13656573 (P.T.A.B. Jan. 4, 2018)

Ex Parte Nazzal et al

Patent Trial and Appeal BoardJan 4, 2018

13656573 (P.T.A.B. Jan. 4, 2018)

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. 13/656,573 10/19/2012 Sami Mahmoud Nazzal 011.08 4963 107354 7590 Edel Patents LLC 8550 United Plaza Blvd., Suite 702 Baton Rouge, LA 70809 EXAMINER BASQUILL, SEAN M ART UNIT PAPER NUMBER 1613 NOTIFICATION DATE DELIVERY MODE 01/08/2018 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): j ohn @ edelpatents. com PTOL-90A (Rev. 04/07) UNITED STATES PATENT AND TRADEMARK OFFICE BEFORE THE PATENT TRIAL AND APPEAL BOARD Ex parte SAMI MAHMOUD NAZZAL, PAUL W. SYLVESTER, and ALAADIN Y. ALAYOUBI Appeal 2017-001371 Application 13/656,573 Technology Center 1600 Before DONALD E. ADAMS, JEFFREY N. FREDMAN, and ROBERT A. POLLOCK, Administrative Patent Judges. FREDMAN, Administrative Patent Judge. DECISION ON APPEAL This is an appeal1 under 35 U.S.C. § 134 involving claims to a vitamin E composition. The Examiner rejected the claims as obvious. We have jurisdiction under 35 U.S.C. § 6(b). We affirm. Statement of the Case Background “Vitamin E is a group of compounds having eight members . . . Compounds and formulations disclosed herein have potential use as 1 Appellants identify the Real Party in Interest as First Tech International Limited (see App. Br. 3). Appeal 2017-001371 Application 13/656,573 pharmaceutical products and may be employed in the treatment of various maladies including cancer and may specifically have uses in the treatment of breast, colon and other related cancers” (Spec. ^ 2). The Specification indicates that vitamin E compounds include a-tocopherol and a, y, and 5- tochotrienols. (See id. at 42). The Claims Claims 56-75 are on appeal. Independent claim 56 is representative and reads as follows: 56. A composition of matter comprising: a. a quantity of vitamin E; b. a glycerol ester; and c. a polyoxyethylated triglyceride; d. wherein the composition of matter is sufficiently homogenized to perform as a self-emulsifying drug delivery system; e. wherein the quantity of vitamin E is at least 15 weight percent of the composition of matter; and f. wherein the quantity of vitamin E is at most 55 weight percent of the composition of matter. The Issue The Examiner rejected claims 56-75 under 35 U.S.C. § 103(a) as obvious over Ho2 and Lipari3 (Ans. 2-8). The Examiner finds “Ho describes self-emulsifying formulations (SEDDS) containing fat-soluble (ergo lipophilic or sparingly soluble in water) drugs which form emulsions upon contact with gastrointestinal 2 Ho et al., US 6,596,306 Bl, issued July 22, 2003. 3 Lipari et al., US 2007/0104780 Al, published May 10, 2007. 2 Appeal 2017-001371 Application 13/656,573 fluids” (Ans. 4). The Examiner finds Ho teaches “TOCOMIN tocotrienols in 25%, each of either palm olein or soybean oil at 58.6%, LABRASOL at 14.5%, and TWEEN 80 at 2.2% of the composition” {id. at 5). The Examiner finds that based on Ho, the “artisan can at once envisage the use of tricaprylin caprylic/capric triglycerides in place of the other two particularly embodied oily vehicles [palm oil or soybean oil] that comprise the total list of suitable alternatives” {id. at 5). The Examiner acknowledges “Ho does not recite the use of polyethoxylated castor oil, ethanol, a glycerol ester, or the precise triglyceride or tocotrienol concentrations claimed recited” (Ans. 6). The Examiner finds Lipari teaches “that a combination of phospholipid, solubilizing agent, and surfactant system each combine to improve the solubilization of the sparingly soluble drug to be deliver” {Ans. 6). The Examiner finds Libari teaches “capric and caprylic acid triglycerides exemplified by CAPTEC 355”; “ethanol” and “polyoxy 35 castor oil such as CREMOPHOR EL” {id.). The Examiner finds Ho and Lipari teach the component concentrations are “very important for establishing enhanced drug absorption and self-emulsifying properties” (Ans. 6). The Examiner finds it obvious to have incorporated any, or indeed all, of the phospholipid, ethanol, or polyoxy castor oil taught by Lipari as either alternative surfactants, solubilizers, or adjuvants designed to improve a SEDDS for the delivery of sparingly soluble therapeutic active agents into the SEDDS taught by Ho as useful for forming finely divided emulsions for delivering the tocotrienol lipophilic active agent. {Id. at 7). 3 Appeal 2017-001371 Application 13/656,573 The issue with respect to this rejection is: Does the evidence of record support the Examiner’s conclusion that Ho and Lipari render claim 56 obvious? Findings of Fact 1. Ho teaches a “pharmaceutical formulation for oral administration which comprises: (i) a fat-soluble drug; (ii) an appropriate oil; and (iii) an appropriate surfactant system; the resulting formulation which self-emulsifies under gentle agitation in the presence of an aqueous medium” (Ho 2:46-52). 2. Ho teaches a “formulation of tocotrienols, in which the tocotrienols are incorporated into a palm olein-surfactant system to form a self-emulsifying system” (Ho 2:54-56). 3. Ho teaches different surfactant systems at various ratio were tried out to get a self-emulsifying drug delivery system (SEDDS). The aim of this part of the study is to incorporate tocotrienols into a suitable surfactant different surfactant systems at various ratio were tried out to get a self-emulsifying drug delivery system (SEDDS). The aim of this part of the study is to incorporate tocotrienols into a suitable surfactant. (Ho 3:64 to 4:3). 4. Ho teaches a table of the final formulation reproduced below: IngredientsS-- Weight per capsule (mg) Tocomrn ®50% 148.66 Palm olein/soybean oil 351,34 Labrasol 87.00 Tween 80 13,00 'Total weight 600.00 4 Appeal 2017-001371 Application 13/656,573 (Ho 4:31-38). 5. Claim 1 of Ho teaches, in part, a self-emulsifying drug delivery composition for use with oral administration of fat-soluble drugs, said composition consisting essentially of: fat-soluble drug selected from the group consisting of tocotrienols, tocopherols ... an oil selected from the group consisting of palm olein and soy bean oil... a surfactant system comprised of a first component consisting of caprylocaproyl macrogolglycerides and a second component consisting of polyoxyethylene sorbitan monooleate (Ho 6:26-38). 6. Claim 3 of Ho teaches, in part, the “composition of claim 1, wherein the fat-soluble drug is about 24.8 weight percent of the composition” (Ho 6:46^17). 7. Ho teaches the studies had optimized three important formulation variables to achieve a superior product with enhanced bioavailability/absorption, namely (i) use of palm olein and soybean oil as the vehicle for fat-soluble drugs like tocotrienols, which help to enhance absorption; (ii) addition of a suitable combination of Labrasol and Tween 80 into the drug/oil mixture to promote self emulsification and thus help to further increase the absorption of tocotrienols; and (iii) a suitable combination of surfactant system (Labrasol and Tween 80) with the oil/drug mixture to optimize drug absorption. (Ho 2:28^10). 8. Lipari teaches “a drug-carrier system having a small-molecule drug of low water solubility in solution in a substantially non-aqueous 5 Appeal 2017-001371 Application 13/656,573 carrier that comprises (a) at least one phospholipid and (b) a pharmaceutically acceptable solubilizing agent. The drug-carrier system, when mixed with an aqueous phase, forms a non-gelling, substantially non transparent liquid dispersion” (Lipari ^ 15). 9. Lipari teaches the carrier comprises two essential components: at least one phospholipid, and a pharmaceutically acceptable solubilizing agent for the at least one phospholipid. The solubilizing agent, or the combination of solubilizing agent and phospholipid, also solubilizes the drug, although other carrier ingredients such as a surfactant optionally present in the carrier can in some circumstances provide enhanced solubilization of the drug. (Lipari ^ 79). 10. Lipari teaches in “one embodiment, the solubilizing agent comprises . . . one or more glyceride materials” (Lipari 82). 11. Lipari teaches a “suitable example of a medium chain triglyceride material is a caprylic/capric triglyceride product such as, for example, Captex 355 EP” (Lipari 86) (see Spec. ^ 42 “triglycerides of caprylic/capric acid sold as Captex® 355 and referred to herein as ‘Captex’ and C8/C10 polyglycolyzed glycerides from coconut oil sold as Labrasol® referred to herein as ‘LabrasoT were provided by BASF.”) 12. Lipari teaches a suitable total amount of glycerides is an amount effective to solubilize the phospholipid and, in combination with other components of the carrier, effective to maintain the drug in solution. For example, glyceride materials such as medium chain and/or long chain triglycerides can be present in a total glyceride amount of about 5% to about 70%. (Fipari 87). 6 Appeal 2017-001371 Application 13/656,573 13. Lipari teaches “to select a suitable surfactant for use in the composition ... a surfactant such as polysorbate 20 can be included in an amount of 0% to about 25%” (Lipari 88). 14. Lipari teaches the use of “Cremophor EL™ of BASF: polyoxyl castor oil” (Lipari 126) (see Spec. ^ 41 “self-emulsifying drug delivery system (SEDDS) formulations described in Table 1 below were prepared using Tween 80 or Cremophor EL as the primary surfactant”). 15. Lipari teaches the drug must normally be formulated at a concentration below its limit of solubility in the carrier. It will be understood that the limit of solubility can be temperature-dependent, thus selection of a suitable concentration should take into account the range of temperatures to which the composition is likely to be exposed. (Lipari ^ 77). Principles of Law “[WJhere the general conditions of a claim are disclosed in the prior art, it is not inventive to discover the optimum or workable ranges by routine experimentation.” In re Aller, 220 F.2d 454, 456 (CCPA 1955). “[T]he discovery of an optimum value of a variable in a known process is usually obvious.” Pfizer, Inc. v. Apotex, Inc., 480 F.3d 1348, 1368 (Fed. Cir. 2007). The rationale for determining the optimal parameters for prior art result effective variables “flows from the ‘normal desire of scientists or artisans to improve upon what is already generally known.’” Id. (quoting In re Peterson, 315 F.3d 1325, 1330 (Fed. Cir. 2003).) 7 Appeal 2017-001371 Application 13/656,573 Analysis We adopt the Examiner’s findings of fact and reasoning regarding the scope and content of the prior art (Ans. 2-8; FF 1-15) and agree that the claims are obvious over Ho and Fipari. We address Appellants’ arguments below. Appellants contend: the rejection should be overturned because, that rejection does not even allege that the proposed combination of prior art meets the claimed emulsification characteristics. Applicant anticipates that the present appeal may motivate a shift in the nature of the rejection including an argument that all of claimed emulsification characteristics are inherent in the combination of Ho ’306 and Fip[]ari ’780. However, that rejection is not the rejection being appealed. (App. Br. 11). We are not persuaded. Both Ho and Fipari are drawn to “a self- emulsifying drug delivery system” (FF 3; cf. FF 8), directly rebutting Appellants’ argument that the prior art fails to satisfy the recitation in claim 56 of a “self-emulsifying drug delivery system.” As Appellants acknowledge in their argument, Appellants show no evidence4 of a difference between the composition of claim 56 and the self-emulsifying systems rendered obvious by the combination of Ho and Fipari. Appellants contend there is “strong evidence rebutting the alleged expectation of success which remains the only evidence of record on that 4 We note Appellants’ citation of Gursoya et al, Self-emulsifying drug delivery systems (SEDDS) for improved oral delivery of lipophilic drugs, 58 Biomedicine & Pharmacotherapy 173 (2004)(Abstract), but this reference is newly cited and not admissible after appeal (see 37 CFR § 41.33(d)(2)). 8 Appeal 2017-001371 Application 13/656,573 issue” and the “record shows a series of prior attempts to create a Vitamin E SEDDS composition with high Vitamin E loading that were unsuccessful” (App. Br. 12). Appellants creates a table including data from Table 2 of Ali5 that shows certain formulations gave different degrees of turbidity, indicating various degrees of self-emulsification (App. Br. 14; cfi Ali 106, visual grading). We find this argument unpersuasive because there is no requirement that every possible composition functions, only that there is a reasonable expectation of success based on the teachings of the prior art. “Obviousness does not require absolute predictability of success ... all that is required is a reasonable expectation of success.'''’ In re Kubin, 561 F.3d 1351, 1360 (Fed. Cir. 2009). Here, Ho teaches a vitamin E formulation that self-emulsifies (FF 4), and Lipari provides extensive guidance on formulations that self- emulsify (see, e.g., Lipari 16-18, Table 1A). Moreover, it is unclear that Ali supports the position Appellants propound because it is unclear that Ali teaches any of the compositions of Table 2 fail to form a self-emulsifying system. Ali teaches: “Within these limits a homogenous transparent microemulsion pre-concentrate is produced. Outside these limits a non-homogenous product or a turbid microemulsion preconcentrate is formed” (Ali 105, col. 2). Thus, Ali is reasonably understood as teaching that there is a turbidity difference, but Ali never indicates that these compositions are not self-emulsifying. Indeed, Ali 5 Ali et al., Comparison between lipolysis and compendial dissolution as alternative techniques for the in vitro characterization of a-tocopherol self- emulsified drug delivery systems (SEDDS), 352 International J. Pharmaceutics 104-114 (2008). 9 Appeal 2017-001371 Application 13/656,573 teaches that formulation 8 that was graded as “milky” also had a Y4 value (percentage of vitamin E dissolved in the dissolution medium) of 91.85, very close to the 95.95 value for the translucent formula 1 (see Ali 106, table 2). Thus, to the extent that Ali shows differences in vitamin E dissolution for 25 different self-emulsifying compositions, that evidence supports the Examiner’s obviousness rejection because each of the 25 compositions was capable of self-emulsifying (see Ali 105, col. 2; “a turbid microemulsion preconcentrate is formed”). In addition, the efficacy differences between the 25 compositions is not relevant to claim 56, because claim 56 imposes no specific percentage of vitamin E that must be dissolved in the aqueous dissolution media after self-emulsification occurs. Appellants contend “there is some evidence that Examiner may beli[e]ve Claim 3 of Ho suggests higher concentrations of Vitamin E than otherwise described in Ho. Any indication that Claim 3 of Ho teaches a SEDDS having 24.8% Vitamin E is a direct contradiction of the teachings of Ho” (App. Br. 15; cf. Reply Br. 4). Appellants contend the “recited limitations of Claim 3 of Ho track the ‘final master formulation’ precisely down to the 10th of 1%. With Tocomin @50% being approximately 50% Vitamin E the percentage of Vitamin E claimed in Ho[.] Claim 3 is no different than the final master formulation, i.e. 12.4%” {id.). We are not persuaded because Ho teaches the amount of tocotrienols may be optimized, specifically teaching that one system “can incorporate a bigger amount of tocotrienols” “compared to the other two systems” (FF 7), reasonably suggesting the amount of vitamin E is a results-effective variable. Moreover, Lipari teaches that drug concentrations may be optimized and 10 Appeal 2017-001371 Application 13/656,573 teaches solubility and temperature are relevant to “selection of a suitable concentration” of active agent (FF 15). Finally, while we agree with Appellants that the master formulation appears to be the descriptive source of the 24.8% value in claim 3 of Ho, claim 3 broadly claims “wherein the fat-soluble drug is about 24.8 weight percent” (FF 6). Appellants provide no evidence that this statement is not enabled by Ho and it does represent a specifically described teaching of Ho. “[DJuring patent prosecution, an examiner is entitled to reject claims as anticipated by a prior art publication or patent without conducting an inquiry into whether or not that prior art reference is enabling. . . . [T]he burden shifts to the applicant to submit rebuttal evidence of nonenablement.” In re Antor Media Corp., 689 F.3d 1282, 1289 (Fed. Cir. 2012). Appellants have provided no evidence that the 24.8 weight percent value for fat-soluble drugs taught by Ho would not have been enabled by Ho. Appellants contend that a mere identification of a compound that can dissolve some quantity of Vitamin E among hundreds or thousands of similarly capable [compounds] is of very little help in a multivariate optimization that would be needed to achi[e]ve the Optimization Objective. Accordingly, a mere identification of a compound that can dissolve some quantity of Vitamin E does not make that compound a result effective variable. (App. Br. 17). Appellants further contend the Examiner has failed to establish Labrasol, Cremophor, Captex, or Ethanol as result effective variables (see App. Br. 18). We find this argument unpersuasive. Ho teaches testing “different surfactant systems at various ratio” (FF 3), and specifically teaches “studies optimized three important formulation variables” including vehicle 11 Appeal 2017-001371 Application 13/656,573 components, surfactant system, and combination of those components (FF 7). Lipari teaches to select “a suitable total amount of glycerides in an amount effective to solubilize the phospholipid” (FF 12) and teaches surfactant amounts can be selected within a range (FF 13). Moreover, Ali, a prior art reference cited by Appellants, demonstrates that the person of ordinary skill in the art, prior to the time of invention, would have known that “[ajmong the critical factors that are frequently considered for the optimal in vitro performance of SEDDS are the surfactant concentration, oil to surfactant ratio, triglyceride and co-solvent content, polarity of the emulsion, and droplet size” (Ali 104, col. 2). Ali further teaches “optimizing the ratio of primary and secondary surfactants, and oil are essential to produce SEDDS with desirable in vitro characteristics” (Ali 113, col. 1). Finally, Ali teaches “standard dissolution studies are suitable for optimizing SEDDS formulations and for identifying critical formulation variables” (Ali 113, col. 1). Thus, Ali evidences that the ordinary artisan would have had assays to optimize SEDDS formulations and would have optimized concentrations of components because these are critical formulation variables. Appellants provide no evidence that such optimization was anything other than routine. Appellants contend they “developed a new SEDDS with unprecedented vitamin E loading and shown it to have exceptional emulsification performance” (Reply Br. 2). We find this argument unpersuasive because Appellants identify no evidence supporting any unexpected results. See In re Soni, 54 F.3d 746, 750 (Fed. Cir. 1995) (“It is well settled that unexpected results must be 12 Appeal 2017-001371 Application 13/656,573 established by factual evidence. Mere argument or conclusory statements . . . [do] not suffice.”) Conclusion of Law The evidence of record supports the Examiner’s conclusion that Ho and Lipari render claim 56 obvious. SUMMARY In summary, we affirm the rejection of claim 56 under 35 U.S.C. § 103(a) as obvious over Ho and Lipari. Claims 57-75 fall with claim 56. No time period for taking any subsequent action in connection with this appeal may be extended under 37 C.F.R. § 1.136(a). AFFIRMED 13