dec. ¶ 9.) Dr. Evans cited a journal article to support his conclusion. 5 Appeal 2008-6177 Application 10/310,824 Analysis The Examiner states that the Specification is “enabling for reducing occurrence of non-melanoma skin cancer development using a topical application of flurbiprofen as a[n] effective NSAID,” but that the Specification “does not reasonably provide enablement for preventing the said cancers” (Ans. 4). In support of this position, the Examiner states: The specification only exemplifies animal test for reducing the yield of papillomas and a possible delay in the onset of tumor development. Human test for evaluating the biological activities of the instant composition is not described. Furthermore, the exemplified animal test does not show complete inhibition or prevention, see figure 1. Therefore, the specification has only enabled the treating said cancers (reduction of occurrence of said cancer or the delay in the onset of tumor development). (Ans. 6.) The Examiner bears the burden of providing an explanation as to why the full scope of the claims is not adequately enabled by the Specification. In re Wright, 999 F.2d at 1561-1562. In this case, the Examiner’s position appears to be that the Specification is not enabled for “preventing . . . non- melanoma skin cancers” as required by independent claims 1 and 100 because the “animal tests” do not show “complete inhibition or prevention” of a skin cancer (Ans. 6). The Examiner contends that prevention requires the method to “’forestall skin cancer completely’” (Ans. 15). The hairless mice model is stated by Appellants to be an accepted model for skin cancer (FF2, 7). The Examiner has not provided evidence which is contrary to the statements in the Specification nor those of Dr. Evans, an inventor, who is also a person knowledgeable in the field to which the invention pertains (Evans Dec. ¶ 3). According to Dr. Evans, persons of 6 Appeal 2008-6177 Application 10/310,824 ordinary skill in the art would have considered the data in the Specification showing “statistically significant reduction in the occurrence of skin cancer lesions in subjects . . . to establish effectiveness of the drug in preventing non-melanoma skin cancers as is described and claimed in the patent application” (FF6). Dr. Evans also states that “prevention” would not be understood by persons of skill in the art to require “absolute prevention” “one-hundred percent of the time” (FF6). The Examiner has not identified any defect in Dr. Evans’s opinion, who is asserted to be “knowledgeable regarding the level of skill contained by a person of ordinary skill in the art to which the invention pertains” (Evans Dec. ¶ 3). Thus, the preponderance of the evidence in this proceeding supports Appellants’ position that the claimed methods are enabled. The Examiner’s misapprehension appears to be based on a claim interpretation that would require non-melanoma skin cancer to be prevented in 100% of the subjects to which flurbiprofen is topically applied (see Ans. 15). However, as explained by Dr. Evans, prevention claims would be reasonably understood to have been satisfied when a cancer is prevented in a significant number of subjects treated with topical flurbiprofen application (FF6). That is, a claim to “preventing” non-melanoma skin cancer is enabled when there is evidence that it would prevent the cancer in a substantial number of subjects to whom it is administered. The claim does not contain language that would require it to prevent cancer in every subject to which the flurbiprofen is administered. Rather, the claim is directed to prevention in a patient. Thus, we conclude that since the claimed method 7 Appeal 2008-6177 Application 10/310,824 would succeed in most patients, it is therefore enabled on a patient by patient basis. The rejection is reversed. OBVIOUSNESS REJECTION OVER FALK, BRUNE, AND NUDELMAN Claims 1-4, 7, 12, 14-19, 69-78, 81, 86, 88-103, 106, 111, and 113- 124 under 35 U.S.C. § 103(a) stand rejected as obvious in view of Falk, Brune, and Nudelman (Ans. 3, 7). Issues on appeal for independent claims 1, 75, and 100 1. Does Falk describe methods “for preventing the occurrence of” (claim 1), “for reducing the occurrence of” (claim 75), and “for preventing” non- melanoma skin cancers in a patient using an NSAID, as in claims 1, 75, and 100, respectively? 2. Would persons of ordinary skill in the art have had reason to utilize flurbiprofen as an NSAID in Falk’s method? 3. Does “consisting essentially of” exclude hyaluronic acid from the formulation of claim 100 “consisting essentially of . . . flurbiprofen” because hyaluronic acid materially affects the formulation’s basic and novel properties? Principles of law “In determining whether obviousness is established by combining the teachings of the prior art, the test is what the combined teachings of the references would have suggested to those of ordinary skill in the art.” In re GPAC Inc., 57 F.3d 1573, 1581 (Fed. Cir. 1995) (internal quotations omitted). “Express suggestion to substitute one equivalent for another need not be present to render such substitution obvious.” In re Fout, 675 F.2d 297, 8 Appeal 2008-6177 Application 10/310,824 301 (CCPA 1982); see also In re Mayne, 104 F.3d 1339, 1340 (Fed. Cir. 1997) (“Because the applicants merely substituted one element known in the art for a known equivalent, this court affirms [the rejection for obviousness].”). Accord KSR Int'l Co. v. Teleflex Inc., 127 S. Ct. 1727, 1740 (2007) (“when a patent claims a structure already known in the prior art that is altered by the mere substitution of one element for another known in the field, the combination must do more than yield a predictable result”). Where, as here, the claimed and prior art products are identical or substantially identical, or are produced by identical or substantially identical processes, the PTO can require an applicant to prove that the prior art products do not necessarily or inherently possess the characteristics of his claimed product. . . . Whether the rejection is based on “inherency” under 35 U.S.C. § 102, on “prima facie obviousness” under 35 U.S.C. § 103, jointly or alternatively, the burden of proof is the same, and its fairness is evidenced by the PTO’s inability to manufacture products or to obtain and compare prior art products. In re Best, 562 F.2d 1252, 1255 (CCPA 1977) (footnote omitted). “[W]hen the PTO shows sound basis for believing that the products of the applicant and the prior art are the same, the applicant has the burden of showing that they are not.” In re Spada, 911 F.2d 705, 708 (Fed. Cir. 1990). “Consisting essentially of” is a transition phrase commonly used to signal a partially open claim in a patent. Typically, “consisting essentially of” precedes a list of ingredients in a composition claim or a series of steps in a process claim. By using the term “consisting essentially of,” the drafter signals that the invention necessarily includes the listed ingredients and is open to unlisted ingredients that do not materially affect the basic and novel properties of the invention. PPG Industries v. Guardian Industries Corp., 156 F.3d 1351, 1354 (Fed. Cir. 1998). 9 Appeal 2008-6177 Application 10/310,824 Findings of Fact (FF) The Falk patent 8. Falk describes topical compositions for application to the skin comprising an effective non-toxic dosage amount of a drug for example a drug which inhibits prostaglandin synthesis for example an NSAID and an effective non-toxic dosage amount of a form of hyaluronic acid (preferably hyaluronic acid or salt thereof) for the transport of the drug to the site of the pathology and/or trauma (Falk, at col. 7, ll. 10-17). 9. Falk states that its compositions may be applied topically to treat diseases and conditions of the skin and/or exposed tissue at the site of the trauma and/or pathology, (for example, basal cell carcinoma, the precancerous, often recurrent, actinic keratoses lesions, fungal lesions, ‘liver’ spots and like lesions (found for the most part in the epidermis), squamous cell tumours (Falk, at col. 7, ll. 42-48). 10. According to Falk, the NSAID blocks prostaglandin synthesis which “then unblocks the macrophages and permits the macrophages of the patient proximate the lesion (for example, the basal cell carcinoma) to destroy the lesion or condition” (Falk, at col. 9, 10-14). Thus, Falk requires an NSAID to have prostaglandin inhibiting activity for it to be effective against cancer. 11. Falk also states that “[t]reatment by dosage amounts of the composition (formulation and/or combination) eliminates the condition without recurrence, even where the lesion has recurred a number of times after unsuccessful treatments according to the prior art” (Falk, at col. 9, ll. 14-18). Falk describes several examples in which basal cell carcinoma was treated with an NSAID formulation resulting in the disappearance of the carcinoma with “no recurrence” (Falk, at col. 35, ll. 25-27 and 45-47). 10 Appeal 2008-6177 Application 10/310,824 12. The hyaluronic acid in Falk’s composition is used to facilitate or cause transport of the NSAID into the skin (Falk, at col. 8, ll. 45-48). 13. Falk describes a formulation comprising 1% and 3% of the NSAID diclofenac and sodium hyaluronate (Falk, at col. 20, ll. 40-50; at col. 23, ll. 45-55). The Brune patent 14. Flurbiprofen is a racemate comprising S(+) and R(-) forms (Brune, at cols. 1-2). 15. Brune teaches that “S(+)-flurbiprofen inhibits the liberation of prostaglandin more markedly than the R(-)-form” (Brune, at col. 2, ll. 25- 27). As shown in Fig. 3 of Brune, at the same concentration, the S-form inhibits prostaglandin synthesis (“PG-Synthesis”) by 95% while the R-form inhibits PG synthesis by 53%. The Nudelman patent 16. Nudelman teaches compounds of Formula I which can be covalently linked to an NSAID (Nudelman, at col. 3, l. 42 to col. 4, l. 4). 17. Flurbiprofen appears in a list of NSAIDs which are described as useful (Nudelman, at col. 7, ll. 35-46; at col. 12, ll. 36-43) and thus would be considered equivalent to other NSAIDs. 18. The compounds can be used for preventing cancers that include squamous carcinomas (Nudelman, at col. 4, l. 17). 19. Nudelman states that it “is believed that the covalent attachment of a beta-oxidation inhibitor [such as an NSAID] in the present compounds is responsible, at least in part, for the enhanced stability and potency of these compounds” (Nudelman, at col. 13, ll. 1-4). 11 Appeal 2008-6177 Application 10/310,824 Analysis Independent claims 1, 75, and 100 involve applying a topical formulation comprising flurbiprofen to prevent the occurrence of non- melanoma skin cancer (claim 1), reduce its occurrence (claim 75), and prevent it (claim 100). In claim 100, the topical formulation is stated to “consist[ ] essentially” of flurbiprofen. Falk teaches that topically applying an NSAID to skin stops the recurrence of basal carcinoma (FF9, 11), which is a skin cancer as in claims 1, 75, and 100. Falk does not disclose that the NSAID is flurbiprofen as required by the claims. However, flurbiprofen is a well-known NSAID having prostaglandin-inhibiting activity (FF14-15, 17), the same activity described by Falk as useful to treat skin cancer (FF10). Thus, persons of ordinary skill in the art would have had reason to use flurbiprofen as the NSAID in Falk’s formulation for its known and expected prostaglandin inhibiting activity. Claims 1-4, 14, and 70-74 Appellants contend that “Falk is focused on the removal of existing skin cancer and actinic keratoses tumors and lesions, not on ‘preventing the occurrence of’ skin cancer” as in the claims (App. Br. 16). Appellants state that Falk describes applying a topical formulation directly to the tumor until it disappears (id.). They assert that “nowhere does Falk disclose, teach or suggest that this topical formulation should be applied to the skin to prevent the occurrence of skin cancer (or to reduce the occurrence of skin cancers), as is claimed by Appellant” (id. at 18). Appellants urge: 12 Appeal 2008-6177 Application 10/310,824 Any patient that has been so unfortunate as to be stricken with non-melanoma skin cancers will readily appreciate the difference between Falk’s treating of cancer tumors by chemical removal after the patient has been diagnosed as having the tumor and Appellant’s prophylactic methods for preventing the occurrence of the tumors. Nevertheless, the Office Action equates chemically killing existing lesion and tumors cells that have been diagnosed by a doctor (i.e., “treating” existing skin cancer tumors), with the Appellant's chemoprevention concept that entails applying a topical formulation as a prophylactic to the skin in order to significantly reduce the chances that new skin cancers will develop on the patient. (Id.) Falk clearly states that its NSAID formulation eliminates basal carcinoma with “no recurrence” (FF11). The Examiner reasonably understood Falk’s teaching that the cancer did not recur after NSAID administration to meet “preventing” as recited in the claims because “recurrence” literally means that cancer did not occur again and is thus prevented. Appellants argue that Falk teaches applying its formulation to a carcinoma already in existence. However, claim 1 does not exclude flurbiprofen application to an existing carcinoma nor does the claim specify a specific administration regime that would exclude Falk’s steps in applying the formulation topically to chemically kill existing lesions. The fact is that Falk states that after the lesions are eradicated by the chemical treatment they do not re-appear – and thus are prevented as in the claims. With regard to the substitution of flurbiprofen for one of the NSAIDs in the Falk patent, Appellants argue that no “discussion is present anywhere in Brune regarding the suitability of such medicaments topically for 13 Appeal 2008-6177 Application 10/310,824 preventing the occurrence of non-melanoma skin cancers, or reducing the occurrence of the same” (App. Br. 19). Therefore, Appellants contend that there would have been no teaching or motivation for modifying the teachings of Falk to produce the invention recited in independent claim 1 (id.). Precise teachings directed to the specific subject matter of a claim are not required to reach a conclusion of obviousness. KSR, 127 S. Ct. at 1741. In this case, the teaching that flurbiprofen is equivalent in activity to other NSAIDS (see FF17 for teaching flurbiprofen in a list of NSAIDs) and that flurbiprofen has prostaglandin inhibiting activity (FF15) would have provided the reason to have used it in Falk’s composition. See also In re Fout, 675 F.2d at 301; In re Mayne, 104 F.3d at 1340; and KSR, 127 S. Ct. at 1740. For the foregoing reasons, we affirm the rejection of claim 1. We also affirm the rejection of dependent claims 2-4, 14, and 70-74 (which incorporate all the limitations of claim 1) because separate arguments for their patentability were not provided. 37 C.F.R. § 41.37(c)(1)(vii). Claims 75-78, 88, and 95-99 Appellants contend, but provide no evidence, that persons of ordinary skill in the art would construe “reducing the occurrence of skin cancer” as recited in claim 75 “to mean that the occurrence of new skin cancer tumors is reduced in a significant matter” (App. Br. 21). This argument is not persuasive. Even if we were to interpret claim 75 to mean reducing the occurrence of “new skin cancer tumors,” Appellants have not provided evidence that preventing the recurrence of a skin cancer at 14 Appeal 2008-6177 Application 10/310,824 a site where it previously existed – as taught by Falk (FF11) – would not involve preventing a new cancer from arising from cells present at the same location. Based on Falk’s teaching that there was no recurrence of basal carcinoma at treated lesions (FF11), the Examiner had a logical basis for believing that Falk’s NSAID formulation reduced and prevented the occurrence of skin cancers at the targeted site. The PTO does not have the ability “to manufacture products or to obtain and compare prior art products.” In re Best, 562 F.2d at 1255. Thus, once sound basis is provided for believing that the prior art accomplishes the same result which is claimed, the burden properly shifts to the applicant to show they are not. See In re Spada, 911 F.2d at 708. Appellants have not met this burden. For the foregoing reasons, we affirm the rejection of claim 75. Dependent claims 76-78, 88, and 95-99 incorporate all the limitations of claim 75 and fall with it because separate arguments for their patentability were not provided. 37 C.F.R. § 41.37(c)(1)(vii). Claims 100-103, 113, and 120-124 Claim 100 is directed to a “method for preventing non-melanoma skin cancers” comprising “applying a topical formulation” which is “consisting essentially” of flurbiprofen. The issue in this rejection is whether “consisting essentially” excludes hyaluronic acid, as taught by Falk, from the claim 100 formulation (see App. Br. 21-22). We interpret the phrase “consisting essentially of” to be partially open-ended in permitting the inclusion of ingredients which “do not materially affect the basic and novel properties of the invention.” PPG Industries v. Guardian Industries Corp., 156 F.3d at 1354. Under this 15 Appeal 2008-6177 Application 10/310,824 interpretation, the underlying question is whether the addition of hyaluronic acid to the formulation of claim 100 materially affects its basic properties. We conclude that the answer to this question is “no.” The Specification teaches that the claimed flurbiprofen is used to prevent skin cancer (FF1). This is the same activity described by Falk for its NSAID composition (FF9). The addition of hyaluronic acid to this composition facilitates NSAID transport into the skin (FF12), but does not change or “materially affect” the NSAID’s basic property in treating skin cancer. Thus, we conclude that hyaluronic acid is not excluded from claim 100. For the foregoing reason and those set forth for claim 1, we affirm the rejection of claim 100. Claims 101-103, 113, and 120-124, which depend on claim 100 and incorporate all its limitations, fall with claim 100 because separate arguments for their patentability were not provided. 37 C.F.R. § 41.37(c)(1)(vii). Claims 7, 69, 81, 94, 106, and 119 As claims 7, 69, 81, 94, 106, and 119 are argued as a group (App. Br. 22), we select claims 7 and 69 as representative to decide the rejection. Claim 7, which depends on claim 1, is directed to a topical formulation which “is substantially free of the S-flurbiprofen enantiomer.” Claim 69, which also depends on claim 1, is directed to a topical formulation in which the flurbiprofen “contains low cyclooxygenase inhibition activity.” Brune discloses that the R-enantiomer of flurbiprofen has less activity in inhibiting prostaglandin than the S-enantiomer (FF15). Nonetheless, since Brune discloses that the R-enantiomer inhibits prostaglandin synthesis – the same activity required by Falk for its NSAIDs 16 Appeal 2008-6177 Application 10/310,824 (FF8, 10) – persons of ordinary skill in the art would have reasonably expected the R-enantiomer to be effective in preventing cancer and thus a logical choice as an NSAID for Falk’s method. A “finding that the prior art as a whole suggests the desirability of a particular combination need not be supported by a finding that the prior art suggests that the combination claimed by the patent applicant is the preferred, or most desirable, combination.” In re Fulton, 391 F.3d 1195, 1200 (Fed. Cir. 2004). In other words, an invention may be suggested by the prior art and therefore obvious, even if inferior to alternatives that would be made by following other prior art suggestions. Thus, we affirm the rejection of claim 7. The R-enantiomer would inherently have “low cyclooxygenase inhibition activity” as it has low prostaglandin inhibiting activity as in claim 69. We affirm its rejection, as well. Claims 81, 94, 106, and 119 falls with claims 7 and 69 because separate arguments for their patentability were not provided. 37 C.F.R. § 41.37(c)(1)(vii). Claims 12, 15, 16, 86, 89, 90, 111, 114, and 115 Dependent claims 12, 86, and 111 add the limitation “wherein said non-melanoma skin cancers comprise basal cell carcinomas, and wherein said patient previously has been diagnosed as having had a basal cell carcinoma” to the limitations of independent claims upon which they depend. Dependent claims 15, 89, and 114 add the limitation where the claimed methods further comprise, before applying of the topical 17 Appeal 2008-6177 Application 10/310,824 formulation, “identifying said patient as being at elevated risk of developing a non-melanoma skin cancer.” Claims 16, 90, and 115 depend from, and thus add the limitation to claims 15, 89, and 114, respectively, that patients are identified as being at elevated risk “whenever said patient previously has been diagnosed as having had a non-melanoma skin cancer.” Appellants contend that Falk relates . . . to the removal of existing skin cancer lesions by chemical means, it does not address explicitly or otherwise suggest to one skilled in the art any reason for determining whether the patient previously has been diagnosed as having had a basal cell carcinoma, or whether the patient is at elevated risk of developing non-melanoma skin cancer (App. Br. 25). This argument is not persuasive. Falk teaches that topically applying its NSAID formulation to a basal carcinoma prevents future occurrence (“recurrence”) of the cancer (FF11). Thus, Falk explicitly discloses the limitation of applying an NSAID to a patient who “has been diagnosed as having had a basal cell carcinoma” recited in claims 12, 86, and 111. With regard to claim 15, 16, and others which refer to a patient identified “as being at elevated risk of developing a non-melanoma skin cancer,” the Examiner states that it is “well known that actinic keratosis is often developed into cancerous cell” and that Falk describes application of its formulation to actinic keratosis (Ans. 16; FF9). Thus, the Examiner’s position appears to be that such a skin area would be an increased risk for developing cancer, meeting the limitation of claim 15, 16, and others. Appellants have not provided evidence to the contrary. 18 Appeal 2008-6177 Application 10/310,824 For the foregoing reasons, we affirm the rejections of claims 12, 15, 16, 86, 89, 90, 111, 114, and 115. Claims 17-19, 91-93, and 116-118 Claims 17-19, 91-93, and 116-118 introduce limitations regarding the amount of NSAID, limiting it to concentrations up to approximately 2% w/v (claims 17, 91, and 116), up to approximately 1% w/v (claims 18, 92, and 117), and up to approximately 0.5% w/v (claims 19, 93, and 118). Appellants contend that “Falk does not teach the use of anything less than 3% by weight NSAID formulations for the treatment of skin cancer or actinic keratoses” (App. Br. 26). We do not agree. Falk clearly describes formulations that comprise 1% of an NSAID (FF13) and thus its teaching falls within the limitations recited in claims 18, 92, and 117. The limitations of “up to approximately 2%” as in claims 17, 91, and 116 and “up to approximately 0.5%” as in claims 19, 93, and 118, are not expressly disclosed in Falk. However, determining effective amounts of NSAID to apply was clearly within the scope of ordinary skill in the art. For instance, Falk generally refers to therapeutic dosages of the NSAID with referring to specific amounts (Falk, at col. 7, ll. 9-20), indicating that effective dosages were routinely determinable. In addition to this, the claimed value of approximately 2% falls within with the disclosed amounts of 1% and 3% NSAID. It is well-established that an overlap in ranges establishes prima facie obviousness. In re Peterson, 315 F.3d 1325, 1329 (Fed. Cir. 2003). Thus, absent evidence to the contrary, we agree with the Examiner’s conclusion that the claimed amounts would have been obvious to persons of ordinary skill in the art. 19 Appeal 2008-6177 Application 10/310,824 We affirm the rejections of claims 17-19, 91-93, and 116-118. OBVIOUSNESS OVER NUDELMAN Claims 1-4, 7, 12, 14-19, 69-78, 81, 86, 88-103, 106, 111, and 113- 124 stand rejected under 35 U.S.C. § 103(a) as obvious over Nudelman (Ans. 11). Issue Does Nudelman describe topical application of flurbiprofen to skin as recited in claims 1, 75, and 100? Analysis Claims 1, 75, and 100 each recite the use of flurbiprofen in preventing and reducing the occurrence of non-melanoma skin cancer. Nudelman teaches a flurbiprofen derivative for preventing skin cancer (FF16, 18), but does not teach flurbiprofen, alone. Rather, Nudelman states that it is necessary to covalently attach it to a Formula I compound to enhance the stability and potency of the latter compounds (FF19). Accordingly, persons of ordinary skill in the art would not have had reason to use flurbiprofen, alone, unattached to the Formula I compound, for skin cancer prevention. We reverse the rejection of claims 1-4, 7, 12, 14-19, 69-78, 81, 86, 88-103, 106, 111, and 113-124. CONCLUSIONS OF LAW The Specification enables preventing skin cancer as recited in claim 1 and 100. We reverse the enablement rejection of claims 1-4, 7, 12, 14-19, 100-103, 106, 111, and 113-124 under 35 U.S.C. § 112, first paragraph. 20 Appeal 2008-6177 Application 10/310,824 We affirm the obviousness rejection of claims 1-4, 7, 12, 14-19, 69- 78, 81, 86, 88-103, 106, 111, and 113-124 in view of Falk, Brune, and Nudelman as Falk describes methods “for preventing the occurrence of” (claim 1), “for reducing the occurrence of” (claim 75), and “for preventing” non-melanoma skin cancers in a patient using an NSAID; persons of ordinary skill in the art would have had reason to utilize flurbiprofen as an NSAID in Falk’s method; “consisting essentially of” does not exclude hyaluronic acid from the formulation of claim 100; and because the specific limitations in the separately argued dependent claims are taught or suggested by Falk in combination with Brune and Nudelman. We reverse the obviousness rejection of claims 1-4, 7, 12, 14-19, 69- 78, 81, 86, 88-103, 106, 111, and 113-124 in view of Nudelman because Nudelman does not teach a topical application of flurbiprofen to skin. TIME PERIOD No time period for taking any subsequent action in connection with this appeal may be extended under 37 CFR § 1.136(a). AFFIRMED cdc HOGAN & HARTSON LLP IP GROUP, COLUMBIA SQUARE 555 THIRTEENTH STREET, N.W. WASHINGTON DC 20004 21