Ex Parte DeLuca et alDownload PDFPatent Trial and Appeal BoardNov 1, 201211231049 (P.T.A.B. Nov. 1, 2012) Copy Citation UNITED STATES PATENT AND TRADEMARK OFFICE __________ BEFORE THE PATENT TRIAL AND APPEAL BOARD __________ Ex parte HECTOR F. DELUCA, EHREN N. RUDOLPH, LAURA MCCARY BLOSS, and JULIA B. ZELLA __________ Appeal 2012-001735 Application 11/231,049 Technology Center 1600 __________ Before JEFFREY N. FREDMAN, ERICA A. FRANKLIN, and SHERIDAN K. SNEDDEN, Administrative Patent Judges. SNEDDEN, Administrative Patent Judge. DECISION ON APPEAL This is an appeal under 35 U.S.C. § 134 involving claims to methods of delaying the onset of Type I diabetes. The Examiner has rejected the claims as obvious. We have jurisdiction under 35 U.S.C. § 6(b). We affirm. Appeal 2012-001735 Application 11/231,049 2 STATEMENT OF THE CASE According to Appellants, the invention relates to methods of delaying the onset of diabetes by administering a vitamin D compound during a detectable treatment window. (See e.g., Specification, 3.) Specifically, a patient is treated “after the development of at least two autoantibodies associated with diabetes, most notably selected from autoantibodies to insulin, glutamic acid decarboxylase, or insulinoma-associated protein” and “before the patient has developed a blood glucose level of 150 mg/dl.” (Id.) Claims 1-6, 8-12 and 14-15 are on appeal. The claims have not been argued separately and therefore stand or fall together. 37 C.F.R. § 41.37(c)(1)(vii). Claim 1 is representative and reads as follows 1. A method of delaying the onset of Type I diabetes or symptoms thereof in a human patient, comprising: detecting the presence of at least two autoantibodies indicative of Type I diabetes in the patient, and, orally administering to the patient a therapeutically effective amount of a vitamin D compound, wherein the vitamin D compound is administered to the patient before the patient's blood sugar level increases to 150 mg/dl, the blood sugar level measured as an average of 5 samples taken throughout a day at least 2 hours apart, wherein the onset of Type I diabetes or diabetes symptoms thereof is delayed. The claims stand rejected as follows: I. Claims 1-6, 8-12 and 14-15 under 35 U.S.C. 103(a) as being unpatentable over the combination of Mathieu et al. (U.S. Patent 5,665,387, issued Sep. 9, 1997), Ziegler et al. (Autoantibody Appearance and Risk for Development if Childhood Diabetes in Offspring of Parents With Type 1 Diabetes, 48 DIABETES 460-468 Appeal 2012-001735 Application 11/231,049 3 (1999)) and Khalil (Spectroscopic and Clinical Aspects of Noninvasive Glucose Measurements, 45 CLINICAL CHEMISTRY 165- 177 (1999)). I. Issue The Examiner concludes that the claimed subject matter is obvious over the combined prior art. (See Ans. 7.) Appellants contend that “the skilled artisan considering Mathieu, Ziegler and Khalil at the time of the invention would not have a reasonable likelihood of success in shifting the early treatment window taught by Mathieu until after at least two autoantibodies are detected in the patient, as required by the rejected claims.” (App. Br. 10.) The issue is: Does the evidence of record support the Examiner‟s conclusion that the combination of Mathieu, Ziegler and Khalil render obvious the method of claim 1? Findings of Fact FF1. The Examiner finds that [s]ince Mathieu teaches the administration of 1α, 25- dihydroxyvitamin D3 (1, 25(OH)2 D3) and it is known in the art that autoantibodies to β-cell antigens precede the development of type 1 diabetes and are commonly used as sensitive markers to identify the preclinical period of diabetes type I with the fact that autoimmune destruction of β-cells leads to Type I diabetes as taught by Ziegler, one of ordinary skills would expect that in testing an individual for the autoantibodies in order to begin the Appeal 2012-001735 Application 11/231,049 4 administration of 1α, 25-dihydroxyvitamin D3 (1, 25(OH)2 D3) to inhibit the destruction of β-cells, which is known to cause Type I diabetes. (Ans. 8-9.) FF2. Mathieu discloses as follows: The invention thus relates to a method for treating primary autoimmune diabetes by administering a suitable dose of one or more vitamin D (analogue(s)) during a suitable period of time to a subject who has a predisposition to develop autoimmune diabetes. The vitamin D analogue(s) is/are administered in an amount to modulate the immune system in an animal or patient to which the amount is administered. A large number of other analogues of 1α,25(OH)2D3 which display a dissociation of their potency to induce cell differentiation/immune effects and their calcemic effects in vivo, have a variable degree of similar protective effects and are able to induce primary or secondary prevention of type I diabetes. (Mathieu, col. 2, ll. 36-41; emphasis added.) FF3. The Examiner finds that “Mathieu does not expressly teach the detection of at least two autoantibodies or testing blood sugar levels an average of 5 times daily.” (Ans. 6.) FF4. The Examiner finds that “Ziegler teaches that autoantibodies to β-cell antigens precede the development of type 1 diabetes and are commonly used as sensitive markers to identify the preclinical period of diabetes type I” and that that “[o]ne would have been motivated to detect at least two autoantibodies” based on the teachings of Ziegler. (Id.) FF5. Zeigler discloses the results of a study “to determine autoantibody distributions and the chronology of antibody appearance from Appeal 2012-001735 Application 11/231,049 5 birth in offspring of parents with type 1 diabetes” and found that “[r]isk for type 1 diabetes was highest in those with more than one islet autoantibody.” (Zeigler, p. 465, left col.) FF6. Zeigler discloses as follows: In conclusion, our data demonstrate that autoimmunity in children of parents with type 1 diabetes is initiated very early in life, with a first peak of antibody appearance by the age of 2 years, that IAAs are present in the majority of these children in the first sample with autoantibodies, and that the detection of multiple antibodies at 2 years of age in offspring of parents with type 1 diabetes is associated with a high risk of progression to disease by age 5 years. These findings need to be confirmed in studies from the general population, but with this knowledge, new concepts of screening programs and intervention strategies aiming to modulate the early stage of the disease process may be considered. (Zeigler, ¶ spanning pp. 467 and 468; emphasis added.) Principles of Law “Obviousness does not require absolute predictability of success .... For obviousness under § 103, all that is required is a reasonable expectation of success.” In re O’Farrell, 853 F.2d 894, 903-904 (Fed. Cir. 1988). A critical step in analyzing these expectations is “casting the mind back to the time of invention, to consider the thinking of one of ordinary skill in the art, guided only by the prior art references and the then-accepted wisdom in the field.” In re Kotzab, 217 F.3d 1365, 1369 (Fed. Cir. 2000). Appeal 2012-001735 Application 11/231,049 6 Analysis Appellants contend that Mathieu does not inform a person of ordinary skill in the art “„that 1α, 25(OH)2 D3 and analogs of 1α, 25(OH)2 D3 can delay the onset of diabetes even after indicators of diabetes, such as insulitis or the presence of autoantibodies to insulin, have been detected.‟” (App. Br. 8, quoting Declaration of Dr. DeLuca, submitted Nov. 18, 2009.) Appellants further argue that “[a]lthough Ziegler indicates that the appearance of autoantibodies correlates to a higher risk of contracting diabetes at a later time, it does not speak to the predictability or success of shifting a diabetes treatment regimen to a later time frame.” (App. Br. 8.) We are not persuaded by Appellants‟ arguments. Rather, we agree with the fact finding and analysis of the Examiner which we adopt as our own. (Ans. 5-15.) In particular, we note that, for obviousness under § 103, all that is required is a reasonable expectation of success. In re O’Farrell, 853 F.2d at 904. Here, Mathieu teaches the ability of vitamin D compounds to induce primary or secondary prevention of Type I diabetes and that these compounds may be administered to subjects who have a predisposition to developing autoimmune diabetes. (FF2.) Zeigler teaches that the risk for subjects having a predisposition to developing autoimmune diabetes is highest in those with more than one islet autoantibody. (FF5 and FF6.) Thus, we agree with the Examiner‟s conclusion that a person of ordinary skill in the art would have had a reasonable expectation of success in treating subjects identified as high risk using the techniques of Zeigler with vitamin D compounds, which are taught by Mathieu to be useful in prevention of autoimmune diabetes. (See e.g., FF1 and FF4.) Appeal 2012-001735 Application 11/231,049 7 While we acknowledge the expertise of Dr. Hector DeLuca, we find that the Declaration does not carry significant persuasive weight. In re Am. Acad. Of Sci. Tech Ctr., 367 F.3d 1359, 1368 (Fed. Cir. 2004) (“The Board has broad discretion as to the weight to give to declarations offered in the course of prosecution.”) In particular, we note that the Declaration fails to consider what the combined teachings of the prior art would have taught a skilled artisan regarding the predictability or success of delaying the onset of Type 1 diabetes or symptoms in a human patient upon detection of the presence of at least two autoantibodies indicative of Type 1 diabetes in the patient. That is, Mathieu expressly teaches administering vitamin D analogs to “a subject who has a predisposition to develop autoimmune diabetes” (Mathieu, col. 2, ll. 36-41; FF 2) and Ziegler teaches that the “[r]isk for type 1 diabetes was highest in those with more than one islet autoantibody.” (Zeigler, p. 465, left col.; FF 5). Therefore, contrary to the Declaration, Ziegler establishes a predisposition for autoimmune diabetes when more than one autoantibody is present in a patient (FF 5) and Mathieu teaches administering vitamin D analogs to patients with a predisposition for autoimmune diabetes, which together reasonably provide a reason and expectation of success in treating Ziegler‟s at risk patients with Mathieus vitamin D analogs. Appeal 2012-001735 Application 11/231,049 8 Conclusion of Law The evidence of record supports the Examiner‟s conclusion that the combination of Mathieu, Ziegler and Khalil renders obvious the method of claim 1. SUMMARY We affirm the rejection of claim 1 under 35 U.S.C. 103(a) as being unpatentable over the combination of Mathieu, Ziegler and Khalil. Pursuant to 37 C.F.R. § 41.37(c)(1)(vii)(2006), we also affirm the rejection of claims 2-6, 8-12 and 14-15, as these claims were not argued separately. AFFIRMED cdc Copy with citationCopy as parenthetical citation
