Ex Parte Isaacs et al

Patent Trial and Appeal BoardJun 28, 2016

10491112 (P.T.A.B. Jun. 28, 2016)

UNITED STA TES p A TENT AND TRADEMARK OFFICE APPLICATION NO. FILING DATE FIRST NAMED INVENTOR 10/491,112 10/01/2004 John Isaacs 27162 7590 06/29/2016 CARELLA, BYRNE, CECCHI, OLSTEIN, BRODY & AGNELLO 5 BECKER FARM ROAD ROSELAND, NJ 07068 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 ATTORNEY DOCKET NO. CONFIRMATION NO. 695458-114 6163 EXAMINER SKELDING, ZACHARY S ART UNIT PAPER NUMBER 1644 MAILDATE DELIVERY MODE 06/29/2016 PAPER Please find below and/or attached an Office communication concerning this application or proceeding. The time period for reply, if any, is set in the attached communication. PTOL-90A (Rev. 04/07) UNITED STATES PATENT AND TRADEMARK OFFICE BEFORE THE PATENT TRIAL AND APPEAL BOARD Ex parte JOHN ISAACS, HERMAN WALDMANN, and GEOFFREY HALE 1 Appeal2013-009136 Application 10/491, 112 Technology Center 1600 Before ERIC B. GRIMES, ULRIKE W. JENKS, and RACHEL H. TOWNSEND, Administrative Patent Judges. JENKS, Administrative Patent Judge. DECISION ON APPEAL This is an appeal under 35 U.S.C. Â§ 134 involving claims directed to a method of treating chronic joint inflammation due to rheumatoid arthritis by administering an anti-CD3 antibody having a mutated Fe region. The Examiner rejects the claims as anticipated and obvious. We have jurisdiction under 35 U.S.C. Â§ 6(b ). We AFFIRM. 1 According to Appellants, the Real Party in Interest is Glaxo Group Limited. (Br. 1.) Appeal2013-009136 Application 10/491,112 STATEMENT OF THE CASE Claims 14--21, 27-30, 32, 33, 35-37, 40-44, 46-48, and 50-52 are on appeal, 2 and can be found in the Claims Appendix of the Appeal Brief. Claim 51 is representative of the claims on appeal, and reads as follows: 51. A method of treating chronic joint inflammation in a human patient having rheumatoid arthritis comprising administering to a human patient in need of said treating a therapeutically effective dose of an anti-CD3 antibody, wherein said antibody is mutated in the F c region to reduce binding to Fe receptors. (Br. 27 (Claims Appendix.) The following grounds of rejection are before us for review: I. claims 28-30, 32, 33, 35-37, 40-44, 46-48, and 51under35 U.S.C. Â§ 103(a) as unpatentable over Bach3 in view of Smith, 4 Hughes, 5 Malfait6 Â· ' II. claims 14--21, 27, 50, and 52 under 35 U.S.C. Â§ 103(a) as unpatentable over Bach in view of Smith, Hughes, 1\1alfait, and further in view ofWaldmann7; and 2 Claim 25 is withdrawn as being directed to a non-elected species (see Final Act. 2; Ans. 3). 3 Bach et al., CA 2,224,256, published June 9. 1999 ("Bach") 4 Smith et al., WO 98/47531, published Oct. 29, 1998 ("Smith"). 5 Hughes et al., Induction of T Helper Cell Hyporesponsivness in an Experimental Model of Autoimmunity by Using Nonmitogenic Anti-CD3 Monoclonal Antibody, 153 J. IMMUN. 3319-3325 (1994) ("Hughes"). 6 Malfait et al., Chronic Relapsing Homologous Collagen-Induced Arthritis in DBN/l Mice as a Model for Testing Disease-Modifying and Remission- Inducing Therapies, 44 ARTH. &RHEUM. 1215-1224 (2001) ("Malfait"). 7 Waldmann et al., WO 00/05268, published Feb. 3, 2000 ("Waldmann"). 2 Appeal2013-009136 Application 10/491,112 III. claims 40-44, 46, 47, and 51under35 U.S.C. Â§ 102(b) as being anticipated by Tso 8 as evidenced by Kraan. 9 I. & II. Obviousness over Bach, Smith, Hughes, and Malfait There are two obviousness rejections, but both rely on the combined teachings of Bach, Smith, Hughes, and Malfait, so we will discuss them together. Because the claims are not separately argued, we focus our discussion on representative claim 51. The issue is: Does the preponderance of evidence of record support the Examiner's conclusion that using anti-CD3 antibodies having a mutated Fe region in human patients with rheumatoid arthritis (RA) would have a reasonable expectation of treating patients having chronic joint inflammation? Findings of Fact We adopt the Examiner's findings of fact and reasoning regarding the scope and content of the prior art (see Final Act. 3-9 10; Office Act. 5-21 11 ; Ans. 4--42). For emphasis only we highlight the following: FF 1. Bach teaches "[a] method of treating spontaneous and ongoing autoimmune diseases in mammals, comprising administering to a mammal, in need of such a treatment, a therapeutically effective amount of one or more non mitogenic anti-CD3 active principles to achieve permanent disease remission through the induction of antigen- 8 Tso et al., US 5,834,597, issued Nov. 10, 1998 ("Tso"). 9 Kraan et al., Asymptomatic Synovitis Precedes Clinically Manifest Arthritis, 41 Arth. & Rheum. 1481-1488 (1998) ("Kraan"). 1Â° Final Office Action, mailed Feb. 16, 2012 ("Final Act."). 11 Office Action, mailed July 14, 2011 ("Office Act."). 3 Appeal2013-009136 Application 10/491,112 specific unresponsiveness, i.e. immune tolerance" (Bach 11, 12 claim 1, see Abstract; Office Act. 5). Autoimmune diseases treated with the antibody include rheumatoid arthritis (Bach 12, claim 1 O; Office Act. 5). The antibody dosage is 5 to 20 mg (Bach 14, claim 29; Office Act. 6) FF2. The Examiner finds that Bach does not "teach the use of an anti-CD3 antibody that has been a mutated in the Fe region" (Office Act. 6). FF3. The Examiner finds that "Smith teaches anti-CD3 antibodies mutated in the Fe region to reduce Fe [receptor] binding" (Office Act. 6; see Smith 88 ("a 'humanized' mAb derived from OKT3 and bearing mutations of 2 amino acids in the Fe portion to impede its binding to FcTRs does not induce human T cell activation in vivo in a preclinical model, but retains the immunosuppressive properties of the native mAb")). FF4. Hughes teaches that treatment with "nmCD3 [(anti-CD3 mAb )] delayed the onset and reduced the severity of arthritis in mice immunized with type II collagen (CII)" (Hughes, Abstract; Office Act. 6). "F(ab')2 fragments of 145-2Cl 1 were prepared by incubating purified mAb with pepsin" (Hughes, 3320). FF5. Hughes teaches that "[t]he first dose of mAb or PBS was administered at the same time as the first CII immunization" (Hughes, 3320). FF6. Malfait teaches that "[t]he chronic relapsing form of CIA [collagen- induced arthritis] more closely resembles RA" (Malfait 1221). 12 The claims section of Bach lacks page numbers but the descriptive section ends on page 10. We therefore consider the first page of claims to be page 11, and number the remaining pages consecutively. 4 Appeal2013-009136 Application 10/491,112 "Chronic relapsing CIA starts as a milder disease than classic CIA" (id.). Malfait suggests that "the chronic model could be used after initial screening of a candidate treatment in classic CIA in order to confirm the therapeutic effect in a chronic relapsing arthritis" (id. at 1223.) FF7. Malfait shows that "[t]wo injections of ... [anti-CD3 plus anti-TNF] antibodies at disease onset suppressed the arthritis for the entire duration of the experiment" (Malfait 1221; Office Act. 6). The anti- CD3 antibody used in the experiment is "145-2C 11 hamster IgG 1" (Malfait 1216, therapeutic agents). FF8. The Specification discloses that "[t]he dose of antibody to be administered to a patient will depend on the condition of the patient and will be at the discretion of the attendant physician." (Spec. 13: 12-14; see Final Act. 3; Office Act. 7.) FF9. Kraan "hypothesized that asymptomatic synovitis may precede the clinical manifestations of RA [rheumatoid arthritis] and that so-called early RA is already a chronic disease. This is supported by the observation that a notable percentage of RA patients have signs of joint destruction at the time of initial diagnosis" (Kraan 1481 ). Kraan used a monkey model to study synovial biopsy during the progression of the disease. "The results clearly indicate that synovial inflammation is present before the joints become painful and swollen" (Kraan 1487). Thus, "when the patient gets signs and symptoms of RA, infiltration with inflammatory cells that may induce joint destruction have been present in the joints for a while" (Kraan 1488). 5 Appeal2013-009136 Application 10/491,112 FFIO. Kraan teaches that "[i]t is obvious that prevention of disability in RA patients may be more successful when down-modulation of the process underlying joint destruction is achieved in early phases rather than in later phases of the disease" (Kraan 1488). Principle of Law "Obviousness does not require absolute predictability of success." In re O'Farrell, 853 F.2d 894, 903 (Fed. Cir. 1988); see also Hoffmann-La Roche Inc. v. Apotex Inc., 748 F.3d 1326, 1331 (Fed. Cir. 2014) ("Conclusive proof of efficacy is not necessary to show obviousness."). The expectation of success need only be reasonable. Pfizer, Inc. v. Apotex, Inc., 480 F.3d 1348, 1364 (Fed. Cir. 2007) ([A] rule of law equating unpredictability to patentability ... would mean that any new salt-including those specifically listed in the [prior art patent] itself-would be separately patentable, simply because the formation and properties of each salt must be verified through testing. This cannot be the proper standard since the expectation of success need only be reasonable, not absolute.). Analysis We adopt the Examiner's findings and conclusion and agree with the Examiner's responses to Appellants' contentions (see Final Act. 3-9; Office Act. 5-21; Ans. 4--42; see FF1-FF7). To summarize, Bach tells one of ordinary skill in the art to treat autoimmune disease, such as rheumatoid arthritis, with anti-CD3 monoclonal antibodies and fragments thereof (FFl ). The Examiner acknowledged that Bach does not disclose antibodies with mutated Fe regions (FF2) and relies on the other three references to support the use of such antibodies (FF3-FF7). The Examiner concludes that it 6 Appeal2013-009136 Application 10/491,112 would have been obvious to one of ordinary skill in the art "to employ the non-mitogenic anti-CD3 antibodies of Smith to treat rheumatoid arthritis since these antibodies lack the toxicity of mitogenic anti-CD3 antibodies and yet retain the potential for 'Th2 cytokine deviation' and therefore for 'suppressing Thi-mediated autoimmune diseases,' as taught by Smith" (Final Act. 6-7). We agree with the Examiner's reasoning and conclusion and find that the combination of Bach, Smith, Hughes, and Malfait cited by the Examiner provides a reasonable expectation of treating chronic joint inflammation associated with rheumatoid arthritis by administering an anti- CD3 antibody having a mutated Fe region as claimed. We address Appellants' arguments below. Appellants contend that "[ t ]he present invention differs from the prior art in that the present invention is defined as treatment of 'chronic joint inflammation in a human patient having rheumatoid arthritis.' This chronic phase of rheumatoid arthritis occurs later in the disease progression after the acute inflammation processes ... have failed to resolve." (Br. 4--5); and that animal models do not provide predictive correlation of success in treating chronic joint inflammation of rheumatoid arthritis with T-cell antibodies in humans (id. at 4--20; see id. at 6 ("animal models of chronic human diseases are especially imperfect")). Specifically, according to Appellants, because the "exact role of T-cells and specific T-cell subsets in early and in established disease remains unclear, [and] their important interactions with other cell subsets have [not] been sufficiently clarified to predict clinical responses on the basis of cell type or cell surface antigen targeted, and "animal models of rheumatoid arthritis were shown not to be predictive of success with respect to anti-CD4, anti-CDS, anti-CD7, and CAMPATH-1 7 Appeal2013-009136 Application 10/491,112 (anti-CD52) antibodies in clinical trials" (Br. 11, citing the Strand Declaration 13), the animal models of Hughes and Malfait, "which teach the treatment of arthritis at or before the onset [of chronic joint inflammation] with an anti-CD3 antibody[,] do not create a reasonable expectation of treating successfully chronic joint inflammation in a human rheumatoid arthritis patient" (id. at 13). We are not persuaded. Appellants' argument is grounded in the position that "treating chronic joint inflammation in a human patient having rheumatoid arthritis," as required by claim 51, is fundamentally different than the prior art teaching of treating rheumatoid arthritis. We find the prior art supports the Examiner's position to the contrary. The Examiner cites Kraan as evidence that by the time one is identified as having rheumatoid arthritis, the disease in the joint of that patient is already considered chronic, and, thus, one cannot distinguish "'treating chronic joint inflammation in a human patient having rheumatoid arthritis' from the obviousness of treating [a patient identified as having] rheumatoid arthritis" (Ans. 7; see FF9 & FFlO). As explained by the Examiner, "even before a patient steps into a clinic reporting the presence of painful and swollen joints for the first time, i.e., even prior to the outward symptoms of clinically manifest joint inflammation, the joints of rheumatoid arthritis patients are already subject to chronic inflammation." (Ans. 7 .) We find Kraan supports the Examiner's interpretation that a patient with rheumatoid arthritis is a patient that already has chronic inflammation (Kraan 1481-1482, 1487-88; FF9 and FFlO), and, thus, the teaching in the prior art of treating inflammation in a patient 13 Declaration by Dr. Vibeke Strand signed Oct. 8, 2009, submitted on Information Disclosure Statement May 6, 2010 ("Strand Dec."). 8 Appeal2013-009136 Application 10/491,112 identified as having rheumatoid arthritis with anti-CD3 antibodies, i.e., Bach, Hughes, and Malfait, necessarily involves treating chronic joint inflammation. We also disagree with Appellants position that Hughes and Malfait cited by the Examiner do not provide a reasonable expectation of treating chronic joint inflammation associated with rheumatoid arthritis. First, animal testing remains generally recognized as a valuable tool in the screening for agents for the application to human diseases, even for treating human patients identified as having rheumatoid arthritis, and thus, chronic joint inflammation. It is important to point out that animal models, generally, sort therapies into two groups: those that have the potential to work and those that do not work. Although successful treatments in animal models may not be absolutely predictive of success when applied to humans, these models remain "useful for identification of therapeutic agents for RA" (Ans. 12 (citing the Williams Declaration 14)). On the other hand, a negative result in an animal model usually evinces a reason not to pursue application of that substance in the modeled disease state. Malfait teaches two types of animal models the chronic relapsing CIA and the more traditional collagen induced model (FF6 and FF7). Malfait suggests using the chronic relapsing CIA model after the initial screening with the traditional model (FF6). The Examiner explains: [ t ]he teachings of Malfait that are of primary relevance to the prima facie case of obviousness ... are that in the homologous collagen induced arthritis animal model[, the chronic relapsing 14 Declaration by Dr. Richard Williams, submitted on Information Disclosure Statement Oct. 1, 2010 ("Williams Dec."). 9 Appeal2013-009136 Application 10/491,112 CIA ofMalfait,] ... administration of two doses of anti-CD3 and anti-TNFa antibodies at the onset of outward symptoms of clinically manifest joint inflammation (days 28 and 32), induced complete remission for the duration of the experiment. (Ans. 14; see FF7.) "[T]he collagen induced arthritis mouse model was (and is) a widely used, art accepted protocol for determining if a given therapeutic agent would be reasonably expected to successfully treat a human patient" (Ans. 12). The Examiner explains that the failure of using depleting antibodies, e.g., anti-CD4, anti-CDS, anti-CD7, and CAMPATH-1 antibodies, does not negate the teachings in the art with respect to the non- depleting anti-CD3 antibodies because the mechanism of action differs between the two types of antibodies (see Ans. 26, 28, 41). We agree with the Examiner's conclusion that the success shown using anti-CD3 antibodies in the art in "treating rheumatoid arthritis in a collagen induced arthritis mouse model prior to, or just after disease onset, ... recognizes that such an antibody will be reasonably expected to successfully treat a human rheumatoid arthritis patient" as well (Ans. 16). Importantly, a finding of "[ o ]bviousness does not require absolute predictability of success." In re O'Farrell, 8S3 F.2d at 903. As further explained by the Examiner the failure in treating rheumatoid arthritis with anti-CD4 and -CDS antibodies is due to "a variety of technical reasons, [for example that] the patients did not receive sufficiently high doses of depleting antibody to substantively affect the pathogenic T cells in their synovial tissue" (Ans. 27 (emphasis removed)). "[T]he primary publications describing these clinical 'failures' do not teach or suggest depleting anti-CD4, -CDS or ---CDwS2 antibodies failed to demonstrate therapeutic efficacy because CD4+ or CDS+ or CDwS2+ T 10 Appeal2013-009136 Application 10/491,112 cells are unimportant in disease pathology" (Ans. 27 (emphasis removed)). Thus, T-cells remain important targets in the disease pathology. As explained by the Examiner "it is significant that non-depleting anti-CD4 antibodies exert their effects via immunomodulatory-type mechanisms, such as CD4 downmodulation" (Ans. 27). This is the same mechanism of action as that of anti-CD3 antibodies (id.). We agree with the Examiner's conclusion that "the knowledge of one of ordinary skill in the art pertaining to the use of anti-T cell antibodies to treat rheumatoid arthritis would not have negated the reasonable expectation of success that one of ordinary skill would have had for treating rheumatoid arthritis with an anti-CD3 antibody in view of the prior art teachings of Bach, Smith, Hughes and Malfait" (Ans. 28). Additionally, Appellants contend that "Kraan teaches away from the present invention by stating that rheumatoid arthritis needs to be treated before it has become chronic" (Br. 8). We are also not persuaded by Appellants contention with respect to the teachings of Kraan. Although we recognize that Kraan suggests the desirability to target treatment early in the disease process underlying joint destruction to prevent disability (FF 10), a recognition that prevention of disability is desirable does not mean that prevention of disability has to occur before development of chronic inflammation. (FF9; see Ans. 13). Kraan explains that "when the patient gets signs and symptoms of RA, infiltration with inflammatory cells that may induce joint destruction have been present in the joints for a while" (FF9 and FFlO). We agree with the Examiner that teaching the desire to identify a patient early in the disease 11 Appeal2013-009136 Application 10/491,112 process, even before symptoms arise (see Ans. 12-13), does not teach away from treating rheumatoid arthritis after the presentation of disease. On the record before us, we conclude the Examiner did not err in rejecting claim 51under35 U.S.C. Â§ 103(a) as being unpatentable over the combination of Bach, Smith, Hughes, and Malfait. Claims 28-30, 32, 33, 35-37, 40-44, and 46-48 were not separately argued and fall with claim 51. Appellants have waived arguments directed to Waldmann (see Br. 22), and therefore we also affirm the rejection of claims 14--21, 27, 50, and 52 under 35 U.S.C. Â§ 103(a) as unpatentable over Bach in view of Smith, Hughes, Malfait, and further in view of Waldmann. III. Anticipation by Tso The issue is: Does the preponderance of the evidence of record support the Examiner's conclusion that treating patients having symptoms of rheumatoid arthritis with an anti-CD3 antibody having Fe region mutation necessarily treats a chronic inflammation as claimed? Findings of Fact FFl 1. Tso teaches antibodies having mutated IgG2 constant regions comprising a nonnaturally occurring segment of amino acids between residues 234 and 237 defined by the EU numbering system. Anti-CD3 antibodies incorporating such IgG2 constant regions can specifically bind to CD3 antigens on T-cells without inducing a mitogenic response in the T-cells through specific binding to Fey receptors. The immunoglobulin specifically binds to a CD3 antigen on the surface of T cells and usually has a binding affinity having a lower limit of about 107 M-1 and an upper limit of about five- 12 Appeal2013-009136 Application 10/491,112 times the binding affinity of the M291 immunoglobulin. (Tso 2: 15-21.) FF12. Tso teaches Pharmaceutical compositions comprising [the anti-CD3] antibodies ... are useful for parenteral administration ... [for] conditions manifesting undesired immune responses ... . Exemplary autoimmune diseases are rheumatoid arthritis, multiple sclerosis, type I diabetes, system[ic] lupus erythematosus and inflammatory bowel disease. (Tso 11: 56-67 (emphasis added).) FF13. Tso teaches that the anti-CD3 "antibodies can be administered for prophylactic and/or therapeutic treatments .... Amounts effective for this use depend upon the severity of the condition and the general state of the patient's own immune system, but generally range from about 0.01 to about 100 mg of antibody per dose." (Tso 12: 25-35.) Principle of Law "[A] reference may anticipate even when the relevant properties of the thing disclosed were not appreciated at the time." Abbott Labs. v. Baxter Pharm. Products, Inc., 471 F.3d 1363, 1367 (Fed. Cir. 2006). Discovery of a property inherent to a prior art process does not render that process patentable, even if the prior art did not appreciate the property. Verdegaal Bros. Inc. v. Union Oil Co., 814 F.2d 628, 633 (Fed. Cir. 1987). Analysis The Examiner finds, and Appellants do not contest, that Tso' s "antibodies [anti-CD3 antibodies mutated in the Fe region to reduce binding to Fe receptors] may be used to treat rheumatoid arthritis" (Ans. 42; Br. 22 ("Tso teaches that these antibodies may be used to treat rheumatoid arthritis"); see FF11-FF13). The Examiner acknowledges that Tso does not 13 Appeal2013-009136 Application 10/491,112 discuss "which stage of rheumatoid arthritis may be treated with Tso' s antibodies" (Ans. 42). The Examiner, however, points to the teachings of Kraan to evidence "that all rheumatoid arthritis patient[ s] are considered to have 'chronic joint inflammation' when they first present with clinically evident disease" (id.). The Examiner reasons that "in treating any patient with clinically evident rheumatoid arthritis according to the teachings of Tso one or ordinary skill in the art is necessarily practicing the claimed invention" (id. at 43). Appellants, however, contend that "no information is provided by Tso as to which stage of rheumatoid arthritis may be treated with Tso' s antibodies" (Br. 22). According to Appellants Kraan teaches "that rheumatoid arthritis must be treated before it has become chronic" (id. at 22- 23). We are not persuaded by Appellants' contentions that Tso's disclosure does not encompass treating chronic joint inflammation in the patient with rheumatoid arthritis as claimed. As explained by the Examiner, by the time patients seek treatment for rheumatoid arthritis their condition is already chronic (FF9). Although Kraan discloses that it may be beneficial to try and treat the disease early before cartilage destruction (FF 10), we agree with the Examiner's assessment that "[t]here are no teachings in Kraan 'that rheumatoid arthritis must be treated before it has become chronic' as asserted by applicant" (Ans. 42). Indeed, Kraan explains that the condition is considered chronic long before clinical symptoms appear (FF9) and early diagnosis would be beneficial for prevention and to mitigate the destruction of tissue (FFlO). We agree with the Examiner that treating patients having 14 Appeal2013-009136 Application 10/491,112 rheumatoid arthritis as taught in Tso would necessarily treat chronic joint inflammation associated with rheumatoid arthritis. On the record before us, we conclude the Examiner did not err in rejecting claim 51under35 U.S.C. Â§ 102(b) as anticipated by Tso. Claims 40-44, 46, and 4 7 were not separately argued and fall with claim 51. SUMMARY We affirm the rejection of claim 51 under 35 U.S.C. Â§ 103(a) over Bach, Smith, Hughes, and Malfait. Claims 28-30, 32, 33, 35-37, 40-44, and 46-48 were not argued separately and fall with claim 51. We affirm the rejection of claims 14--21, 27, 50, and 52 rejected under 35 U.S.C. Â§ 103(a) over Bach in view of Smith, Hughes, Malfait, and further in view of Waldmann. We affirm the rejection of claim 51under35 U.S.C. Â§ 102(b) by Tso as evidenced by Kraan. Claims 40-44, 46, and 47 were not separately argued and fall with claim 51. 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. Â§ 1.136(a). AFFIRMED 15