12883873 (P.T.A.B. Jun. 17, 2014)

Ex Parte Lichtenberger

Patent Trial and Appeal BoardJun 17, 2014

12883873 (P.T.A.B. Jun. 17, 2014)

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. 12/883,873 09/16/2010 Lenard M. Lichtenberger 102087-0102 5669 22428 7590 06/17/2014 FOLEY AND LARDNER LLP SUITE 500 3000 K STREET NW WASHINGTON, DC 20007 EXAMINER KISHORE, GOLLAMUDI S ART UNIT PAPER NUMBER 1612 MAIL DATE DELIVERY MODE 06/17/2014 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 PATENT TRIAL AND APPEAL BOARD __________ Ex parte LENARD M. LICHTENBERGER __________ Appeal 2014-002745 Application 12/883,873 Technology Center 1600 __________ Before DEMETRA J. MILLS, JEFFREY N. FREDMAN, and ULRIKE W. JENKS, Administrative Patent Judges. FREDMAN, Administrative Patent Judge. DECISION ON APPEAL This is an appeal1 under 35 U.S.C. § 134 involving claims to a pharmaceutical composition that is a NSAID-in-oil suspension. The Examiner rejected the claims as obvious. We have jurisdiction under 35 U.S.C. § 6(b). We reverse. 1 Appellant identifies the Real Party in Interest as The Board of Regents of the University of Texas System (see App. Br. 1). Appeal 2014-002745 Application 12/883,873 2 Statement of the Case Background “NSAIDs constitute a family of compounds, the first of which to be discovered being aspirin, that have the capacity to inhibit a number of biological pathogenic processes including; fever, inflammation, pain, thrombosis and carcinogenesis” (Spec. 1, ll. 22-24). The Specification teaches that “our group evaluated the GI toxicity of a number of NSAIDs that were chemically pre-associated with synthetic or purified PC [phosphatidylcholine], prior to administration, and obtained evidence that these novel drugs were far less injurious, with regards to GI lesion formation and bleeding than the unmodified NSAIDs” (Spec. 5, ll. 13- 16). The Specification teaches that the “applicability of this approach to human disease was recently confirmed when pilot clinical studies revealed that PC - aspirin, employing purified (93% pure) PC, induced significantly fewer gastric lesions in human subjects than unmodified aspirin” (Spec. 5, ll. 16-19). The Claims Claims 53-56 and 59-64 are on appeal. Independent claim 53 is representative and reads as follows: 53. A pharmaceutical composition that is a non- steroidal anti-inflammatory drug (NSAID)-in-oil suspension, comprising a lecithin oil consisting of soy lecithin components in sunflower oil, wherein said lecithin oil has about 33-40 wt.% phosphatidylcholine (PC), about 26-31 wt.% triglycerides, about 8-13 wt.% free fatty acids, and about 5-9 wt. % glycolipids and a solid NSAID, wherein Appeal 2014-002745 Application 12/883,873 3 (a) the NSAID associates with a phospholipid of the lecithin oil, (b) the NSAID is present in a therapeutically effective amount, and (c) the composition has a gastrointestinal (GI) toxicity that is reduced relative to the NSAID alone. The issue The Examiner rejected claims 53-56 and 59-64 under 35 U.S.C. § 103(a) as obvious over Lichtenberger ’4512 or Lichtenberger ’7803 or Lichtenberger ’0734 and Dickinson5 and Ghyczy6 (Ans. 3-5). The Examiner finds that “Lichtenberger discloses formulations containing a phospholipid and NSAIDs for the treatment of pain and inflammation. The phospholipids taught are DPPC and lecithin” (Ans. 3). The Examiner finds that “[s]ince Lichtenberger uses lecithin which is [the] same as applicant's, it is the examiner’s position that lecithin in Lichtenberger contains the same amounts of phosphatidylcholine” (Ans. 3). The Examiner finds that “Dickinson discloses ibuprofen and lecithin formulations. The process of preparing aqueous suspensions of ibuprofen by the addition [of] ibuprofen to lecithin such as soybean lecithin” (Ans. 4). The Examiner finds that “Ghyczy teaches that NSAIDs have side effects such as bleeding and stomach ulcers and administration together with 2 Lichtenberger et al., US 5,955,451, issued Sept. 21, 1999. 3 Lichtenberger et al., WO 96/22780 A1, published Aug. 1, 1996. 4 Lichtenberger et al., WO 98/13073 A1, published Apr. 2, 1998. 5 Dickinson, J., US 6,287,592 B1, issued Sept. 11, 2001. 6 Ghyczy et al, US 4,421,747, issued Dec. 20, 1983. Appeal 2014-002745 Application 12/883,873 4 phospholipids reduces the ulceration. The phospholipids taught include those from soy bean [sic] and eggs” (Ans. 4). The Examiner finds that “Lichtenberger, WO 98 and 96 do not specifically teach ‘lecithin oil’” (Ans. 4). The Examiner finds it obvious [T]o include an oil in additional amounts in the lecithin preparations of Dickinson and/or Ghyczy with a reasonable expectation of success would have been obvious to one of ordinary skill in the art since Lichtenberger, WO 96 and WO 98 teach that the complexes of NSAID and phospholipids or lecithin or these complexes along with an oil could be used. (Ans. 5). The issues with respect to this rejection are: (i) Does the evidence of record support the Examiner’s conclusion that the cited prior art renders obvious a composition comprising “a lecithin oil consisting of soy lecithin components in sunflower oil” and “a solid NSAID” where the lecithin oil has “about 33-40 wt.% phosphatidylcholine (PC), about 26-31 wt.% triglycerides, about 8-13 wt.% free fatty acids, and about 5-9 wt. % glycolipids” as required by claim 53? (ii) If so, has Appellant presented evidence of secondary considerations, that when weighed with the evidence of obviousness, is sufficient to support a conclusion of non-obviousness? Findings of Fact 1. Lichtenberger ’451 teaches that “the combination of low amounts of nonsteroidal anti-inflammatory drugs with phospholipid have potent pharmacological activity, while doses of the drug alone (i.e., without zwitterionic phospholipid) do not” (Lichtenberger ’451, col. 4, ll. 8-12). Appeal 2014-002745 Application 12/883,873 5 2. Lichtenberger ’451 teaches an example where “the NSAID is aspirin, salicylate, a salt thereof, or a combination thereof. While any of a number of different zwitterionic phospholipids may be employed in the composition of the method, in some embodiments, the phospholipid is dipalmitoyl phosphatidyl choline, phosphatidyl choline, or a combination thereof” (Lichtenberger ’451, col. 5, ll. 57-62). 3. Lichtenberger ’451 teaches that “the sodium salts of the NSAIDs are readily soluble in either saline or water, and are removed from solution as a complex within minutes after an equimolar concentration of DPPC is added as a lipidic suspension” (Lichtenberger ’451, col. 16, ll. 45-49). 4. Lichtenberger ‘451 teaches that: NSAID was added to chloroform at a 30 nM final concentration. DPPC was dissolved in the chloroform that was contained in half the tubes at a final concentration which ranged between 5-40 nM, prior to the addition of the NSAID salt. DPPC, as well as PC and other zwitterionic phospholipids useful in the practice of the invention, may also be dissolved in other organic solvents, such as ethanol, in the practice of the present invention. The tubes were gently mixed at 25° C. for 16 hrs (Lichtenberger ‘451, col. 16, ll. 1-9). 5. Dickinson teaches that The ibuprofen and soybean lecithin were milled together and then blended with the remaining powder excipients until a homogeneous mixture was obtained. . . . The contents of the sachet were placed into a cup and 200 ml substantially boiling water added. The ibuprofen melted and was immediately emulsified to form a satisfactory drink formulation. The emulsified phase was Appeal 2014-002745 Application 12/883,873 6 present as small droplets distributed evenly throughout the drink to give satisfactory slightly cloudy homogeneous appearance. (Dickinson, col. 14, ll. 8-17.) 6. Dickinson teaches that the “granular mixture may also be prepared by granulating the ibuprofen, soybean lecithin and sodium lauryl sulphate in a high speed mixture using aqueous ethanol as the granulating liquid” (Dickinson, col. 14, ll. 30-33). 7. Ghyczy teaches that the “novel mixture of the present invention comprising non-steroidal antiphlogistic substances and phospholipid is particularly suitable for oral application where the molar ratio of antiphlogistic substance to phospholipid ranges from about 1:0.1 to about 1:20, and preferably from about 1:0.5 to about 1:2” (Ghyczy, col. 3, ll. 17 22). 8. Ghyczy teaches that: The mixture can be prepared by dissolving the antiphlogistic substance and the phospholipid in a suitable organic solvent such as methanol, ethanol or chloroform and by subsequently separating the solvent from the mixture by distillation. The antiphlogistic substance can also be dissolved in water at a suitable pH with the phospholipid being stirred into the solution. (Ghyczy, col. 3, ll. 23-28.) 9. The Shaw Declaration7 teaches that: [A] person knowledgeable in the lipids field would read “lecithin oil” in the ’873 application as referring to a free- 7 Declaration of Dr. Walter A. Shaw, filed Oct. 11, 2012. Appeal 2014-002745 Application 12/883,873 7 flowing composition of lecithin (USP/NF definition) in an oil, as illustrated by the product PHOSAL 35 SB. This interpretation of the ’873 application pertains, I believe, because the term “lecithin oil” is generally not used in the field to designate a purified PC dispersed in an oil. Rather, this terminology typically would be used for products similar to Phosal® 35 SB, i.e., to denote crude lipid mixtures dissolved in oil. (Shaw Decl. 3 ¶ 10.) 10. The Marathi Declaration8 teaches that “the suspensions of NSAID in lecithin oil, as described in the ’873 application, exhibit properties that distinguish the suspensions both from NSAIDS alone and from microemulsions, per the ‘073 publication, that contain aspirin, PC, and triglyceride” (Marathi 2 ¶ 7). 11. Figure 6 of the Marathi Declaration is reproduced below: 8 First Declaration of Dr. Upendra K. Marathi, submitted Feb. 21, 2013. Appeal 2014-002745 Application 12/883,873 8 “As shown in Figure 6 . . . the aspirin tablet (composition V) exhibited rapid release into simulated gastric fluid, while composition VI exhibited only a slightly delayed and slightly reduced release in simulated gastric fluid. By contrast, composition VII was characterized by a different ASA release profile, displaying not only a substantial reduction of ASA release, but also a significant delay in ASA release” (Marathi Decl. 6 ¶ 18). 12. The Lichtenberger Declaration9 teaches: [S]everal observations about NSAID-in-lecithin oil suspensions that were unexpected in light of conventional knowledge, as evidenced by the above-discussed documents. That is, NSAID-in-lecithin oil suspensions (1) exhibit a reduced GI toxicity, relative to an NSAID alone, that (2) pertains even in formulations that contain a lower amount of PC than the 1: 1 molar ratio of PC:NSAID formulations that W096, W098 and the ‘451 patent disclose and that the field favored before the subject application was filed, and (3) they also display an increase in NSAID long-term stability, compared to the NSAID:PC emulsions or aqueous lipidic suspensions made heretofore. (Lichtenberger Decl. 3 ¶ 8.) Principles of Law “In proceedings before the Patent and Trademark Office, the Examiner bears the burden of establishing a prima facie case of obviousness based upon the prior art.” In re Fritch, 972 F.2d 1260, 1265 (Fed. Cir. 1992). 9 Declaration of Dr. Lenard M. Lichtenberger, submitted Jul. 31, 2013. Appeal 2014-002745 Application 12/883,873 9 “[O]bviousness requires a suggestion of all limitations in a claim.” CFMT, Inc. v. Yieldup Int’l Corp., 349 F.3d 1333, 1342 (Fed. Cir. 2003). “[E]vidence rising out of the so-called ‘secondary considerations’ must always when present be considered en route to a determination of obviousness.” Stratoflex, Inc. v. Aeroquip Corp., 713 F.2d 1530, 1538 (Fed. Cir. 1983). Analysis Prima facie case The Examiner finds that Since Lichtenberger, WO 98, WO 96 teach the same NSAIDs and lecithin and oil, they would be in the same form (either as a suspension or solution) just as in instant case whether the references hint at a suspension or not. It is unclear to the examiner how compositions containing the same ingredients would be in a solution form in one case and in a suspension form in another case (Ans. 6). We find the Examiner’s position unpersuasive. The compositions of Lichtenberger ’451, Dickinson, and Ghyczy differ from the claimed composition, which requires “soy lecithin components in sunflower oil,” with a specific lipid composition. None of the references teach placing soy lecithin in sunflower oil, as required by both independent claims, nor do the references teach the specific lipid component concentrations. For example, the Examiner finds that “egg lecithin contains 69 % phosphatidylcholine and soybean lecithin contains 21 % phosphatidylcholine; Further according to Dickenson [sic], lecithin contains various other phospholipids, triglycerides (oils), fatty acids and Appeal 2014-002745 Application 12/883,873 10 carbohydrates” (Ans. 4). Even if we, incorrectly, assumed that these sources had 26-31 wt% triglycerides, 8-13 wt% free fatty acids, and 5-9 wt.% glycolipids, both soybean lecithin and egg lecithin differ from the claimed 33-40 wt% phosphatidylcholine amount required by both claims 53 and 54. However, we cannot correctly assume that egg lecithin or soybean lecithin inherently have the required amounts of triglycerides, free fatty acids, and glycolipids required by claims 53 and 54. “Inherency, however, may not be established by probabilities or possibilities. The mere fact that a certain thing may result from a given set of circumstances is not sufficient.” MEHL/Biophile Int’l Corp. v. Milgraum, 192 F.3d 1362, 1365 (Fed. Cir. 1999). Nor has the Examiner established that the changes in ranges would have been obvious, since neither the 21 % phosphatidylcholine in soybean lecithin or the 69 % phosphatidylcholine in egg lecithin either falls into, or adjacent to, the claimed 33-40 wt% range claimed. The Examiner also does not establish that the amounts of triglycerides, free fatty acids or glycolipids in the prior art fall into, or adjacent, the claimed ranges, as required for a presumption of obviousness. See, e.g., In re Peterson, 315 F.3d 1325, 1329 (Fed. Cir. 2003). Thus, the Examiner provides no example in the prior art of an NSAID in an “in-oil suspension” with “soy lecithin components in sunflower oil” and where the lecithin oil has “about 33-40 wt.% phosphatidylcholine (PC), about 26-31 wt.% triglycerides, about 8-13 wt.% free fatty acids, and about 5-9 wt. % glycolipids” as required by both independent claims 53 and 54. Appeal 2014-002745 Application 12/883,873 11 Unexpected results Appellant contends that “the declaration from Dr. Upendra Marathi details the unexpectedly greater hydrophobicity and surprisingly different NSAID release profile in simulated gastric fluid of the presently claimed NSAID-in-lecithin oil suspensions as compared to emulsions that contain aspirin, PC and a triglyceride oil as disclosed in the Lichtenberger references” (App. Br. 19). We agree with Appellant. As noted by Appellant, Figure 6 of the Marathi Declaration shows a comparison between a product formed by the claimed method and a product formed by the closest prior art method of Lichtenberger ’451 (FF 11). We agree that Lichtenberger ’451 is at least as close prior art as either Dickinson or Ghyczy, since none of the prior art uses the same oil, sunflower oil, or the same lipid concentrations as required by claims 53 and 54. In the comparison of the claimed invention with Lichtenberger ’451, the dissolution rate of aspirin in mock stomach acid at the 60 minute timepoint differed from 80% dissolution for the prior art with only 20% dissolution in the instantly claimed invention (FF 11). In the absence of any evidence presented by the Examiner explaining why such a difference would have been expected, we agree with Appellant that this represents a substantial and unexpected difference, which is consistent with the claimed invention, and represents a comparison with the closest prior art. Conclusion of Law (i) The evidence of record does not support the Examiner’s conclusion that the cited prior art renders obvious a composition comprising “a lecithin Appeal 2014-002745 Application 12/883,873 12 oil consisting of soy lecithin components in sunflower oil” and “a solid NSAID” where the lecithin oil has “about 33-40 wt.% phosphatidylcholine (PC), about 26-31 wt.% triglycerides, about 8-13 wt.% free fatty acids, and about 5-9 wt. % glycolipids” as required by claim 53. (ii) In addition, Appellant has presented evidence of secondary considerations, that when weighed with the evidence of obviousness, is sufficient to support a conclusion of non-obviousness. SUMMARY In summary, we reverse the rejection of claims 53-56 and 59-64 under 35 U.S.C. § 103(a) as obvious over Lichtenberger ’451 or Lichtenberger ’780 or Lichtenberger ’073 and Dickinson and Ghyczy. REVERSED cdc