10785924 (B.P.A.I. Feb. 13, 2009)

Ex Parte Gilchrest et al

Board of Patent Appeals and InterferencesFeb 13, 2009

10785924 (B.P.A.I. Feb. 13, 2009)

UNITED STATES PATENT AND TRADEMARK OFFICE __________ BEFORE THE BOARD OF PATENT APPEALS AND INTERFERENCES __________ Ex parte BARBARA A. GILCHREST and MINA YAAR1 __________ Appeal 2008-5035 Application 10/785,924 Technology Center 1600 __________ Decided:2 February 13, 2009 __________ Before DONALD E. ADAMS, ERIC GRIMES, and MELANIE L. McCOLLUM, Administrative Patent Judges. McCOLLUM, Administrative Patent Judge. DECISION ON APPEAL This is an appeal under 35 U.S.C. § 134 involving claims to a method of inhibiting β-amyloid binding to the p75 nerve growth factor receptor. 1 The real party in interest is the Trustees of Boston University (App. Br. 3). 2 The two-month time period for filing an appeal or commencing a civil action, as recited in 37 C.F.R. § 1.304, begins to run from the decided date shown on this page of the decision. The time period does not run from the Mail Date (paper delivery) or Notification Date (electronic delivery). Appeal 2008-5035 Application 10/785,924 2 The Examiner has rejected the claims as anticipated, nonenabled, and/or not supported by an adequate written description. We have jurisdiction under 35 U.S.C. § 6(b). We affirm. STATEMENT OF THE CASE Alzheimer’s disease “is characterized by progressive dementia together with neuropathological findings of ‘senile plaques’ in the brain formed by deposits of β-amyloid protein, surrounded by clusters of degenerating neurons” (Spec. 1: 15 to 2: 1). “[N]euronal cells express a high affinity (p140trkA) and a low affinity receptor (p75NTR) for nerve growth factor (NGF)” (id. at 6: 16-17). The Specification discloses that “these nerve growth factor receptors are also expressed on melanocytes and that β-amyloid binds to the low affinity nerve growth factor receptor, p75NTR, expressed on the melanocyte surface” (id. at 6: 17-20). In addition, the Specification discloses that “binding of β-amyloid to the p75NTR activates the receptor, resulting in apoptotic cell death of the melanocytes” (id. at 6: 20-22). The Specification also discloses that “β-amyloid mediated-apoptosis can be competitively blocked by providing nerve growth factor or a biologically active fragment, analog or derivative thereof” (id. at 6: 22-24). Claims 56-77 are on appeal.3 We will focus on claim 74, which reads as follows: A method of inhibiting β-amyloid-mediated activation of p75 nerve growth factor receptor of a target cell, comprising contacting the target cell with a small organic molecule, wherein the target cell expresses p75 nerve 3 Claims 48-55 are also pending but have been withdrawn from consideration by the Examiner (App. Br. 3). Appeal 2008-5035 Application 10/785,924 3 growth factor receptor, and wherein β-amyloid is present at a concentration sufficient to mediate activation of the p75 nerve growth factor receptor, wherein the small organic molecule binds to the p75 nerve growth factor receptor with at least about half the affinity as nerve growth factor and competitively inhibits binding of β-amyloid to the p75 nerve growth factor receptor, thereby inhibiting β-amyloid protein or β-amyloid peptide activation of the p75 nerve growth factor receptor of a cell. The Examiner relies on the following reference: Shahrooz Rabizadeh et al., Expression of the low-affinity nerve growth factor receptor enhances β-amyloid peptide toxicity, 91 PROC. NATL. ACAD. SCI. USA 10703-10706 (1994) (hereinafter “Rabizadeh”). Appellants rely on the following references: David C. Horwell, The ‘peptoid’ approach to the design of non- peptide, small molecule agonists and antagonists of neuropeptides, 13 TRENDS BIOTECHNOL. 132-134 (1995) (hereinafter “Horwell”); Gerhard Klebe and Thomas Mietzner, A fast and efficient method to generate biologically relevant conformations, 8 J. COMPUT. AIDED MOL. DES. 583-606 (1994) (hereinafter “Klebe”); Neil Q. McDonald et al., New protein fold revealed by a 2.3-Å resolution crystal structure of nerve growth factor, 354 NATURE 411-414 (1991) (hereinafter “McDonald”); and B. S. Chapman and I. D. Kuntz, Modeled structure of the 75-kDa neurotrophin receptor, 4 PROTEIN SCI. 1696-1707 (1995) (hereinafter “Chapman”). Claims 56-77 stand rejected under 35 U.S.C. § 112, first paragraph, as failing to comply with the enablement and written description requirements (Ans. 4 & 8). Claims 56, 57, 61-63, 65-67, 69, 70, and 74-77 stand rejected under 35 U.S.C. § 102(b) as anticipated by Rabizadeh (Ans. 10). Appeal 2008-5035 Application 10/785,924 4 ENABLEMENT The Examiner contends that the Specification “does not enable any person skilled in the art to which it pertains, or with which it is most nearly connected, to make or use the invention commensurate in scope with these claims” (Ans. 4). Issue Did the Examiner err in concluding that the Specification does not enable the full scope of the claim term “small organic molecule”? Findings of Fact 1. The Specification discloses: Activation of the p75 nerve growth factor receptor can be determined by measuring the β-amyloid activation of the p75 nerve growth factor receptor of neural crest-derived cells, in culture or in a tissue sample, in the presence of the test substance and comparing the results with the β-amyloid activation of the p75 nerve growth factor receptor of neural crest-derived cells in a control culture or sample without the test-substance. A decrease of β-amyloid activation of the p75 nerve growth factor receptor of neural crest-derived cells in the test sample compared to β-amyloid activation of the p75 nerve growth factor receptor of neural crest-derived cells in the control sample is indicative of a substance that inhibits β-amyloid-mediated apoptosis in neural crest-derived cells. (Spec. 4: 20 to 5:2.) 2. The Specification also discloses that “[b]inding of NGF to p75NTR is mediated through amino acid residues 29-36, TDIKGKEV (SEQ ID NO: 2), that are part of the β-hairpin loop of NGF” (id. at 19: 1-2). Appeal 2008-5035 Application 10/785,924 5 3. In addition, the Specification discloses that, “[i]f lysine (K) at position 34 is replaced by alanine (A), the resulting mutant NGF molecule still binds p75NTR but with 50% lower affinity” (id. at 19: 3-4). 4. The Specification also discloses that “in β-amyloid the amino acid residues 28-30 . . . are KGA, a sequence that appears to permit p75NTR binding by β-amyloid” (id. at 19: 5-7). 5. In addition, the Specification discloses that the “amino acid sequences of the NGF fragments, analogues, derivatives, variants and mutants of the present invention can be altered to optimize NGF binding to p75NTR, by methods known in the art by introducing appropriate nucleotide changes into native or variant DNA encoding the NGF, or by in vitro synthesis of the desired NGF” (id. at 21: 9-12). 6. The Specification also discloses: [T]he melanocyte culture model can be used to identify substances that block the p75NTR binding of β-amyloid, and thus block β-amyloid-mediated neuronal apoptosis. Several assay methods are available in the art to measure p75 nerve growth factor receptor activation by β-amyloid protein or β-amyloid peptide and include an assay to determine melanocyte cell yield, an assay to determine the inducement of Bax protein expression; an assay to determine the onset of melanocyte apoptosis or an assay to determine the presence of plaque-like structures in the melanocyte culture. (Id. at 22: 1-7.) 7. In addition, the Specification discloses that “candidate substances that inhibit the binding of amyloid protein/peptide can also be identified using in vitro binding assays well known in the art, such as surface plasmon resonan[ce] (SPR). For example, peptide libraries and other small Appeal 2008-5035 Application 10/785,924 6 organic molecule libraries can be screened using proximity assays or Biospecific Interaction Analysis (BIA).” (Id. at 22: 22-26.) 8. The Specification also states: [T]he tripeptide lysine-glycine-alanine [KGA] is a candidate substance for use as a therapeutic to alleviate the symptoms of Alzheimer’s disease. The melanocyte culture model system can be used to identify and evaluate other peptides containing the KGK or KGA sequence, or various analogs of the KGK or KGA tripeptide, to determine an optimum conformation and composition that will bind p75NTR and, thus, block the binding of the apoptosis-inducing β-amyloid ligand without interfering with NGF binding that is beneficial. Because evaluation of candidate substances is made with melanocytes obtained specifically from the individual at risk, or with the diagnosis of [Alzheimer’s disease], the probability of identifying an effective candidate substance is very high. (Id. at 23: 13-22.) 9. In addition, the Specification discloses administering “a substance, e.g., a cyclic peptide comprising KGK or KGA, or an analog thereof” (id. at 24: 7-8). 10. In particular, the Specification discloses synthesizing “the pentapeptide CKGAC (SEQ ID NO: 3)” and that the “cysteine residues flanking the ends of the pentapeptide can be linked, e.g., by a disulfide bond, to maintain the conformation required for binding of the peptide to the p75NTR, thus inhibiting, or preventing apoptosis” (id. at 24: 9-14). 11. The Specification also states that the “length of the peptide can be longer than a pentapeptide, as long as the KGA, or analog peptide is maintained in a configuration suitable for binding activity” (id. at 24: 14-16). Appeal 2008-5035 Application 10/785,924 7 12. Specifically, the Specification discloses a cyclic decapeptide (SEQ ID NO: 4) “synthesized by attaching two cysteine residues to the beginning and the end of the β-amyloid fragment consisting of amino acids 24-31: VGSNKGAI (SEQ ID NO: 1)” and that this peptide “competitively inhibited 125I-β-amyloid binding” and blocked cell loss (id. at 12: 23-28; see also Spec. 24: 17 & 30: 4-19). Principles of Law “The first paragraph of 35 U.S.C. § 112 requires, inter alia, that the specification of a patent enable any person skilled in the art to which it pertains to make and use the claimed invention . . . without ‘undue experimentation.’” In re Vaeck, 947 F.2d 488, 495 (Fed. Cir. 1991) (citing In re Wands, 858 F.2d 731, 737 (Fed. Cir. 1988)). Some experimentation, even a considerable amount, is not “undue” “if it is merely routine, or if the specification . . . provides a reasonable amount of guidance with respect to the direction in which the experimentation should proceed.” In re Wands, supra. In particular, “sufficient disclosure . . . to teach those of ordinary skill how to make and how to use the invention . . . means that the disclosure must adequately guide the art worker to determine, without undue experimentation, which species among all those encompassed by the claimed genus possess the disclosed utility.” In re Vaeck, 947 F.2d at 496. “Whether undue experimentation is needed is not a single, simple factual determination, but rather is a conclusion reached by weighing many factual considerations.” In re Wands, supra. Factors to be considered include: (1) the quantity of experimentation necessary, (2) the amount of direction or guidance presented, (3) the presence or absence of Appeal 2008-5035 Application 10/785,924 8 working examples, (4) the nature of the invention, (5) the state of the prior art, (6) the relative skill of those in the art, (7) the predictability or unpredictability of the art, and (8) the breadth of the claims. Id. In re Wands concerned a claim directed to a method utilizing an antibody to assay for a substance comprising hepatitis B-surface antigen (HBsAg) determinants, wherein the antibody is a monoclonal high affinity IgM antibody having a particular binding affinity for the HBsAg determinants. 858 F.2d at 734. The issue was “whether the specification enables one skilled in the art to make the monoclonal antibodies that are needed to practice the invention.” Id. at 735. In Wands, the Specification disclosed “a procedure for immunizing mice against HBsAg, and the use of lymphocytes from these mice to produce hybridomas that secrete monoclonal antibodies specific for HBsAg.” Id. at 734. “Hybridoma cells that secrete the desired antibodies then must be isolated from [an] enormous number of other cells in the mixture[, which] is done through a series of screening procedures.” Id. at 737. “The PTO [did] not question that the screening techniques used by Wands were well known in the monoclonal antibody art.” Id. at 738. Finding that “[p]ractitioners of this art are prepared to screen negative hybridomas in order to find one that makes the desired antibody,” the Federal Circuit concluded that the record indicates that “the amount of effort needed to obtain [the] antibodies is not excessive.” Id. at 740. “[T]he PTO bears an initial burden of setting forth a reasonable explanation as to why it believes that the scope of protection provided by Appeal 2008-5035 Application 10/785,924 9 that claim is not adequately enabled by the description of the invention provided in the specification of the application.” In re Wright, 999 F.2d 1557, 1561-62 (Fed. Cir. 1993). “If the PTO meets this burden, the burden then shifts to the applicant to provide suitable proofs indicating that the specification is indeed enabling.” Id. at 1562. In meeting Appellants’ burden, “[a]ttorney’s argument in a brief cannot take the place of evidence.” In re Pearson, 494 F.2d 1399, 1405 (CCPA 1974). Analysis In the present case, the Examiner finds: [T]he specification, while being enabling for methods of inhibiting p75 nerve growth factor receptor (p75NGFR—also referred to in the specification as p75NTR) mediated apoptosis of cells expressing p75NGFR comprising administering NGF or compounds comprising the polypeptides of amino acid sequences 1, 2, 3 or 4, does not reasonably provide enablement for methods of inhibiting p75NGFR mediated apoptosis of cells expressing p75NGFR comprising administering any small organic molecule as broadly claimed. (Ans. 4.) In particular, the Examiner finds that “the claim covers every conceivable structure for achieving the stated property (the ability to inhibit p75NGFR mediated apoptosis) while the specification discloses at most only those structures known by the inventor to achieve the stated result, which is NGF or one of the peptides of SEQ ID NOs: 1-4” (id. at 15). The Examiner concludes: [D]ue to the large quantity of experimentation necessary to test for all possible small molecules capable of inhibiting p75NGFR mediated apoptosis in cells expressing p75NGFR, the lack of direction/guidance presented in the specification and the absence of working examples directed to administration of any small molecule save NGF (SEQ ID NOs: 1-4), the complex Appeal 2008-5035 Application 10/785,924 10 nature of the invention, the unpredictability of the effects of mutation on protein structure and function, and the breadth of the claims which fail to recite limitations on all possible small molecules that would be capable of inhibiting p75NGFR mediated apoptosis of cells expressing p75NGFR, undue experimentation would be required of the skilled artisan to make and/or use the claimed invention in its full scope. (Id. at 16.) We agree with the Examiner. Claim 74 recites contacting the target cell with a “small organic molecule [that] binds to the p75 nerve growth factor receptor with at least about half the affinity as nerve growth factor and competitively inhibits binding of β-amyloid to the p75 nerve growth factor.” As noted by the Examiner, the term “‘small organic molecule’ . . . includes organic ring structures, peptides, nucleic acids, sugars, lipids, etc.” (Ans. 18). The Specification discloses peptides that “bind[] to the p75 nerve growth factor receptor” (Findings of Fact (FF) 2, 10, & 12). In addition, the Specification describes assays that can be used to identify molecules having this property (FF 1 & 6-8). However, the Specification does not provide sufficient guidance as to which non-peptide small organic molecules should be subjected to these assays in order to identify such molecules. Therefore, we agree that the Examiner has set forth a prima facie case that it would require undue experimentation to make and use small organic molecules within the full scope of claim 74. Appellants argue that “the methods of the present invention utilize small organic molecules that are functionally described in a very narrow way. These small organic molecules inhibit p75 nerve growth factor receptor mediated apoptosis and/or β-amyloid binding to p75 nerve growth Appeal 2008-5035 Application 10/785,924 11 factor receptor of target cells that express the p75 nerve growth factor receptor.” (App. Br. 8.) Furthermore, the assays for identifying the small organic molecules of the invention are well described and involve routine steps known by those of skill in the art. Identification of these small organic molecules that function as described is simply a matter of repeating one or more of the described assays until a desirable small organic molecule is found. For one of skill in the art, performing the assays described in the present application is a matter of routine experimentation. Such experimentation is neither undue nor burdensome. (Id.) Thus, Appellants argue: Just as in In re Wands, the specification describes in great detail the assays for identifying the small organic molecules used in the claimed methods of the invention. Furthermore, one of ordinary skill in the art, when identifying the small organic molecules would be prepared to screen libraries, such as those that have been described in specification on page 22, lines 24- 26, in order to determine which small organic molecules exhibit the desired characteristics for use with the claimed methods of the invention . . . . The fact that the instant application is drawn to a more expansive pool of molecules than was the application of In re Wands does not negate that assertion that one of skill in the art, using the Applicants’ specification would be able to make and use the claimed invention. (Id. at 9.) We are not persuaded. As noted by Appellants, practicing the full scope of the invention in Wands requires the use of screening assays. Wand, 858 F.2d at 737. However, Wands’ Specification disclosed a method for producing antibody-secreting cells to be subjected to these screening assays. Id. at 734. In contrast, in the present case, the compounds to be subjected to the screening assays are “small organic molecules.” The Specification does Appeal 2008-5035 Application 10/785,924 12 not provide sufficient guidance as to which small organic compounds should be subjected to the assays. In addition, Appellants have not provided sufficient evidence that practitioners in this art would be enabled, without further guidance, to screen the full scope of the broad category of small organic molecules in order to find ones that have the desired binding. Thus, we do not agree that the holding in In re Wands demonstrates that the present enablement rejection should be reversed. Conclusion Appellants have not shown that the Examiner erred in concluding that the Specification does not enable the full scope of the claim term “small organic molecule.” We therefore affirm the enablement rejection of claim 74. Claims 56-73 and 75-77 have not been argued separately and therefore fall with claim 74. 37 C.F.R. § 41.37(c)(1)(vii). WRITTEN DESCRIPTION The Examiner contends that the claims contain “subject matter which was not described in the specification in such a way as to reasonably convey to one skilled in the relevant art that the inventor(s), at the time the application was filed, had possession of the claimed invention” (Ans. 8). Issue Did the Examiner err in concluding that the Specification does not provide adequate written description to support the claim term “small organic molecule”? Findings of Fact 13. Horwell “describes a rationale and strategy for the design of low molecular weight, non-peptide ligands (peptoids), using the chemical Appeal 2008-5035 Application 10/785,924 13 structure of mammalian neuropeptides as a starting point” (Horwell, Abstract). 14. Horwell defines “peptoid” as “a non-peptide agent that has been designed using the chemical structure of mammalian neuropeptides as the starting point, and may act as either a pharmacological functional agonist or an antagonist” (id. at 132). 15. Horwell states that “[t]here are classical precedents for the use of small molecule hormone and neurotransmitters as ‘chemical leads’ to therapeutically useful agonists and antagonists” (id.). 16. However, Horwell states that “[p]olypeptides are more complex chemical leads than the small molecule hormones” (id. at 133). 17. In particular, Horwell states that “[p]eptides are polyfunctional ligands and have a large degree of conformational freedom associated with the many freely rotatable bonds found in the polyamide backbone and in the amino acid side chains” (id.). 18. Horwell discloses “a hypothesis that the ‘problem’ of a large, flexible polypeptide can be reduced to a small-molecule surrogate as a synthetic ‘device’ if three or fewer amino acid residues are identified as critical for receptor recognition” (id.). 19. Horwell also indicates that its “ideas and rationale . . . have been put into practice . . . , resulting in the rational design of antagonists and agonists for several neuropeptides” (id.). 20. In addition, Horwell states that “[w]e hope that this approach will provide other peptoids that are able to bind at the active site of the protein target with specific interactions that may endow members of a Appeal 2008-5035 Application 10/785,924 14 congeneric peptoid series with either antagonistic or agonistic properties” (id. at 134). 21. Klebe discloses that “reliance on just the crystal structures of a ligand itself may not, in most cases, be an infallible and reliable indicator of a biologically active conformation” (Klebe 584). 22. Therefore, Klebe discloses “a knowledge-based approach toward conformational analysis. This ‘knowledge’ . . . is not stored in terms of ‘rules’, but incorporated into an extended set of conformational libraries which are directly derived from crystal data by a statistical evaluation of conformational preferences.” (Id. at 585.) 23. Klebe also discloses that the “produced conformers possess some probability to represent geometries that are likely to resemble those actually adopted at the binding site of a protein” (id. at 604). 24. McDonald discloses the crystal structure of the murine NGF dimer (MacDonald, Abstract). 25. McDonald also discloses the presence of a β–hairpin turn at residues 30-33 (id. at 412). 26. Chapman discloses “a molecular model of NTR, also called p75NGFR” (Chapman, Abstract). 27. Chapman also discloses that “NTR appears to bind in the dimer interface of NGR, making two sets of contacts” (id.). 28. Chapman states that an “application of this study might be to discover small molecule agonists that mimic the ability of [neurotrophins] to prevent cell death induced by the NTR” (id. at 1704). Appeal 2008-5035 Application 10/785,924 15 Principles of Law The first paragraph of 35 U.S.C. § 112 “requires a ‘written description of the invention’ which is separate and distinct from the enablement requirement.” Vas-Cath Inc. v. Mahurkar, 935 F.2d 1555, 1563 (Fed. Cir. 1991). An adequate written description of a chemical invention “requires a precise definition, such as by structure, formula, chemical name, or physical properties.” University of Rochester v. G.D. Searle & Co., Inc., 358 F.3d 916, 927 (Fed. Cir. 2004); Regents of the Univ. of Cal. v. Eli Lilly & Co., Inc., 119 F.3d 1559, 1566 (Fed. Cir. 1997); Fiers v. Revel, 984 F.2d 1164, 1171 (Fed. Cir. 1993). “A description of what a material does, rather than of what it is, usually does not suffice.” Rochester, 358 F.3d at 923; Eli Lilly, 119 F.3d at 1568. Instead, the “disclosure must allow one skilled in the art to visualize or recognize the identity of the subject matter purportedly described.” Id. However, not all functional descriptions “necessarily fail as a matter of law to meet the written description requirement; rather, the requirement may be satisfied if in the knowledge of the art the disclosed function is sufficiently correlated to a particular, known structure.” Amgen Inc. v. Hoechst Marion Roussel, Inc., 314 F.3d 1313, 1332 (Fed. Cir. 2003). In addition, possession of a genus “may be achieved by means of a recitation of a representative number of [compounds] . . . falling within the scope of the genus.” Eli Lilly, 119 F.3d at 1569. Possession may not be shown by merely describing how to obtain possession of members of the claimed genus. See Rochester, 358 F.3d at 927. Appeal 2008-5035 Application 10/785,924 16 Analysis The Examiner finds that, “[w]ith the exception of NGF or compounds comprising the polypeptides of amino acid sequences 1, 2 . . . , 3, and 4 . . . , the skilled artisan cannot envision the detailed chemical structure of the encompassed small organic molecules” (Ans. 9). The Examiner also finds that “NGF and the peptide[s] of SEQ ID NOS: 1-4 are not representative of the vast genus of molecules encompassed by the term ‘small organic molecules’” (id. at 27). We agree with the Examiner. Claim 74 recites contacting the target cell with a “small organic molecule [that] binds to the p75 nerve growth factor receptor with at least about half the affinity as nerve growth factor and competitively inhibits binding of β-amyloid to the p75 nerve growth factor receptor.” As noted by the Examiner, “‘small organic molecules’ . . . are not limited to peptides or proteins, but encompass any small carbon containing molecule capable of carrying out the required functions” (Ans. 30). However, the Specification does not describe any non-peptide small organic molecules that bind to the p75 nerve growth factor receptor, nor does the Specification disclose the physical properties or provide another precise definition of these molecules. Therefore, we agree with the Examiner that the Specification does not adequately describe species representative of the genus of small organic molecules recited in claim 74. Appellants argue that “it is axiomatic in patent law that an inventor can establish reduction to practice in one of two ways: 1) by demonstrating actual reduction to practice or 2) by filing an enabling patent application and thus establishing constructive reduction to practice” (App. Br. 10). Appeal 2008-5035 Application 10/785,924 17 Therefore, Appellants argue that, “[b]ecause . . . the specification is enabling, the filing of the specification represents constructive reduction to practice, and thus, demonstrates that Applicants were in possession of the invention at the time of filing” (id.). We are not persuaded. First, as discussed above, we do not agree that Appellants have overcome the Examiner’s prima facie case that the claims are not enabled. In addition, the first paragraph of 35 U.S.C. § 112 “requires a ‘written description of the invention’ which is separate and distinct from the enablement requirement.” Vas-Cath Inc. v. Mahurkar, supra. Thus, even if the Specification enabled claim 74, it would not necessarily follow that the Specification provided written description support for claim 74. Appellants also argue that the “specification clearly describes the structure required for binding p75NTR” (App. Br. 10). To support this statement, Appellants refer to the Specification at page 21, line 9, to page 23, line 22 (id.). We are not persuaded. The cited portion of the Specification indicates that assays for identifying substances having the claimed properties are known, that “peptide libraries and other small organic molecule libraries can be screened,” and that “the probability of identifying an effective candidate substance is very high” (FF 6-8). However, describing how to identify molecules having the claimed function is not a description of “the structure required for binding p75NTR,” as argued by Appellants. See Rochester, 358 F.3d at 927. The cited portion of the Specification also discloses that the “amino acid sequences of the NGF fragments, analogues, derivatives, variants and Appeal 2008-5035 Application 10/785,924 18 mutants of the present invention can be altered to optimize NGF binding to p75NTR” (FF 5), that “the tripeptide lysine-glycine-alanine [KGA] is a candidate substance,” and that “other peptides containing the KGK or KGA sequence, or various analogs of the KGK or KGA tripeptide, [can be evaluated] to determine an optimum conformation and composition that will bind p75NTR and, thus, block the binding of the apoptosis-inducing β-amyloid ligand” (FF 8). However, claim 74 is directed to a method that uses a “small organic molecule” that has the claimed function. The molecules are not limited to NGF fragments, analogues, derivatives, variants, and mutants or even to peptides containing the tripeptide KGA or KGK, or analogs thereof. Thus, these disclosures are not representative of the claimed genus. Referring to Horwell and Klebe, Appellants additionally argue that, “at the time of the invention, there were well known methods in the art to design molecules and test their biological activity once a few naturally occurring or synthetic molecules having a desired function were identified” (App. Br. 10).4 We are not persuaded. Horwell “describes a rationale and strategy for the design of low molecular weight, non-peptide ligands (peptoids), using the chemical structure of mammalian neuropeptides as a 4 This argument appears to be more relevant to the enablement rejection. However, this argument does not persuade us to reverse the enablement rejection. In particular, both Horwell and Klebe describe the difficulties associated with designing non-peptide equivalents to peptides (FF 15-17 & 21). Although they propose techniques to deal with these difficulties (FF 13, 18, 19, & 22), we do not agree that the disclosure of techniques that may or may not work is sufficient to demonstrate that non-peptide equivalents can be uncovered without undue experimentation (see FF 20 & 23). Appeal 2008-5035 Application 10/785,924 19 starting point” (FF 13). In addition, Klebe discloses “a knowledge-based approach toward conformational analysis[, where the] ‘knowledge’ . . . is not stored in terms of ‘rules’, but incorporated into an extended set of conformational libraries which are directly derived from crystal data by a statistical evaluation of conformational preferences” (FF 22). However, neither reference describes the physical properties or another precise definition of molecules that bind to the p75 nerve growth factor receptor. Referring to McDonald and Chapman, Appellants also argue that, “at the time of the invention, receptor-ligand binding models existed for designing analogs of the highly conserved protein NGF and its relatives” (App. Br. 11). McDonald discloses the crystal structure of the murine NGF dimer (FF 24) and Chapman discloses a molecular model of p75 nerve growth factor receptor (FF 26). However, Appellants have not shown that the crystal structure of NGF or the molecular model of the p75 nerve growth factor receptor provides sufficient information about molecules other than NGF that bind to the p75 nerve growth factor receptor to describe these molecules. Conclusion Appellants have not shown that the Examiner erred in concluding that the Specification does not provide an adequate written description to support the claim term “small organic molecule.” We therefore affirm the written description rejection of claim 74. Claims 56-73 and 75-77 have not been argued separately and therefore fall with claim 74. 37 C.F.R. § 41.37(c)(1)(vii). Appeal 2008-5035 Application 10/785,924 20 ANTICIPATION The Examiner finds that Rabizadeh teaches “a method of inhibiting p75NGFR mediated apoptosis in PC12 cells transfected to express p75NGFR . . . by administering NGF in the presence of βAP” (Ans. 11). The Examiner also finds that the “NGF used by Rabizadeh et al. meets the limitation of ‘small organic molecule’ absent a specific definition in the spec[i]fication or claims, since peptides are small and organic” (id. at 12). Appellants argue that “one of skill in the art would not consider the term ‘small organic molecule’ to include a protein such as NGF. Instead, one of skill in the art would describe a protein such as NGF as a macromolecule.” (App. Br. 13.) Issue Did the Examiner err in concluding that NGF is a “small organic molecule”? Findings of Fact 29. Rabizadeh discloses that the “low-affinity nerve growth factor receptor (NGFR) p75NGFR induces apoptosis in the absence of nerve growth factor (NGF) binding but enhances neural survival when bound to NGF” (Rabizadeh, Abstract). 30. In particular, Rabizadeh discloses that “cells that express p75NGFR . . . were sensitive to [β-amyloid peptide] toxicity, with a LD50 of ≈5 µM, but that the LD50 increased to ≈50 µM in the presence of NGF” (id. at 10705). 31. The term “macromolecule” is defined as a “molecule, usually organic, composed [of] an aggregation of hundreds or thousands of atoms” Appeal 2008-5035 Application 10/785,924 21 Hawley’s Condensed Chemical Dictionary, 14th ed. (2002) (definition attached). The definition goes on to state: Such giant molecules are generally of two types. (1) Individual entities (compounds) that cannot be subdivided without losing their chemical identity. Typically these are proteins, many of which have molecular weights running into the millions. (2) Combinations of repeating chemical units (monomers) linked together into chain or network structures called polymers; each monomer has the same chemical constitution as the polymer, e.g., isoprene (C5H8) and polyisoprene (C5H8)n. . . . (Id.) 32. “NGF is a dimeric molecule, with 118 amino acids per protomer” (McDonald 411). Principles of Law “A claim is anticipated only if each and every element as set forth in the claim is found, either expressly or inherently described, in a single prior art reference.” Verdegaal Bros., Inc. v. Union Oil Co., 814 F.2d 628, 631 (Fed. Cir. 1987). “It is axiomatic that, in proceedings before the PTO, claims in an application are to be given their broadest reasonable interpretation consistent with the specification.” In re Sneed, 710 F.2d 1544,1548 (Fed. Cir. 1983). However, claim language must be interpreted according to how it would have been understood by those skilled in the art at the time the application was filed. See Schering Corp. v. Amgen Inc., 222 F.3d 1347, 1353 (Fed. Cir. 2000). In addition, if an Applicant wants to be his own lexicographer and give a term other than its ordinary meaning, the Specification must clearly redefine the term so as to put one skilled in the art on notice that the term has Appeal 2008-5035 Application 10/785,924 22 been redefined. Process Control Corp. v. HydReclaim Corp., 190 F.3d 1350, 1357 (Fed. Cir. 1999). Analysis Rabizadeh discloses contacting, in the presence of β-amyloid, a cell that expresses p75 nerve growth factor receptor with an organic molecule, NGF, that “binds to the p75 nerve growth factor receptor with at least about half the affinity as nerve growth factor and competitively inhibits binding of β-amyloid to the p75 nerve growth factor receptor,” as recited in claim 74 (emphasis added) (FF 29-30). However, we do not agree that the Examiner has set forth a prima facie case that NGF would be considered a “small organic molecule.” In particular, we agree with Appellants that one of ordinary skill in the art would consider NGF to be a “macromolecule” (FF 31-32). In the attached definition, a macromolecule is referred to as a “giant” molecule. Thus, although we recognize that “small” is a relative term and that NGF is small relative to many objects, we do not agree that the Examiner has set forth a prima facie case that one of ordinary skill in the art would consider NGF to be a “small” molecule. The Examiner argues that “[n]owhere in the specification is NGF or other larger polypeptides clearly excluded in a definition of molecules that could be used in the claimed methods” (Ans. 34). Therefore, the Examiner argues that “the plain meaning defined in Appellants’ arguments is inconsistent with the specification, which does not exclude macromolecules” (id. at 35). Appeal 2008-5035 Application 10/785,924 23 We agree with the Examiner that the Specification does not clearly exclude NGF or other large polypeptides from being substances that could be used in the methods described therein. However, the Examiner has not pointed to a passage in the Specification suggesting that the term “small organic molecule” should be interpreted to include NGF and other large polypeptides. Therefore, we agree with Appellants that the term “small organic molecule” should be interpreted as it would be by one of ordinary skill in the art. Conclusion The Examiner has not set forth a prima facie case that NGF would be considered a “small organic molecule.” We therefore reverse the anticipation rejection of claim 74 and of claims 56, 57, 61-63, 65-67, 69, 70, and 75-77, which recite or depend from a claim that recites a “small organic molecule.” ORDER We affirm the enablement and written description rejections of claims 56-77. However, we reverse the anticipation rejection of claims 56, 57, 61-63, 65-67, 69, 70, and 74-77. 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 LP Appeal 2008-5035 Application 10/785,924 24 HAMILTON, BROOK, SMITH & REYNOLDS, P.C. 530 VIRGINIA ROAD P.O. BOX 9133 CONCORD, MA 01742-9133