2020005326 (P.T.A.B. Apr. 2, 2021)

George Shlieout et al.

Patent Trials and Appeals BoardApr 2, 2021

2020005326 (P.T.A.B. Apr. 2, 2021)

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. 11/464,704 08/15/2006 George Shlieout 032591-9007-01 (SPH0526) 9044 17567 7590 04/02/2021 (AbbVie) 1 North Waukegan Road North Chicago, IL 60064 EXAMINER ROSENTHAL, ANDREW S ART UNIT PAPER NUMBER 1613 NOTIFICATION DATE DELIVERY MODE 04/02/2021 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): abbvie_patents_abt_prk@abbvie.com PTOL-90A (Rev. 04/07) UNITED STATES PATENT AND TRADEMARK OFFICE BEFORE THE PATENT TRIAL AND APPEAL BOARD Ex parte GEORGE SHLIEOUT, CLAUS-JUERGEN KOELLN, FRITHJOF SCZESNY, JENS ONKEN, and GUIDO RUESING Appeal 2020-005326 Application 11/464,704 Technology Center 1600 Before DONALD E. ADAMS, RYAN H. FLAX, and RACHEL H. TOWNSEND, Administrative Patent Judges. TOWNSEND, Administrative Patent Judge. DECISION ON APPEAL Pursuant to 35 U.S.C. § 134(a), Appellant1 appeals from the Examiner’s decision to reject claims 77–82 and 84–15 directed to processes for the manufacture of pancreatin micropellet cores as being obvious. Oral argument was heard on March 23, 2021. We have jurisdiction under 35 U.S.C. § 6(b). We affirm. Our affirmance also includes new grounds of rejection. 1 We use the term “Appellant” to refer to “applicant” as defined in 37 C.F.R. § 1.42. Appellant identifies the real party in interest as AbbVie Pharmaceuticals GmbH. (Appeal Br. 1.) Appeal 2020-005326 Application 11/464,704 2 STATEMENT OF THE CASE “Pancreatin is a mixture of different physiologically active endogenous ingredients which are derived from mammalian pancreas glands and comprised of several different digestive enzymes such as lipases, amylases and proteases.” (Spec. 3:9–11.) “Pancreatin for pharmaceutical use is typically of bovine or porcine origin with porcine pancreatin being preferred.” (Id. at 3:14–15.) “Pancreatin microspheres are the treatment of choice for diseases or disorders caused by digestive enzyme deficiency in mammals such as humans.” (Id. at 1:13–14.) “This is due to the fact that high-performance pancreatin microsphere products . . . provide a therapeutically effective load of active enzymes while at the same time providing properly sized microspheres capable of targeting the optimal location in the digestive tract where digestive enzyme activity will be needed, in particular the upper intestine.” (Id. at 1:14–18.) According to Appellant’s Specification it “has previously been understood” with respect to “manufacturing pancreatin micropellet products by extrusion and subsequent spheronisation of the extrudates” that “synthetic oils like paraffins, e.g. liquid paraffins (mineral oils)[,] . . . [were] a necessary excipient.” (Id. at 1:27–30.) Appellant’s invention is directed to pancreatic micropellets that are enteric coated and are substantially free of synthetic oils. (Id. at 1:8–11, 2:18–20.) Claims 77, 82, 112, and 136, reproduced below, are illustrative of the claimed subject matter: 77. A pharmaceutical composition comprising: (a) a pancreatin core, wherein the core consists of: (i) 70% to 90% pancreatin; and Appeal 2020-005326 Application 11/464,704 3 (ii) 10% to 30% of at least one pharmaceutically acceptable binding agent, wherein the percentages of components are weight to weight of the core; and (b) an enteric coating on the core; wherein the pancreatin core and the enteric coating are substantially free of synthetic oils, and wherein at least 55% of lipase activity in the composition is released within 30 minutes in a buffer solution at pH 6 as measured according to United States Pharmacopoeia. 82. A delayed-release oral pharmaceutical composition comprising: (a) pancreatin micropellet cores comprising (i) pancreatin; and (ii) at least one pharmaceutically acceptable binding agent, wherein the cores are substantially free of synthetic oils; and (b) an enteric coating on the cores; wherein the enteric coating is substantially free of monomeric phthalic acid esters; wherein the composition has a relative gastric acid resistance of 75% or more following incubation for 2 hours in a phosphate buffer solution at pH 5; and wherein at least 65% of lipase activity in the enteric coated pancreatin micropellets is released in 30 minutes in a phosphate buffer solution at pH 6.0 at 37°C, in a dissolution apparatus, using a paddle speed of 50 rpm, following 2 hours incubation in a gastric juice without enzymes at 37°C, in a dissolution apparatus, using a speed of 100 rpm. 112. A delayed-release oral pharmaceutical composition comprising: (a) pancreatin micropellet cores comprising (i) one active pharmaceutical ingredient consisting essentially of pancreatin and (ii) at least one pharmaceutically acceptable binding agent, wherein the cores contain no more than a pharmaceutically acceptable trace amount of synthetic oils; and Appeal 2020-005326 Application 11/464,704 4 (b) an enteric coating on the cores; wherein the composition has a relative gastric acid resistance of 75% or more following incubation for 2 hours in a phosphate buffer solution at pH 5; and wherein at least 65% of lipase activity in the enteric coated pancreatin micropellets is released in 30 minutes in a phosphate buffer solution at pH 6.0 at 37°C, in a dissolution apparatus, using a paddle speed of 50 rpm, following 2 hours incubation in a gastric juice without enzymes at 37°C, in a dissolution apparatus, using a speed of 100 rpm. 136. A delayed-release oral pharmaceutical composition comprising: (a) pancreatin micropellet cores consisting essentially of pancreatin and one or more suitable pharmaceutically acceptable excipients, wherein at least one excipient is a pharmaceutically acceptable binding agent; and (b) an enteric coating on the cores; wherein the composition has a relative gastric acid resistance of 75% or more following incubation for 2 hours in a phosphate buffer solution at pH 5; and wherein at least 65% of lipase activity in the enteric coated pancreatin micropellets is released in 30 minutes in a phosphate buffer solution at pH 6.0 at 37°C, in a dissolution apparatus, using a paddle speed of 50 rpm, following 2 hours incubation in a gastric juice without enzymes at 37°C, in a dissolution apparatus, using a speed of 100 rpm. (Appeal Br. 36– 45 (V. Claims Appendix (emphasis added).) REFERENCES The prior art relied upon by the Examiner is: Name Reference Date Sander-Struckmeier US 7122357 B2 Oct. 17, 2006 Maio US 2004/0101562 A1 May 27, 2004 Appeal 2020-005326 Application 11/464,704 5 REJECTIONS We review the Examiner’s rejection of claims 77–82 and 84–159 under pre-AIA 35 U.S.C. § 103(a) as being unpatentable over Sander- Struckmeier and Maio. We however also institute the following new grounds of rejection, discussed in detail below: Claims 77–82 and 84–159 under 35 U.S.C. § 102(b) as being anticipated by Maio. Claims 77–82 and 84–135 as being indefinite under 35 U.S.C. § 112, second paragraph. OPINION I. Obviousness The Examiner finds that Sander-Struckmeier teaches forming microsphere cores of pancreatin and polyethylene glycol with propan-2-ol. (Final Action 8.) The Examiner further finds that “the mixture is extruded and rounded using liquid paraffin and propan-2-ol prior to drying” and that if any of the liquid paraffin, which was added after formation of the core, remains, it would be about 2% or less of the core material, assuming complete evaporation of the alcohol. (Id. at 8, 9.) The Examiner concludes that the 2% or less of the liquid paraffin that might remain in the core “qualifies as being a ‘trace’ amount or wherein the core is ‘substantially free’ of said oil.” (Id. at 9.) In addition, the Examiner concludes that because “Applicant has not provided what the basic and novel characteristics of ‘consisting essentially of’ exactly are . . . then oils in trace amounts are permitted to be present in the final composition of claim 136 even though Appeal 2020-005326 Application 11/464,704 6 synthetic oils are not, per se, a pharmaceutically acceptable excipient as defined by the Applicant in the specification at (pg 5, lns 18-19).” (Id.) The Examiner also finds that the core is taught to be enteric coated. (Id. at 8.) The Examiner acknowledges that Sander-Struckmeier does not explicitly teach the lipase activity and its release time, but concludes that because the “prior art teaches the identical chemical structure” claimed, the properties claimed “are necessarily present. In re Spada, 911 F.2d 705, 709 (Fed. Cir. 1990).” (Id. at 9.) The Examiner recognizes that “Sander-Struckmeier does not teach an enteric coating that is substantially free of monomeric phthalic acid esters” (Id. at 10). This is not a limitation of independent claims 77, 112, and 136. However, it is a limitation required by independent claim 82, and dependent claims 109 (depending from independent claim 77), 113 (depending from independent claim 112), and 137 (depending from independent claim 136)). The Examiner finds that replacing the enteric coating of Sander- Struckmeier with one that is substantially free of monomeric phthalic acid esters would have been obvious in light of the teachings of Maio. (Id.) The Examiner states that “Maio teaches pancreatin micropellets consisting of pancreatin and PEG4000 that are formed into spherical granules and coated with an enteric coating [0052–0053].” (Id.) The Examiner notes that the enteric coating taught “comprises HP-55 polymer, triethylcitrate, and talc and is completely free of monomeric phthalic acid esters.” (Id.) The Examiner concludes that substituting the coating of Maio for the coating of Sander-Struckmeier would have been obvious because, “[g]enerally, it is prima facie obvious to substitute one equivalent component or process for Appeal 2020-005326 Application 11/464,704 7 another, each of which is taught by the prior art to be useful for the same purpose (see MPEP 2144.06).” (Id.) Appellant disagrees with the Examiner’s position that about 2% liquid paraffin in the Sander-Struckmeier cores complies with the requirements of the independent claims, namely that the core be “substantially free of synthetic oils” or that it “contain[s] no more than a pharmaceutically acceptable trace amount of synthetic oils,” or “consist[] essentially of pancreatin and one or more suitable pharmaceutically acceptable excipients.” (Appeal Br. 10–12.) According to Appellant these phrases should be construed as requiring pancreatin core compositions “containing approximately 0% synthetic oils.” (Appeal Br. 23–25.) Appellant urges that its claim construction is consistent with the definition in the Specification as-filed. Appellant states “[t]he specification ‘repeatedly, consistently, and exclusively’ depicts the invention as eliminating the need for synthetic oils in pancreatin micropellet cores and/or pancreatin micropellets yet retaining their functions” and that the “specification has provided ample guidance to enable a person of ordinary skill to draw a line between synthetic oils being present in small amounts, e.g., as impurities in the starting materials, versus essential ingredients intentionally added in the pancreatin formulation. (Id. at 25.) In particular, Appellant argues that none of the exemplified compositions contain synthetic oil “as a necessary excipient,” but “the specification recognizes that the starting materials may contain small amounts of synthetic oils” and “thus the specification expressly characterizes synthetic oils as ‘pharmaceutically acceptable trace contaminants’” that may be present due to unavoidable impurities introduced into the formulation by the starting Appeal 2020-005326 Application 11/464,704 8 materials. (Id. at 25–26.) According to Appellant, “[t]he Examiner’s position requiring Appellant to specify a particular number as the cutoff between their invention and the prior art is improper and impractical.” (Id. at 26.) Appellant argues that the Examiner’s interpretation that 2% liquid paraffin of Sander-Struckmeier that was added purposefully during the process of making the core is inconsistent with the Specification’s definition of “substantially free of synthetic oils.” (Appeal Br. 16.) Appellant also argues that the Examiner’s claim interpretation is inconsistent with the Specification. In particular, Appellant argues that the Specification’s description of the primary purpose of the invention is “to provide patients with a pancreatin micropellet product in compliance with the current advice of the health authorities and which does not include synthetic oils such as mineral oil” like the prior art compositions of Boedecker/Sander- Struckmeier. (Appeal Br. 17–18). In addition, Appellant points out that the Specification describes “how to manufacture an extrudable mixture to form pancreatin micropellet cores even though the mixture is substantially free of synthetic oils” (id. at 17), and that all of its exemplified compositions “do not contain any synthetic oil as an added excipient” (id. at 16). Furthermore, Appellant argues that the testimony of Dr. Robert Joseph Kuhn, submitted in the Declaration dated September 16, 2019 (Kuhn Declaration), supports the conclusion that “one of ordinary skill in the art would not have considered the claimed pancreatin formulations with ‘no more than a pharmaceutically acceptable trace amount of synthetic oils’ to include Sander-Struckmeier’s composition which has about 2% liquid paraffin in the pancreatin cores.” (Id. at 19–20.) Appellant also argues that Appeal 2020-005326 Application 11/464,704 9 the Examiner’s conclusion improperly relied on “definitions of trace amounts from technological areas not remotely related to the claimed invention to form the claim interpretation.” (Id. at 20–22.) CLAIM CONSTRUCTION To resolve the foregoing dispute, we must construe certain claim terms; namely, the language in independent claims 77 and 82, respectively, “wherein the pancreatin core . . . [is] substantially free of synthetic oils” and “wherein the cores are substantially free of synthetic oils,” and in independent claim 112, “wherein the cores contain no more than a pharmaceutically acceptable trace amount of synthetic oils.” We apply the broadest reasonable interpretation standard to claims that are pending in an application. In this endeavor, to determine the interpretation that is reasonable in light of the record evidence and the understanding of one skilled in the art, we “consider the claims in light of the specification and teachings in the underlying patent.” In re Power Integration, Inc., 884 F.3d 1370, 1375 (Fed. Cir. 2018) (quoting In re CSB- Sys. Int’l, Inc., 832 F.3d 1335, 1341 (Fed. Cir. 2016)). A. “substantially free of synthetic oils” Appellant’s Specification defines the phrase “substantially free of synthetic oils” to mean: that the manufacturing processes described herein and used to make the pancreatin micropellet cores and/or pancreatin micropellets do not utilize one or more synthetic oils as an excipient although synthetic oils may be present as pharmaceutically acceptable trace contaminants in the pancreatin, binding agent(s), enteric coating constituents, the enzyme-friendly organic solvents and/or excipients which are used to manufacture the pancreatin micropellet cores and/or pancreatin micropellets described herein. Appeal 2020-005326 Application 11/464,704 10 (Spec. 4:6–12.) Rather than defining this quantitative term in measurable amounts, this definition speaks in terms of a processing activity, standing in stark contrast to the Specification definition of the phrase “substantially free of enzyme-friendly organic solvents,” which is defined to be “less than about 5% by weight of the pancreatin micropellet core.” (Spec. 6:12–14). Nevertheless, “we must respect this lexicographic choice” to define “substantially free of synthetic oils” in terms of a specific manufacturing process. Biogen MA, Inc. v EMD Serono, Inc., 976 F.3d 1326, 1336 (Fed. Cir. 2020); Edwards Lifesciences LLC v. Cook Inc., 582 F.3d 1322, 1329 (Fed. Cir. 2009) (“[W]e will adopt a definition that is different from the ordinary meaning when ‘the patentee acted as his own lexicographer and clearly set forth a definition of the disputed claim term in . . . the specification’.”). We note that the processing activity that reflects when the core is deemed to be substantially free of synthetic oils is “the manufacturing process described herein,” not any and all manufacturing processes, contrary to Appellant’s suggestion (Appeal Br. 16). In this regard, we note the manufacturing process described in Appellant’s Specification for making “uncoated pancreatin micropellet cores” that is an alleged “inventive” embodiment involves mixing pancreatin with PEG 4000 “in a commercially available high shear mixer and thoroughly moistened with . . . 2-propanolol. (Spec. 13:7–14.) The mixture is then “extruded by means of a commercially available extruding press” at a “temperature . . . less than 50 ºC while pressing.” (Id. at 13) The extrudate is cut and placed in “a Appeal 2020-005326 Application 11/464,704 11 commercially available rounding apparatus and rounded to give approximately elliptically or approximately spherically shaped micropellet cores” where additional 2-propanol is added while rounding. (Id. at 13:13–18.) We conclude that where a pancreatin core is made by some other process, Appellant’s definition provided in the Specification is not applicable.2 In such a case, we are left to ascertain from the remainder of the Specification what would reasonably be understood to be within the scope of “substantially free of synthetic oils.” In that regard, we disagree with Appellant that “containing approximately 0% synthetic oils” (Appeal Br. 23.) is the correct scope of the phrase. First, that Appellant’s examples of pancreatin cores made by the disclosed process do not identify any synthetic oils being present in any amount as an added excipient (Appeal Br. 17) does not require the upper limit of synthetic oils to be about 0% percent. “While a court may look to the specification and prosecution history to interpret what a patentee meant by a word or phrase in a claim, extraneous limitations cannot be read into the claims from the specification or prosecution history.” Bayer AG v. Biovail Corp., 279 F.3d 1340, 1348 (Fed. Cir. 2002). 2 We also do not find the Declaration testimony of Mr. Kuhn persuasive on whether the presence of 2% paraffin would be considered substantially free of synthetic oils. (Kuhn Declaration ¶ 11.) That is because Mr. Kuhn relies on the definition in the Specification which as we have discussed is limited to addition of synthetic oils in the processes disclosed in the Specification for making pancreatin micropellets. Appeal 2020-005326 Application 11/464,704 12 We note that nothing in the specific definition or the remaining description sets an upper quantitative limit for the amount of synthetic oils in the core to be deemed “substantially free” of synthetic oils. That is true despite the fact that amounts of liquid paraffin specifically added during a prior art extrusion process of making pancreatin micropellets are calculable. (See Kuhn Declaration ¶ 10.) The Specification explains regarding synthetic oils and the prior art that [t]he use of synthetic oils like paraffins, e.g. liquid paraffins (mineral oils), in particular highly liquid paraffin (light mineral oil) has previously been understood to be a necessary excipient for manufacturing pancreatin micropellet products by extrusion and subsequent spheronisation of the extrudates. (Spec. 1:27–30.) It is further noted, that governmental health authorities have recently recommended that “mineral oil not be provided indiscriminately to either pregnant women or infants.” (Id. at 1:19–23.) The Specification does not state what governmental health authorities recommend regarding amounts of synthetic oils such as mineral oil that are pharmaceutically acceptable as an excipient. Instead, it merely states governmental health authorities have initiated a reassessment of the compatibility of certain pharmaceutical excipients which had previously been used in the formulation of pancreatin- containing products and have provided advice concerning specific pharmaceutical excipients (see e.g. US Code of Federal Regulations, 21 CFR §201.302), such as mineral oil. It is recommended today that mineral oil not be provided indiscriminately to either pregnant women or infants. Appeal 2020-005326 Application 11/464,704 13 (Spec. 1:19–26.) We note that 21 C.F.R. § 201.302, which is concerned with labeling and misbranding, states with regard to studies about mineral oil use: studies have indicated that when mineral oil is used orally near mealtime it interferes with absorption from the digestive tract of provitamin A and the fat-soluble vitamins A, D, and K, and consequently interferes with the utilization of calcium and phosphorus, with the result that the user is left liable to deficiency diseases. When so used in pregnancy it predisposes to hemorrhagic disease of the newborn. 21 C.F.R. § 201.302(a). In addition the regulation states: There is accumulated evidence that the indiscriminate administration of mineral oil to infants may be followed by aspiration of the mineral oil and subsequent “lipoid pneumonia.” Id. at § 201.302(b). In light of the studies, the regulation provides that labeling should not encourage use of mineral oil during pregnancy or administration to infants and it should include a warning against consumption other than at bedtime and against administration to infants. Id. at § 201.302(c), (d). However, the regulation does not state what amount of mineral oil is outside of acceptable limits in drugs for internal use. Thus, the regulation referred to in the Specification does not provide any indication of a specific quantitative amount of a mineral oil that would not be acceptable to include in a composition intended for pharmaceutical use.3 And we cannot 3 For these reasons, the claim interpretation issue is not analogous to that in TF3 LTD. v. TreMilano LLC, 894 F.3d 1366 (Fed. Cir. 2018). (See Appeal Br. 14.) That is we do not have a situation in which the claims were interpreted by the Examiner “more broadly then the description in the Appeal 2020-005326 Application 11/464,704 14 conclude from any of this that there is a governmental recommendation that no amount of mineral oil or other synthetics oils are pharmaceutically acceptable in a pancreatin composition. That the FDA may now require a warning with respect to pregnant patients or infants be provided on formulations that include an amount of mineral acid, but does not require removal of prior formulations from the market, does not mean that the amounts of mineral oil present in the marketed formulations are not pharmaceutically acceptable. According to Appellant, “it is clear from the as-filed [S]pecification that the pancreatin micropellets of the claimed invention were improvements of pancreatin compositions that were available in the art and contained synthetic oil, specifically the pancreatin compositions of Boedecker [which are the same as Sander- Struckmeier].” (Appeal Br. 18.) Even if true, Appellant’s claim language does not require that synthetic oils be completely absent, just that it be “substantially free from” such oils. And, even Appellant’s explicit definition of “substantially free from synthetic oils,” which is tied to the process of manufacture disclosed in the Specification, states that synthetic oils “may be present” as pharmaceutically acceptable trace contaminants, even though synthetic oils “are not to be regarded as” “suitable pharmaceutically acceptable binding agents” (Spec. 5:6–7), “suitable pharmaceutically acceptable excipients” (Spec. 5:8) “suitable enzyme-friendly organic solvents” (Spec. 5:34). Thus, we do not conclude from Appellant’s Specification that specification.” (Id. (citing TF3 LTD. v. TreMilano LLC, 894 F.3d at 1372– 73)). Appeal 2020-005326 Application 11/464,704 15 “substantially free from synthetic oils” means approximately 0% synthetic oils. Furthermore, that Appellant intended to pursue patent protection for a composition that is different from the prior art does not require that we construe the phrase “substantially free from synthetic oils” to not include formulations that have 2% mineral acid associated with the pancreatin core. If such a precise limitation were desired, Appellant could have drafted a claim reciting “less than about 2% synthetic oils.” We do not find compelling Appellant’s argument that the rationale in In re Marosi, 710 F.2d 799 (Fed. Cir. 1983) should apply to the claim construction at issue here. (Appeal Br. 24–25.) First, unlike in Marosi, Appellant’s claims are not directed to what was found surprising to the inventors, i.e., making a pancreatin composition using an extrusion process where synthetic oils need not be added to the mixture that is to be extruded or in the rounding of the cut extrudate. In particular, Appellant’s Specification states: It has now been surprisingly found that pancreatin micropellet cores which are suitable for enteric coating, are high in enzymatic activity and are substantially free of synthetic oils like paraffins, e.g. highly liquid paraffin, can be produced by the processes described herein. It has further been found that the manufacturing process described herein is an improvement when compared to known processes which use mineral oil or known processes which would e.g. need more process steps to produce pancreatin micropellet cores. (Spec. 3:16–22 (emphases added).) In addition, the Specification states: Appeal 2020-005326 Application 11/464,704 16 In one embodiment, the pancreatin micropellet cores are created in process step b.) by extrusion. Remarkably, an extrudable mixture is obtained even though the mixture is substantially free of synthetic oils. (Spec. 6:24–26.) The Specification continues noting: [T]hen the extrudate fragments are brought to a suitable length for the forming step. This can be done e.g. by means of a cutting device arranged downstream to the extruding press in a manner known to the a person of ordinary skill in the art. The forming in process step c.) can be carried out e.g. in a customary rounding apparatus. In the rounding apparatus, the extrudate fragments are then formed into an approximately spherical or approximately ellipsoidal shape in the presence of additional enzyme-friendly organic solvent which may be the same or different than the enzyme-friendly organic solvent used in process step a). (Spec. 6:33–7:2.) The Specification explains with respect to the processing in the rounding apparatus that the processing is improved relative to other known processes. For example, a lower amount of enzyme-friendly organic solvent needs to be added when forming the pancreatin micropellet cores into an approximately spherical or approximately ellipsoidal shape and fewer of the extrudate fragments stick to parts of the rounding apparatus when the process is practiced with an extruder and rounding apparatus. (Id. at 7:4–9.) The Specification states that “the pancreatin micropellet cores and the pancreatin micropellets produced according to the processes disclosed herein and not using synthetic oils unexpectedly show essentially the same properties as pancreatin micropellet cores and micropellets produced according to known processes using mineral oil such as the processes disclosed in U.S. Patent No. 5,378,462.” (Id. at 7:17–21 (emphasis added).) Appeal 2020-005326 Application 11/464,704 17 However, the claims on appeal are not directed to a process of manufacturing a pancreatin micropellet, much less one described in the Specification, nor is the product claimed directed to a product made by the disclosed process. Cf. Marosi, 710 F.3d at 800, 802–03 (noting that the claims were directed to a process (or product-by- process) that did not require use of alkali metal in synthesizing a particular type of zeolite structure: “[W]e note that appellants’ invention, simply put, is the discovery that zeolites may be synthesized without the presence in the reaction mixture of alkali metal.”). Thus, we do not have claims requiring “the practical elimination” of an essential ingredient. Id. As such, and unlike the claims presented in In re Marosi, whether or not a person could “draw a line between unavoidable impurities in starting materials and essential ingredients” in a manufacturing process to make pancreatin cores or compositions does not control the claim interpretation here. Marosi, 710 F.2d at 803. We do note, however, the Specification provides some indication that the phrase “substantially free” with respect to amounts by weight of a composition can include amounts in excess of 2%. In particular, as we noted above, the Specification defines the term “substantially free of enzyme-friendly organic solvents” to “mean[] that the quantity of enzyme-friendly organic solvents present in the pancreatin micropellet cores would be less than about 5% by weight of the pancreatin micropellet core.” (Spec. 6:12–14.) We conclude that a composition that includes 2% by weight of synthetic oils may be deemed to be “substantially free of synthetic Appeal 2020-005326 Application 11/464,704 18 oils” provided that the remaining limitations of the claim are met. Thus, with respect to claim 77, if a composition had a pancreatin core that only “consists of” pancreatin4 and pharmaceutically acceptable binding agents (which Appellant’s Specification defines synthetic oils to not be (Spec. 5)), then we would find such a composition to be substantially free of synthetic oils. And with respect to claim 82, if a composition had a pancreatin core that “comprises” pancreatin and pharmaceutically acceptable binding agents and synthetic oils are present, then we would find such a composition to be substantially free of synthetic oils. B. “contain[s] no more than a pharmaceutically acceptable trace amount of synthetic oils” Appellant contends that this phrase is interchangeable with substantially free of synthetic oil and should be interpreted to mean approximately 0% of synthetic oils for the same reasons. (Appeal Br. 23 n. 6.) While we agree with Appellant that the phrases can have the same meaning, just as we do not find support in the Specification for construing substantially free as meaning approximately 0% of synthetic oils, we do not find support in the Specification for construing the trace amount phrase in this way. The Specification does not define the phrase “pharmaceutically acceptable trace amount.” And as discussed above, we do not find the reference to regulatory reassessment of labeling drugs with mineral oil as an 4 Appellant’s Specification teaches that pancreatin “is a mixture of different physiologically active endogenous ingredients which are derived from mammalian pancreas glands.” (Spec. 3.) Appeal 2020-005326 Application 11/464,704 19 excipient to provide an indication that mineral oils should be present in pancreatin products at close to 0%. Appellant further points to the Declaration testimony of Mr. Kuhn to argue that “one of ordinary skill in the art would not consider 2% paraffin, as described in Sander-Struckmeier, as a pharmaceutically acceptable trace amount of synthetic oil, nor would it be a suitable pharmaceutically acceptable excipient.” (Appeal Br. 20.) In arriving at his conclusion, Mr. Kuhn contends that 2% paraffin would not be considered to be such an amount in light of the fact that Appellant’s Specification “indicates the certain excipients that have been used in the formulation of pancreatin containing products, such as mineral oil, should be reassessed. (Specification at para. 4.).” (Kuhn Declaration ¶ 12.) Mr. Kuhn also considered that EPI treatment requires chronic intake of pancreatin products, and 2% of paraffin in a product “would cause cumulative toxicity that would not be pharmaceutically acceptable” given patients who suffer EPI from birth, and take pancreatin products “three to five times a day, two or more capsules each time in order to receive nourishment from their food.” (Kuhn Declaration ¶ 13.) Mr. Kuhn states: “In view of the context of this chronic application, small amounts of synthetic oil administered over a long period of time would not be pharmaceutically acceptable.” (Id.) We do not find Mr. Kuhn’s testimony persuasive because, as discussed above, Appellant’s Specification does not indicate any particular level of mineral oil that must be avoided generally, or by Appeal 2020-005326 Application 11/464,704 20 pregnant women specifically. And as we discussed above, the FDA regulation referenced does not provide such information either. Moreover, Appellant’s Specification does not state that the prior art formulations that include mineral oils have been required to be removed from the market. Thus, Mr. Kuhn’s conclusion as to why 2% mineral oil would not be considered a pharmaceutically acceptable trace amount is unsupported by an evidentiary foundation and we decline to give it persuasive weight. See Perreira v. Secretary of the Dept. of HHS, 33 F.3d 1375, 1377 (Fed. Cir. 1994) (“An expert opinion is no better than the soundness of the reasons supporting it.”); In re Beattie, 974 F.2d 1309, 1313 (Fed. Cir. 1992) (opinion evidence in declarations has little value without factual support); Velander v. Garner, 348 F.3d 1359, 1371 (Fed. Cir. 2003) (“The Board has broad discretion as to the weight to give to declarations offered in the course of prosecution.”). In light of the fact that there is no evidence indicating prior art pancreatin products having mineral oil in measurable quantities have been required to be withdrawn from the market, we conclude that the phrase “pharmaceutically acceptable trace amount” includes amounts of mineral oil that were extant in commercially available prior art pancreatin compositions. Does the Sander-Struckmeier Pancreatin Core Read on the Claimed Pancreatin Core? The Examiner and Appellant are in agreement that Sander- Struckmeier teaches inclusion of about 2% liquid paraffin (mineral oil) in the preparation of the pancreatin core. The Examiner contends Appeal 2020-005326 Application 11/464,704 21 that this 2% meets the substantially free of, or trace amount requirements of claims 77, 82, and 112. (Final Action 9.) And the Examiner contends that because Appellant has not provided what the basic and novel characteristics of the pancreatin core is, and the pharmaceutical composition claimed by Appellant in claim 136 is said to comprise the core and enteric coating on the core, the oil added during spherical shaping that may remain on the core that is dried and in the final composition that is enterically coated of Sander- Struckmeier meets the limitations of claim 136. (Final Action 9.) Appellant argues that because the paraffin is intentionally added as an excipient in Sander-Struckmeier and “is present in the formulation in an amount that is required to perform its intended function,” it is erroneous to consider the core of Sander-Struckmeier to meet the limitations of claims 77, 82, 112, and 136. (Appeal Br. 18, 19, 11–12.) A. Claim 77 We think the Appellant has the better argument with respect to claim 77. “[C]losed transition phrases such as ‘consisting of’ are understood to exclude any elements, steps, or ingredients not specified in the claim.” AFG Indus., Inc. v. Cardinal IG Co., 239 F.3d 1239, 1245 (Fed. Cir. 2001). The claim requires that the pancreatin core “consists of” pancreatin and at least one pharmaceutically acceptable binding agent and the Specification states that the mineral oils are not to be considered as such a binding agent. We do not find that the paraffin oil (“liquid paraffin”) in Sander-Struckmeier is added as a binding Appeal 2020-005326 Application 11/464,704 22 agent. That is because it is added after the core is extruded and cut, but before rounding, as an aid in spheronization. (Sander-Struckmeier 10:39–51.) Consequently, we do not agree with the Examiner that Sander-Struckmeier discloses the pancreatin core of claim 77. B. Claim 82 We think the Examiner has the better argument with respect to claim 82 because that claim indicates the pancreatin core is one “comprising” pancreatin and at least one pharmaceutically acceptable binding agent. “‘Comprising’ is a term of art used in claim language which means that the named elements are essential, but other elements may be added and still form a construct within the scope of the claim.” Genentech, Inc. v. Chiron Corp., 112 F.3d 495, 501 (Fed. Cir. 1997). Thus, here, the core is permitted to include other elements besides pancreatin and binding agents, and as noted above, the liquid paraffin is added after the core is extruded and cut, but before rounding, as an aid in spheronization (Sander-Struckmeier 10:39–51). Thus, the liquid paraffin is not provided to the core as a binding agent. Although claim 82 also requires that the core be “substantially free of synthetic oils,” for the reasons discussed above in the claim construction, we conclude that having 2% paraffin oil is within the scope of that limitation. The fact that the paraffin oil is intentionally added during the process of rounding the compressed extrudated core material does not require a different conclusion. The intent for which an ingredient is added to a composition does not change its character as an ingredient in the composition as claimed. “[A] claimed product shown to be present in the prior art cannot be rendered patentable Appeal 2020-005326 Application 11/464,704 23 solely by the addition of source or process limitations.” Amgen, Inc. v. Hoechst Marion Roussel, Inc., 314 F.3d 1313, 1354 n.20 (Fed. Cir. 2003). C. Claim 112 As with claim 82, we find the Examiner has the better argument with respect to claim 112. Like claim 82, claim 112 recites the “pancreatin micropellet cores comprising,” which allows for other elements besides those recited to be added and still form a construct within the scope of the claim. Genentech, 112 F.3d at 501. Moreover, for the reasons discussed above in the claim construction section, we conclude that having 2% paraffin oil is within the scope of “no more than a pharmaceutically acceptable trace amount,” even though mineral oil is intentionally added during the process of rounding the compressed extrudated core material. D. Claim 136 We also find the Examiner has the better argument with respect to claim 136. Use of “consisting essentially of” language “opens the claims to the inclusion of ingredients which would not materially affect the basic and novel characteristics of appellant’s compositions as defined in the balance of the claim.” In re Janakirama-Rao, 317 F.2d 951, 954 (CCPA 1963). According to Appellant, the basic and novel characteristic of the composition is that it be substantially free of synthetic oil and yet retain the therapeutic effectiveness. (Appeal Br. 12 n 2.) Not having a particular ingredient is not an appropriate “characteristic” in the consisting essentially of assessment. Id. at 953–954 (“Certainly no characteristics whatever are set forth in the Appeal 2020-005326 Application 11/464,704 24 claims, unless it be in the word ‘optical,’ which modifies ‘glass. . . . But no basic or novel characteristic to be so affected can be deduced from the disclosure and none was shown in brief or argument. We therefore find that the board was correct in holding that there is no showing of properties patentably distinguishing appellant’s claimed glasses from those of the reference.’”). The question is whether the 2% synthetic oil amount which becomes part of the Sander- Struckmeier pancreatin core on rounding of the extrudate materially affects the fundamental character, i.e. properties, of that pancreatin core. Appellant’s evidence demonstrating that the core can be adequately enterically coated with or without synthetic oils present and the core is therapeutically active with or without the synthetic oils present (Appeal Br. 27, 29, 31) seems to us to be compelling evidence that the fundamental character of the pancreatin core is not altered by the presence of 2% synthetic oil being present on the spheronized core in the Sander-Struckmeier example. Unexpected Results As noted above, the Examiner’s position with respect to obviousness is only relevant to those claims that recite enteric coatings that are substantially free of monomeric phthalic acid esters because that is the limitation that the Examiner asserts is not disclosed by Sander-Struckmeier. This is a limitation required by independent claim 82, dependent claims 109 (depending from independent claim 77), 113 (depending from independent claim 112), and 137 (depending from independent claim 136)). It is not a Appeal 2020-005326 Application 11/464,704 25 limitation of independent claims 112, and 136. Thus, we understand the Examiner’s rejection of claims 77, 112, and 136 to be one of anticipation. As we noted above, we do not agree with the Examiner that Sander- Struckmeier discloses a composition that meets the limitations of claim 77. However, such is not true with respect to claims 112 and 136. Appellant’s reliance on unexpected results to establish patentability of these claims that are anticipated by Sander-Struckmeier is not persuasive. Evidence of secondary considerations, such as unexpected results, cannot overcome a rejection based on anticipation. In re Wiggins, 488 F.2d 538, 543 (CCPA 1973). Consequently, we need not consider Appellant’s arguments regarding unexpected results as to claims 112 and 136. “It is well settled that ‘anticipation is the epitome of obviousness.’” In re McDaniel, 293 F.3d 1379, 1385 (Fed. Cir. 2002) (quoting Connell v. Sears, Roebuck & Co., 722 F.2d 1542, 1548 (Fed. Cir. 1983)). And thus, we affirm the Examiner’s rejection of claims 112 and 136 as being anticipated by Sander-Struckmeier. Regarding claim 82, we note that Appellant’s argument with respect to unexpected results is directed to the absence of synthetic oils, not to the elements of the enteric coating, much less that of it being free of monomeric phthalic acid esters. (Appeal Br. 29, Kuhn Declaration ¶ 20.) However, as we noted above claim 82 does not require about 0% synthetic oils. This is true with respect to claims 113 and 137, as well. Consequently, we do not find Appellant’s evidence of unexpected results to establish non-obviousness over Sander-Struckmeier and Maio persuasive. Thus, we affirm the Examiner’s rejection of claims 82, 113, and 137 as being obvious from Sander-Struckmeier and Maio. Appeal 2020-005326 Application 11/464,704 26 Appellant does not separately argue the dependent claims. Thus, we affirm the Examiner’s rejections as to the obviousness over Sander- Struckmeier and Maio of claims dependent from claims 82, 112, and 136 and not already discussed. 37 C.F.R. § 41.37(c)(1)(iv). II. Anticipation by Maio The Examiner identified paragraphs 52 and 53 as being relevant to the claims on appeal. We agree but note that Maio is more relevant to the claims on appeal than merely for what the Examiner cited the reference as teaching. In particular, Maio’s paragraph 52 teaches pancreatin pellets that were made by direct spheronization of pancreatin and PEG4000. Paragraph 53 explains that those spherical pellets are coated with HP-55, triethylcitrate and talc, which is an enteric coating. Maio’s process described in paragraphs 52 and 53 for creating the pancreatin micropellets and providing an enteric coating thereon does not use mineral oils. Appellant’s Specification states that it was remarkable that an “extrudable mixture is obtained even though the mixture is substantially free of synthetic oils.” (Spec. 6:25–26.) However, Appellant’s claims are directed to compositions not the method by which they are made. And, Maio teaches pancreatin - PEG 4000 pellet compositions that are subsequently enterically coated and are made without the use of synthetic oils. Thus, the Maio composition also meets the “substantially free of synthetic oils” limitations of claims 77 and 82, as well as meeting the “cores contain no more than a pharmaceutically acceptable trace amount of synthetic oils” of claim 112, and pancreatin micropellet cores consisting Appeal 2020-005326 Application 11/464,704 27 essentially of pancreatin and one or more suitable pharmaceutically acceptable excipients” of claim 136. In light of this, the claimed composition has not been shown to be “remarkable” over the prior art. As the Examiner indicated in the statement of rejection (Final Action 9), where the chemical composition claimed is taught by the prior art, one of ordinary skill in the art has reason to conclude that the properties recited by the claim are also necessarily achieved. In re Spada, 911 F.2d 705, 709 (Fed. Cir. 1990) (“When the claimed compositions are not novel they are not rendered patentable by recitation of properties, whether or not these properties are shown or suggested in the prior art.”); In re Best, 562 F.2d 1252, 1254 (CCPA 1977) (“‘[I]t is elementary that the mere recitation of a newly discovered function or property, inherently possessed by things in the prior art, does not cause a claim drawn to those things to distinguish over the prior art.”). We conclude that the enterically coated pancreatin pellets taught in Maio’s example 4 anticipate the compositional elements required by claims 77, 82, 112, and 136, and that they necessarily have the release characteristics claimed. This rejection applies to the dependent claims on appeal as well given that Maio teaches these pellets are microspheres. (Maio ¶ 42) Although Maio, and the primary paragraphs we rely on now, were before Appellant during prosecution, the thrust of the Examiner’s rejection is different from what we set forth now. Thus, we designate this rejection as a new ground of rejection. Appeal 2020-005326 Application 11/464,704 28 III. Indefiniteness A claim is properly rejected as indefinite under 35 U.S.C. § 112, second paragraph, if, after applying the broadest reasonable interpretation in light of the specification, the metes and bounds of a claim are not clear because the claim “contains words or phrases whose meaning is unclear.” In re Packard, 751 F.3d 1307, 1310, 1314 (Fed. Cir. 2014) (per curiam) (approving, for pre-issuance claims, the standard from MPEP § 2173.05(e)); see also Ex parte McAward, Appeal 2015-006416, 2017 WL 3669566, at *5 (PTAB Aug. 25, 2017) (precedential)(adopting the approach for assessing indefiniteness approved by the Federal Circuit in Packard). Further, claims, when read in light of the specification, must “reasonably apprise those skilled in the art both of the utilization and scope of the invention” using language “as precise as the subject matter permits.” Packard, 751 F.3d at 1313. As discussed in the claim construction section above, Claim 112 recites that the cores contain “no more than a pharmaceutically acceptable trace amount of synthetic oils.” We determine that it is not reasonably possible to interpret this claim and dependent claims thereon with sufficient clarity to satisfy 35 U.S.C. § 112, second paragraph. See In re Packard, 751 F.3d 1307, 1313 (Fed. Cir. 2014) (per curiam). Appellant’s arguments on appeal suggest that there is no universality regarding synthetic oils as to what is pharmaceutically acceptable, whether that be with respect to time or geographic location. The Specification does not provide a standard by which one is to determine pharmaceutical acceptance. Accordingly, we enter a new ground of rejection as to claim 112 and claims dependent thereon. Moreover, to the extent that Appellant has argued substantially free Appeal 2020-005326 Application 11/464,704 29 of synthetic oils is equivalent to the meaning of pharmaceutically acceptable trace amount of synthetic oils (Appeal Br. 12, n. 3), we enter a new ground of rejection as to claims 77 and 82 and claims dependent thereon. DECISION SUMMARY Claim(s) Rejected 35 U.S.C. § Reference(s)/Basis Affirmed Reversed New Grounds 77–82, 84–159 103 Sander- Struckmeier, Maio 78–82, 84–103, 106, 107, 112–159 77–81, 104, 105, 108, 109, 110, 111 77–82, 84–159 102 Maio 77–82, 84–159 77–82, 84–135 112, second paragraph 77–82, 84–135 Overall Outcome 78–82, 84–103, 106, 107, 112–159 77–82, 84–159 TIME PERIOD FOR RESPONSE This decision contains a new ground of rejection pursuant to 37 C.F.R. § 41.50(b). 37 C.F.R. § 41.50(b) provides “[a] new ground of rejection pursuant to this paragraph shall not be considered final for judicial review.” 37 C.F.R. § 41.50(b) also provides that the Appellant, WITHIN TWO MONTHS FROM THE DATE OF THE DECISION, must exercise one of the following two options with respect to the new ground of rejection to avoid termination of the appeal as to the rejected claims: Appeal 2020-005326 Application 11/464,704 30 (1) Reopen prosecution. Submit an appropriate amendment of the claims so rejected or new Evidence relating to the claims so rejected, or both, and have the matter reconsidered by the examiner, in which event the prosecution will be remanded to the examiner. . . . (2) Request rehearing. Request that the proceeding be reheard under § 41.52 by the Board upon the same Record. . . . Further guidance on responding to a new ground of rejection can be found in the Manual of Patent Examining Procedure § 1214.01. Affirmed; 37 C.F.R. 41.50(b)