15226126 - (D) (P.T.A.B. Oct. 27, 2020)

immatics biotechnologies GmbH

Patent Trials and Appeals BoardOct 27, 2020

15226126 - (D) (P.T.A.B. Oct. 27, 2020)

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. 15/226,126 08/02/2016 Toni WEINSCHENK 2912919-018008 3220 84331 7590 10/27/2020 McBee Moore & Vanik, IP, LLC 7900 Westpark Drive, Suite A100 McLean, VA 22102 EXAMINER RAWLINGS, STEPHEN L ART UNIT PAPER NUMBER 1643 NOTIFICATION DATE DELIVERY MODE 10/27/2020 ELECTRONIC Please find below and/or attached an Office communication concerning this application or proceeding. The time period for reply, if any, is set in the attached communication. Notice of the Office communication was sent electronically on above-indicated "Notification Date" to the following e-mail address(es): docketing@mmviplaw.com eofficeaction@appcoll.com smcbee@mmviplaw.com PTOL-90A (Rev. 04/07) UNITED STATES PATENT AND TRADEMARK OFFICE __________ BEFORE THE PATENT TRIAL AND APPEAL BOARD __________ Ex parte TONI WEINSCHENK, OLIVER SCHOOR, CLAUDIA TRAUTWEIN, NORBERT HILF, STEFFEN WALTER, and HARPREET SINGH __________ Appeal 2020-000111 Application1 15/226,126 Technology Center 1600 __________ Before RICHARD M. LEBOVITZ, RYAN H. FLAX, and RACHEL H. TOWNSEND, Administrative Patent Judges. TOWNSEND, Administrative Patent Judge. DECISION ON APPEAL This is an appeal under 35 U.S.C. § 134(a) involving claims to a pharmaceutically acceptable salt of a particular peptide sequence, and a fusion protein, which have been rejected as directed to patent-ineligible subject matter, and/or as being indefinite and for obviousness-type double patenting. We have jurisdiction under 35 U.S.C. § 6(b). 1 We use the word “Appellant” to refer to “applicant” as defined in 37 C.F.R. § 1.42. Appellant identifies the real party in interest as Immatics Biotechnologies GmbH. (Appeal Br. 1.) Appeal 2020-000111 Application 15/226,126 2 We reverse the rejection for patent-ineligible subject matter, but affirm the obviousness-type double patenting rejection which was not challenged on appeal. STATEMENT OF THE CASE Claims 1–4, 7, 9–14, and 21–27 are on appeal. Claim 1 is representative and reads as follows: 1. A peptide consisting of the amino acid sequence of GLWHHQTEV (SEQ ID NO: 21) in the form of a pharmaceutically acceptable salt, wherein said peptide is produced by solid phase peptide synthesis or produced by a yeast cell or bacterial cell expression system. (Appeal Br. 48.) The following grounds of rejection by the Examiner are before us on review: Claims 1, 3, 4, 9–14, and 21–26 under 35 U.S.C. § 101 as being directed to patent-ineligible subject matter.2 Claims 1, 3, 4, 9–14, and 21–27 on the ground of nonstatutory obviousness-type double patenting as being unpatentable over claims 1–16 of U.S. Patent No. 9,289,478. 2 In the Final Rejection the Examiner rejected claims 1–4, 7, 9–14, and 21– 26. In the Answer, the Examiner withdrew the rejection as applied to claims 2 and 7. The Examiner also withdrew the rejection of claims 2 and 7 under 35 U.S.C. §112(b) as being indefinite. Appeal 2020-000111 Application 15/226,126 3 DISCUSSION I I. Patent Eligible Subject Matter The Dispute The Examiner finds that claim 1 is directed to a judicial exception, “namely, a peptide or a composition comprising a peptide in which the peptide is not markedly different from a naturally occurring peptide, such that claimed invention is distinguished from the naturally occurring product.” (Final Action 2–3, 7.) The Examiner states: the derivation of a salt of the peptide does not create a marked difference between the claimed invention and the naturally occurring peptide. This is especially true since upon dissolution of the salt the peptide [] is present in solution as it exists in nature. Similarly it is submitted that the acylation or pegylation of the peptide or its linkage to a solid resin does not substantially alter its structure by creating a marked and significant difference between it and its naturally occurring counterpart. (Id. at 3.) The Examiner indicates that formation of a salt, or acylating a peptide, may be analogized to putting a scarf around a snowman, in that the addition of the scarf does not change the structure of the underlying snowman. (Id. at 9–10.) The Examiner indicates that just as the snowman structure is the same when the scarf is removed, the removal of the salt group from the peptide when placed in solution results in a peptide being “essentially the same as it was before the salt was formed,” i.e., “its structure has not been markedly altered.” (Id. at 10; Ans. 7.) Regarding the requirement in claim 9 that the peptide is acylated, the Examiner further states: Appeal 2020-000111 Application 15/226,126 4 while it is appreciated that acylation of peptides has been understood to alter the functional properties of the peptides, as well as their structures, acylation is not necessarily evidence of a transformation at the "hands-of-man", which distinguishes the acylated peptide from its naturally occurring counterpart. (Ans. 18.) The Examiner also finds that because prior art teaches that some naturally occurring proteins have been found to be acylated and bound to HLA class I in vivo, and that a large percentage “of all proteins [in humans] receive an acetyl group at their N-terminus” that the claimed acylated peptide consisting of the amino acid sequence of SEQ ID NO: 21 “is certainly not distinguished from its natural counterpart,” though “[i]t is however not known.” (Id. at 18–19.) Regarding the requirement in claim 10 that the peptide is pegylated, the Examiner further finds that the claim scope includes “non-covalent pegylation” and such pegylation “does not alter the structure of the peptide, at least not such that the reversal of the process cannot restore the peptide as it originally occurred; and moreover, once such a peptide is released from PEG, its biologic properties are unchanged.” (Id. at 20.) In addition, the Examiner finds that, even as to covalent attachment, although such a structure “is not naturally occurring” (id. at 21), “the difference is merely the result of routine and conventional modification of the naturally occurring peptide of the same amino acid sequence,” which “is not regarded as being a ‘marked’ difference” (id. at 20). “[T]he difference is not such that the claimed invention has been transformed into a new and useful product having a function that is significantly different from that of the naturally occurring peptide of the same amino acid sequence.” (Id. at 21.) Appellant argues that “the proper analysis for step 2A [in considering patent-eligibility] is to look at what is claimed and determine whether it has Appeal 2020-000111 Application 15/226,126 5 an identical natural counterpart. If an identical counterpart to what is claimed does not exist, that is the end of the analysis.” (Appeal Br. 14 (emphasis omitted).) Appellant points out that “there is no naturally occurring peptide of SEQ ID No: 21 either in free form or in the form of a pharmaceutically acceptable salt” and, therefore, “it is impossible for the claims to be ‘directed’ to a judicial exception.” (Id. at 15.) Appellant argues that it is an improper analysis under § 101 to “parse[] [the claim] into i) the 9-amino acid and ii) a salt.” (Id. at 17.) Appellant explains that [a]n amino acid sequence having SEQ ID NO: 21 is either found within a hydrophobic internal domain of a 1211 amino acid NRCAM protein, or a peptide having SEQ ID NO: 21 is found associated with an MHC-1 molecule on the surface of antigen presenting cells. (Id. at 17–18.) Undergirding Appellant’s argument is the testimony of Dr. Lawrence Stern. (Id. at 20–24 (citing Stern Declaration3).) Appellant further explains, with support from the testimony of Dr. Stern, that the claimed peptide salt is markedly different from how the peptide having the amino acid sequence of SEQ ID NO: 21 is found in nature, i.e., “either within a twisted beta-strand domain of the NRCAM protein or associated with an MHC-I molecule.” (Id. at 25–29.) In addition, Appellant explains, with support from the testimony of Dr. Stern, that even assuming a free peptide of SEQ ID NO: 21 exists in nature, the claimed pharmaceutically acceptable salt is structurally and functionally different from such a free peptide. (Id. at 29–30.) 3 Declaration of Dr. Lawrence Stern, dated May 16, 2018 (“Stern Declaration”). Appeal 2020-000111 Application 15/226,126 6 Appellant argues that the Examiner “offered no evidence rebutting any of Dr. Stern’s factual statements” or the “literature-based factual evidence” in support thereof, and instead maintained the rejection of ineligibility only on an analogy to dressing a snowman. (Id. at 32–34, 36– 39.) Regarding the claims to the acylated and pegylated peptide consisting of the amino acid sequence of SEQ ID NO: 21, Appellant indicates that there is no record evidence that such compounds exist in nature. (Id. at 42.) Analysis 35 U.S.C. § 101 defines patent-eligible subject matter. An invention is patent-eligible if it claims a “new and useful process, machine, manufacture, or composition of matter.” 35 U.S.C. § 101. The Supreme Court, however, has carved out exceptions to what would otherwise appear to be within the literal scope of § 101, e.g., “[l]aws of nature [and] natural phenomena” such as products of nature that are considered “building blocks of human ingenuity.” Alice Corp. v. CLS Bank Int’l, 573 U.S. 208, 216 (2014) (citing Ass’n for Molecular Pathology v. Myriad, 569 U.S. 576 (2013) and Mayo Collaborative Servs. v. Prometheus Labs, Inc., 566 U.S. 66, 89 (2012)). “[T]he ‘manifestations of laws of nature’ are ‘part of the storehouse of knowledge,’ ‘free to all men and reserved exclusively to none.’” Manual of Patent Examiner Procedure (“MPEP”) § 2106.04 (b) (quoting Funk Bros. Seed Co. v. Kalo Inoculant Co., 333 U.S. 127, 130 (1948)). “When a law of nature or natural phenomenon is claimed as a physical product, the courts have often referred to the exception as a ‘product of nature.’” MPEP § 2106.04(b)(II). Appeal 2020-000111 Application 15/226,126 7 The Supreme Court has established a two-step framework for “distinguishing patents that claim laws of nature, natural phenomena, and abstract ideas from those that claim patent-eligible applications of those concepts.” Alice, 573 U.S. at 216. “First, we determine whether the claims at issue are directed to” a patent-ineligible concept. Id. If so, “we consider the elements of each claim both individually and ‘as an ordered combination’ to determine whether the additional elements ‘transform the nature of the claim’ into a patent-eligible application.” Id. at 217 (quoting Mayo, 566 U.S. at 78–79). The United States Patent and Trademark Office (“PTO”) issued 2019 Revised Patent Subject Matter Eligibility Guidance (“Guidance”), indicating how the PTO would analyze patent eligibility under the Supreme Court’s two-step framework. 84 Fed. Reg. 50–57 (January 7, 2019).4 Under the Guidance, in determining what concept a claim is “directed to,” we first look to whether the claim recites any judicial exceptions, including laws of nature, natural phenomena, and/or abstract ideas. (Guidance, 84 Fed. Reg. at 53–54.) (“Step 2A, Prong One”). If it does, then we look to whether the claim recites additional elements that integrate the recited judicial exception into a practical application. (Id. at 54–55 (citing MPEP § 2106.05(a)–(c), (e)–(h)).) (“Step 2A, Prong Two”). 4 “All USPTO personnel are, as a matter of internal agency management, expected to follow the guidance.” Id. at 51; see also USPTO, October 2019 Update: Subject Matter Eligibility 1 (the “October 2019 Update”) (available at https://www.uspto.gov/sites/default/files/documents/peg_oct_2019_ update.pdf). Appeal 2020-000111 Application 15/226,126 8 Only if a claim (1) recites a judicial exception and (2) does not integrate that exception into a practical application, i.e., it is found to be “directed to” a judicial exception, do we then look to whether the claim contains an “‘inventive concept’ sufficient to ‘transform’” the claimed judicial exception into a patent-eligible application of the judicial exception. Guidance, 84 Fed. Reg. at 56; see also Alice, 573 U.S. at 221 (quoting Mayo, 566 U.S. at 82). Claims alleged to be patent-ineligible because they recite products of nature are properly analyzed under the framework of the Guidance. See Guidance, 84 Fed. Reg. at 54 n.20 (“This notice does not change the type of claim limitations that are considered to recite a law of nature or natural phenomenon. For more information about laws of nature and natural phenomena, including products of nature, see MPEP 2106.04(b) and (c).”). Applying the Guidance and binding legal precedent, we disagree with the Examiner’s conclusion that the claims are directed to patent-ineligible subject matter. We address independent claim 1 as the representative claim for our analysis. There is no dispute that claim 1, which recites a peptide in the form of a pharmaceutically acceptable salt, is a composition and, thus, falls squarely within the “composition of matter” statutory category. Consequently, we proceed to the next steps of the analysis. STEP 2A, Prong One: In Step 2A, Prong One of the Guidance, we evaluate whether claim 1 recites a judicial exception, i.e., whether it sets forth or describes a product of nature in accordance with the guidance in MPEP 2106.04 (b) and (c). Guidance, 84 Fed. Reg. at 54; October 2019 Update. Appeal 2020-000111 Application 15/226,126 9 a. Product of Nature Analysis Claim 1 requires a peptide “consisting of the amino acid sequence GLWHHQTEV (SEQ ID NO: 21)” where that peptide is a pharmaceutically acceptable salt. The claim includes recitation of a peptide having an amino acid sequence that is undisputedly found in nature as part of a protein having a larger sequence. As Appellant’s Specification indicates, SEQ ID NO: 21 is a peptide having an amino acid sequence from the 1211 amino acid NRCAM protein, a single-pass type I transmembrane protein interacting with ankyrin, and which is overexpressed in glioblastoma multiforme tissue as compared to normal brain tissue. (Subst. Spec. 27 (Table 1), 44.) However, as Appellant points out, the claim does not recite a free peptide, but rather a pharmaceutically acceptable salt of that peptide. Thus, the amino acid sequence of the peptide salt cannot be anything other than SEQ ID NO: 21, but that peptide having the sequence must be in ionic combination with another ion to form a pharmaceutically acceptable salt. The claimed salt is a structurally different chemical composition than a free peptide, as even the Examiner acknowledges (Ans. 5 (that the peptide is a salt “simply means one or more of the amino acid residues of which the peptide is composed has been ionized[ ] and has formed an ionic bond with whatever cation (e.g., Na+) or anion (e.g., C1-) might be present.”). (See Stern Declaration ¶ 20 (“Salts are formed when a compound that is ionized in solution forms a strong ionic interaction with an oppositely charged counterion, leading to neutralization of the charges . . . .”), id. ¶¶ 23–24 (“[P]eptides of any length . . . will therefore have a one free amino group (NH2,) referred to as the amino terminus or N-terminus and one free carboxyl group (COOH) referred to as the carboxyl or C-terminus . . . . Appeal 2020-000111 Application 15/226,126 10 [T]here can also be ionizable groups in the side chains (‘R’) of the amino acid residues within the peptide.”).) Appellant’s expert explained, with reference to numerous articles, that a peptide with the amino acid sequence of SEQ ID NO: 21 would not exist in the body as a salt. (Stern Declaration ¶¶ 32–33, 35.) Dr. Stern explained that peptide fragments, such as a peptide having the amino acid sequence SEQ ID NO: 21, that arise when proteins are degraded, are themselves degraded within a few seconds if not associated with other proteins involved in degradation, ER transport and loading of the peptide onto MHC-1 molecules. (Stern Declaration ¶ 32.) Dr. Stern notes that “[i]n the absence of peptide binding, neither the peptide nor the MHC molecule by itself is stable, or persists” in nature. (Id. ¶ 33 (emphasis omitted).) Dr. Stern further explains that even if the free peptide existed in the cell, “there is no acid-base reaction that could occur in the cytoplasm or ER of a cell . . . that would result in formation of a peptide salt.” (Id. ¶ 35.) That is because “[t]he formation of salts requires specific combinations of acids or bases in specific concentrations, at a defined ratio (stoichiometry), so that there is a set number of moles of acid and moles of base in a controlled environment[, and] [t]he cytoplasm of a cell is not such an environment.” (Id.) Dr. Stern notes that the cytoplasm “would not contain either the peptides or the acid or base counterpart in sufficient quantities in sufficient proximity to each other to form a peptide salt.” (Id.) Furthermore, Dr. Stern explains that “[e]ven if all the water in cell were removed, specific salts would not form, because of the highly complex mixtures of anions and cations present.” (Id.) Appeal 2020-000111 Application 15/226,126 11 The Examiner has not provided any evidence in contravention of the foregoing testimony by Dr. Stern. Rather, the Examiner asserts that peptide in salt form, nevertheless, will consist of the amino acid SEQ ID NO: 21 and thus is not “significantly changed.” (Ans. 5, 7.) The Examiner also asserts, without evidentiary support, that because of the presence of certain amino acids in the sequence “it is conceivable that the salt of the peptide may have formed by association with two cations and one anion.” (Ans. 6–7.) The Examiner states: naturally occurring peptides such as the peptide of SEQ ID NO: 21 are expected to exist at physiological pH (pH = 7.4) in the body of human in or on the surface of a cell expressing NRCAM in the context of an HLA-A2 class I complex . . . . Furthermore, as example, it is known that most of the Na+ in the body is present in the blood (plasma) and the interstitial, extracellular fluid, which surrounds the cells[ ], where it might freely associate with the negatively charged carboxyl terminus and/or the negatively charged glutamic acid residue of the peptide lying the in the cleft of the HLA complex to form a salt thereof. (Ans. 10.) Also, relying on general principles of chemistry, the Examiner posits that because the peptide is present in an aqueous solution in vivo within the cytosol, the endoplasmic reticulum, and at the surface of cells in complex with an HLA class I molecule, it will be ionized and because there are “counterions of the appropriate charge” naturally present in each situation in the body, a salt will form. (Ans. 11–15.) The Examiner’s assertion that, in general, the peptide fragment of protein degraded by a proteasome will naturally form a salt in the cytosol, the ER, or the MHC because there are counterions such as sodium, chloride and potassium around in the cell lacks any evidentiary foundation. And, it is Appeal 2020-000111 Application 15/226,126 12 contradicted by the testimony of Dr. Stern that salt formation requires specific combinations of acids or bases in specific concentrations, at a defined ratio (stoichiometry), so that there is a set number of moles of acid and moles of base in a controlled environment. The Examiner did not establish that the cytosol, the ER and the MHC in vivo are such a controlled environment with respect to peptide fragments of the protein degraded by a proteasome. In addition, the Examiner’s position that the free peptide is extant in the first place for long enough to form a salt is contradicted by Dr. Stern’s testimony that any free peptide of the collagen protein degraded by a proteasome would be rapidly degraded if it is not associated with certain other proteins in the cytosol or in transport to the endoplasmic reticulum or when bound in the MHC. While an amino acid sequence consisting of SEQ ID NO: 21 is unquestionably identical to the peptide sequence found in NRCAM, which Appellant does not dispute, we conclude that the preponderance of the evidence favors finding that the claimed pharmaceutically acceptable salt of the peptide consisting of the amino acid sequence of SEQ ID NO: 21 is not a product that occurs in nature. Furthermore, we disagree with the Examiner’s conclusion that the claimed invention is not markedly different from a naturally occurring peptide consisting of an amino acid sequence of SEQ ID NO: 21.5 The 5 We note, but do not find it necessary to respond to, Appellant’s arguments concerning any alleged misapplication of law in the MPEP. (Appeal Br. 10.) We need not address this argument because we conclude that the Examiner erred in evaluating the claimed invention as a whole. Appeal 2020-000111 Application 15/226,126 13 Examiner’s analysis does not properly address the claimed structure, as discussed above. The markedly different characteristics analysis is not applied to the component parts of the claimed salt, but to the compound as a whole. See, e.g., MPEP § 2106.04(c)(I)(A). As the MPEP notes, The courts have emphasized that to show a marked difference, a characteristic must be changed as compared to nature, and cannot be an inherent or innate characteristic of the naturally occurring counterpart or an incidental change in a characteristic of the naturally occurring counterpart. Myriad, 569 U.S. at 580 [ ]. Thus, in order to be markedly different, applicant must have caused the claimed product to possess at least one characteristic that is different from that of the counterpart. Id. § 2106.04(c)(II)(C). As the MPEP further explains, the “[m]arkedly different characteristics can be expressed as the product’s structure, function, and/or other properties, and are evaluated based on what is recited in the claim on a case-by-case basis.” Id. § 2106.04(c)(II). The question for consideration here is whether the structure claimed is different from the peptide sequence as it is found in nature. As just discussed, the evidence of record favors Appellant’s position that the claimed peptide does not exist in nature as a free peptide. Furthermore, it cannot be said that the pharmaceutically acceptable salt of amino acid peptide of SEQ ID NO: 21 is merely an isolated component of a larger structure known to be present in nature, similar to DNA isolated from the human genome. Cf. Myriad, 569 U.S. at 593 (“Nor are Myriad’s claims saved by the fact that isolating DNA from the human genome severs chemical bonds and thereby creates a nonnaturally occurring molecule.”); see also Roche Molecular Sys., Inc. v. CEPHEID, 905 F.3d 1363 (Fed. Cir. 2018) (finding similar to the claimed DNA at issue in Appeal 2020-000111 Application 15/226,126 14 Myriad, that the claimed primers were necessarily present in the natural genome of Mtb). In Myriad, the Supreme Court determined that naturally occurring, but isolated, DNA fell within the product of nature exception because “Myriad’s claims . . . do [not] rely in any way on the chemical changes that result from the isolation of a particular section of DNA.” Myriad, 569 U.S. at 593. The Court in Myriad, however, also noted that “creation of a cDNA sequence from mRNA results in an exons-only molecule that is not naturally occurring” and determined that such a chemical construct is patent-eligible. Id. at 594. Here, the markedly different characteristic for the claimed peptide is not merely due to the breaking of chemical bonds of the protein, but it is rather based on chemical differences between the NRCAM protein as it is found in nature, and the claimed pharmaceutically acceptable salt of the peptide of SEQ ID NO: 21 that is in ionic interaction with an oppositely charged counterion. That structural difference is not an inherent or innate characteristic of the naturally occurring peptide as it is found in nature or an incidental change as Appellant’s expert testimony and underlying supporting evidence establishes. We conclude that, like the cDNA in Myriad, the pharmaceutically acceptable salt of the peptide consisting of amino acid SEQ ID NO: 21 is markedly different from the naturally occurring peptide sequence of amino acid SEQ ID NO: 21 found in NRCAM.6 6 In addition to this structural difference, Dr. Stern contends that the free peptide would be poorly soluble in aqueous solution (Stern Declaration ¶ 39) whereas “[s]alts of hydrophobic peptides have been shown improve their solubility in aqueous solutions, just as salts of other compounds improve Appeal 2020-000111 Application 15/226,126 15 Accordingly, under Guidance Step 2A, Prong 1, we conclude that the composition of claim 1 does not recite a product of nature, and thus is not directed to a patent ineligible judicial exception. Our analysis of the issue need not proceed further. We similarly conclude that claims 9, 10, 13, and 14, which recite an “acylated” or a “pegylated” “peptide consisting of the amino acid sequence of GLWHHQTEV (SEQ ID NO: 21) or a pharmaceutically acceptable salt thereof” are not directed to a product of nature. The Examiner does not dispute that these claims are directed to a structure that is chemically different than that found in nature. (Ans. 18 (“[I]t is appreciated that acylation of peptides has been understood to alter the functional properties of the peptides, as well as their structures”); Ans. 19–20 (covalent attachment of PEG “is expected to alter, not only the structure of the peptide, but also its functional characteristics” and non-covalent pegylation is a structural alteration that can be reversed to “restore the peptide as it originally occurred”). The Examiner contends that even with the structural differences, the peptide sequence itself is not changed by the modifications. (Id. at 19–23.) their solubility” (id. ¶ 41). He also contends that “[p]eptides are not very stable in free form, without modifications” (id. ¶ 42) and that “the peptide claimed in the Immatics application can undergo hydrolysis in aqueous solution in free form” (id. ¶ 43), whereas “[f]ormation of peptide salts stabilizes the peptides from physical degradation, discussed above, to some extent” (id. ¶ 46). In light of our conclusion regarding the marked structural difference, we need not address Appellant’s additional argument and testimony of Dr. Stern that the physical properties of the pharmaceutically acceptable salt of the claimed peptide fragment is markedly different than a free peptide fragment if it existed in nature. Appeal 2020-000111 Application 15/226,126 16 The Examiner’s evidence offered in the Answer that an acylated peptide degradation product has been found bound to an HLA class I molecule does not establish the claimed acylated peptide having the specifically claimed sequence occurs naturally in the human body, or that this is the case for any peptide derived endogenously from the breakdown of a protein by a proteasome, nor does it contradict Appellant’s expert’s testimony and underlying evidence relied upon that such does not exist. (See Stern Declaration ¶ 69.) Furthermore, the Examiner’s position that even with the structural differences because of the addition of an acyl group or PEG, the peptide sequence itself is not changed by the modification is an improper analysis. As explained, the markedly different characteristics analysis is not applied to the component parts of the claimed acylated or pegylated peptide claimed, but to the compound as a whole. The difference in structure is more than mere excising a DNA or a peptide from a larger protein; the structure of these compounds as a whole, just as with the pharmaceutically acceptable salt of claim 1, chemically speaking, is different from that which is naturally occurring. That is so even if the structure can be arrived at using routine and conventional chemical modifications. An analysis of whether the activity to arrive at that different structure may not be an inventive concept is not a relevant consideration here. MPEP § 2106.04(c) (“[O]nce a markedly different characteristic in [a] product is shown, no further analysis would be necessary for eligibility because no product of nature exception is recited (i.e., Step 2B is not necessary because the answer to Step 2A is NO).”). Appeal 2020-000111 Application 15/226,126 17 In light of the foregoing, we do not affirm the Examiner’s rejection of claims 1, 3, 4, 9–14, and 21–26 under 35 U.S.C. § 101 as being directed to patent-ineligible subject matter. II. Non-statutory double patenting Appellant did not argue the substance of this rejection nor has it indicated that a terminal disclaimer was filed. Thus, we summarily affirm the Examiner’s rejection based on the judicially created doctrine of obviousness-type double patenting for the reasons advanced by the Examiner in the Final Rejection. See MPEP § 1205.02 (“If a ground of rejection stated by the examiner is not addressed in the appellant’s brief, appellant has waived any challenge to that ground of rejection and the Board may summarily sustain it, unless the examiner subsequently withdrew the rejection in the examiner’s answer.”). DECISION SUMMARY In summary: Claims Rejected 35 U.S.C. § Reference(s)/Basis Affirmed Reversed 1, 3, 4, 9– 14, 21–26 101 Eligibility 1, 3, 4, 9– 14, 21–26 1, 3, 4, 9– 14, 21–27 Nonstatutory Double Patenting 1, 3, 4, 9– 14, 21–27 Overall Outcome 1, 3, 4, 9– 14, 21–27 TIME PERIOD FOR RESPONSE No time period for taking any subsequent action in connection with this appeal may be extended under 37 C.F.R. § 1.136(a). See 37 C.F.R. § 1.136(a)(1)(iv). Appeal 2020-000111 Application 15/226,126 18 AFFIRMED