12343922 (P.T.A.B. Aug. 31, 2016)

Ex Parte WU

Patent Trial and Appeal BoardAug 31, 2016

12343922 (P.T.A.B. Aug. 31, 2016)

UNITED STA TES p A TENT AND TRADEMARK OFFICE APPLICATION NO. FILING DATE 12/343,922 12/24/2008 2292 7590 09/02/2016 BIRCH STEW ART KOLASCH & BIRCH, LLP POBOX747 FALLS CHURCH, VA 22040-0747 FIRST NAMED INVENTOR Rong-Tsun WU 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. 5992-0123PUS 1 5249 EXAMINER OLSON, ERIC ART UNIT PAPER NUMBER 1673 NOTIFICATION DATE DELIVERY MODE 09/02/2016 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): mailroom@bskb.com PTOL-90A (Rev. 04/07) UNITED STATES PATENT AND TRADEMARK OFFICE BEFORE THE PATENT TRIAL AND APPEAL BOARD Ex parte RONG-TSUN WU1 Appeal2014-003135 Application 12/343,922 Technology Center 1600 Before ERIC B. GRIMES, JEFFREY N. FREDMAN, and RICHARD J. SMITH, Administrative Patent Judges. GRIMES, Administrative Patent Judge. DECISION ON APPEAL This is an appeal under 35 U.S.C. Â§ 134 involving claims to therapeutic methods, which have been rejected as anticipated and obvious. We have jurisdiction under 35 U.S.C. Â§ 6(b). We affirm. STATEMENT OF THE CASE The Specification discloses an extract from Polygonum multiflorum in which "the major component was 2,3,5,4' -tetrahydroxystilbene 2-0-B-D- glucopyranoside," which is also referred to in the Specification as 1 Appellant identifies the Real Party in Interest as National Yang-Ming University. (Br. 1.) Appeal 2014-003135 Application 12/343,922 "compound A." (Spec. 9-10.) Compound A is disclosed to enhance kidney expression of erythropoietin (Epo ), enhance kidney function, and increase liver expression of both Epo and hepatocyte growth factor. (Id. at 12-13, 15, 17.) Epo is an erythropoiesis-stimulating agent. (Id. at 2.) Claims 1-3 and 7-13 are on appeal. Claim 1 is illustrative and reads as follows: 1. A method for enhancing erythropoietin formation in a subject in need thereof comprising the step of administering to the subject an effective amount of a compound of the formula: HO~.Â·.-.-.-.-.-.-.-./;. IÂ·Â·Â·Â·Â·Â·Â·Â·Â·Â·~ - )H ~~--------\\ / OH en wherein R is a glycosyl group. Claims 8, 10, and 12 are also independent and are directed to a method of enhancing erythropoiesis (claim 8), a method of enhancing kidney function (claim 10), and a method of enhancing the expression of hepatocyte growth factor (claim 12), in subjects in need thereof, but are otherwise identical to claim 1. 2 Appeal 2014-003135 Application 12/343,922 The claims stand rejected as follows: Claims 1, 2, 7, and 10-13 under 35 U.S.C. Â§ 102(b) as anticipated by Wang,2 as evidenced by Chong3 and Hayat,4 or alternatively under 35 U.S.C. Â§ 103(a) as obvious based on Wang, Chong, and Hayat (Ans. 2, 7); Claims 1-3 and 10-13 under 35 U.S.C. Â§ 102(b) as anticipated by Kimura, 5 as evidenced by Yazihan6 and Hayat, or alternatively under 35 U.S.C. Â§ 103(a) as obvious based on Kimura, Yazihan, and Hayat (Ans. 4, 8); and Claims 1-3 and 8-13 under 35 U.S.C. Â§ 102(b) as anticipated by Wu7 as evidenced by Kim8 and Hayat (Ans. 5). 2 R. \"X/ ang et al., Changes in hippocampal S}'napses and learning-memo!}' abilities in age-increasing rats and effects of tetrahydroxystilbene glucoside in aged rats, 149 NEUROSCIENCE 739--46 (2007). 3 Zhao Zhong Chong et al., Erythropoietin Requires NF-KB and its Nuclear Trans location to Prevent Early and Late Apoptotic Neuronal Injury During /J-Amyloid Toxicity, 2 CURR NEUROVASC RES. 387-99 (2005). 4 Amir Hayat et al., Erythropoietin stimulating agents in the management of anemia of chronic kidney disease, 2 PATIENT PREFERENCE AND ADHERENCE 195-200 (2008). 5 Yoshiyuki Kimura et al., Effects of Stilbene Components of Roots of Polygonum ssp. On Liver Injury in Peroxidized Oil-fed Rats, 49 JOURNAL OF MEDICINAL PLANT RESEARCH 51-54 (1963). 6 Nuran Yazihan et al., Erythropoietin attenuates hydrogen peroxide- induced damage of hepatocytes, 18 TURK. J. GASTROENTEROL. 239--44 (2007). 7 Wu, US 2005/0042314 Al, published Feb. 24, 2005. 8 Hyun Ki Kim et al., A New Stilbene Glucoside Gallatefrom the Roots of Polygonum multiflorum, 31 ARCH. PHARM. RES. 1225-29 (2008). 3 Appeal 2014-003135 Application 12/343,922 I The Examiner has rejected claims 1, 2, 7, and 10-13 as anticipated by Wang, as shown by Chong and Hayat, or as obvious based on these three references. The Examiner finds that Wang discloses administration of 2,3,5,4' -tetrahydroxystilbene-2-0-B-D-glucoside, or TSG, to reduce age- related neurodegeneration. (Ans. 2-3.) The Examiner finds that TSG reversed loss of synapses in the brains of the treated rats, and "[t]his synapse loss is considered to be a model of cognitive decline in Alzheimer's disease." (Id. at 3.) The Examiner cites Chong and Hayat as evidence, respectively, that an Alzheimer's disease patient and a subject in need of enhanced kidney function are both subjects in need of increased Epo production. (Id. at 3--4.) Alternatively, the Examiner concludes that it would have been obvious to administer TSG to an Alzheimer's disease patient based on Wang's treatment of an animal model of Alzheimer's disease. (Id. at 7-8.) We will affirm the rejection of claim 1. Wang discloses treatment of aged rats with TSG, the same compound referred to as "compound A" in Appellant's Specification. (Wang 739, abstract.) Wang reports that administration of TSG resulted in "significant improvement in the leaming- memory abilities in the water maze tests associated with an increase in the number of synapses and synaptic vesicles, . . . suggesting that TSG may be beneficial for the treatment of Alzheimer disease." (Id.) Wang also reports that in an earlier study, "TSG showed a significant improvement of leaming- memory abilities and inhibition of amyloid plaque formation in APP transgenic mice of Alzheimer's disease." (Id. at 739, right col.) 4 Appeal 2014-003135 Application 12/343,922 Chong discloses that Alzheimer's disease involves B-amyloid (AB) toxicity of neurons and that "EPO is an effective entity at the neuronal cellular level against AB toxicity." (Chong 387, abstract.) We agree with the Examiner that Chong shows that the animal models of Alzheimer's disease that were treated by Wang are therefore subjects in need of enhanced Epo formation, as recited in claim 1, because Epo is effective against AB toxicity to neurons in Alzheimer's disease patients. Appellant argues that "Wang teaches that TSG may be beneficial for the treatment of Alzheimer disease (AD), whereas Chong teaches that erythropoietin (EPO) may be effective for AD .... Neither Wang nor Chong teaches or suggests that administering TSG can certainly enhance EPO formation." (Br. 6.) This argument is unpersuasive, because Wang teaches administering the same compound to subjects that are encompassed by the claim language, and therefore carries out a process within the scope of claim 1. Although Wang does not disclose that administering TSG enhances Epo formation, "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). "The general principle that a newly-discovered property of the prior art cannot support a patent on that same art is not avoided if the patentee explicitly claims that property." Id. at 1368. We therefore affirm the rejection of claim 1. Claims 2 and 7 fall with claim 1. 37 C.F.R. Â§ 41.37( c )(1 )(iv). 5 Appeal 2014-003135 Application 12/343,922 With regard to claims 10 and 12, Appellant argues that the references do not disclose or suggest the claimed methods because the evidence does not show that TSG is associated with kidney function or expression of hepatocyte growth factor. (Br. 8.) The Examiner cites Hayat as evidence that one of the functions of the kidney is to produce Epo and concludes that "a subject in need of increased erythropoietin production is reasonably considered to be a subject in need of enhanced kidney function." (Ans. 4.) The Examiner states that "[fJor these reasons, the rats treated by Wang et al. are reasonably considered to be in need of enhanced hepatocyte growth factor expression, enhanced erythropoietin formation, and enhanced kidney function." (Id.) We will affirm the rejection of claim 10. Hayat discloses that "the kidney is the sole source of erythropoietin (EPO) synthesis in adults." (Hayat 195.) Since one of the functions of the kidney is to produce Epo, a subject in need of enhanced Epo formation (claim 1) is also a subject in need of enhanced kidney function (claim 10). The broadest reasonable interpretation of claim 10, therefore, includes treatment of a subject in need of enhanced Epo formation. Because, for the reasons discussed above, Wang and Chong show that the rats treated with TSG by Wang were subjects in need of enhanced Epo formation, the evidence provided by Hayat shows that they were also subjects in need of enhanced kidney function, as recited in claim 10. Claim 11 falls with claim 10. 37 C.F.R. 41.37(c)(l)(iv). However, the Examiner has not pointed to evidence in any of the cited references showing that the Alzheimer's disease model animals treated with TSG by Wang were subjects in need of enhanced expression ofhepatocyte 6 Appeal 2014-003135 Application 12/343,922 growth factor, as recited in claim 12. Thus, the Examiner has not provided evidence that the method disclosed by Wang meets the limitations of claim 12, and we therefore reverse the rejection of that claim, as well as dependent claim 13. II The Examiner has rejected claims 1-3 and 10-13 as anticipated by Kimura, as evidenced by Y azihan and Hayat, or alternatively as obvious based on Kimura, Y azihan, and Hayat. The Examiner finds that Kimura discloses that TSG treatment reduced markers of liver injury in rats fed peroxidized lipids. (Ans. 4.) The Examiner cites Appellant's Specification as evidence that "various diseases including liver cirrhosis and fatty liver" can be treated by regulating expression of hepatocyte growth factor. (Id.) The Examiner finds that Y azihan discloses that Epo reduces cell death caused by hydrogen peroxide in a hepatoma cell line, "indicating that a subject undergoing peroxide-induced liver damage is 'a subject in need' of enhanced erythropoietin formation" and relies on Hayat as evidence that a subject in need of enhanced Epo formation is also a subject in need of enhanced kidney function. (Id. at 5.) We will affirm the rejection. Kimura discloses "the effects of stilbene components of the roots of Polygon um spp. on rat liver injury caused by oral administration of peroxidized com oil." (Kimura 51, right col.) The stilbene components include TSG. (Id. at 51, abstract (referring to TSG by its chemical name).) Kimura discloses that TSG inhibited elevation of serum lipids and transaminases caused by peroxidized com oil. (Id. at 52, right 7 Appeal 2014-003135 Application 12/343,922 col.) Kimura thus discloses "the protective actions of stilbene components such as piceid and [TSG] against liver injury." (Id. at 54, left col.) Y azihan discloses a study of the effect of Epo on hydrogen peroxide (H202)-induced liver damage. (Yazihan 239, Background/aims.) Yazihan concludes that its "results suggest ... [a] protective role of EPO against hepatic H202 toxicity" (id. at 243, right col.) and that "[e]rythropoietin treatment may be considered as a therapeutic agent during oxidative injuries ofhepatocytes." (Id. at 239, Conclusions.) Yazihan therefore provides evidence that the rats treated with TSG by Kimura are subjects in need of enhanced Epo formation, as recited in claim 1. As with the rejections based on Wang, Hayat shows that subjects in need of enhanced Epo formation are also subjects in need of enhanced kidney function, as recited in claim 10, because one of the functions of the kidney is to produce Epo. Finally, with regard to claim 12, Appellant's Specification itself provides evidence that the rats treated by Kimura are subjects in need of enhanced expression of hepatocyte growth factor. The Specification states that diseases or disorders treated by regulating the expression of hepatocyte growth factor include "acute hepatitis, liver cirrhosis, fulminant hepatitis, fatty liver, surgical treatments for liver transplantation, partial resection and ischemia." (Spec. 5: 1-3, 10-11.) Yazihan states that "[h ]igh levels of hydrogen peroxide (H202) are observed during inflammatory and ischemic states of the liver and usually lead to cellular dysfunction and cytotoxicity." (Yazihan 239, Background.) Thus, the rats with liver damage caused by peroxidized com oil that are 8 Appeal 2014-003135 Application 12/343,922 treated with TSG by Kimura are subjects in need of enhanced expression of hepatocyte growth factor, as recited in claim 12. As with the rejections based on Wang, Appellant argues that "none of the cited references teach or suggest administering TSG for enhancing erythropoietin formation." (Br. 9.) As previously discussed, however, "a reference may anticipate even when the relevant properties of the thing disclosed were not appreciated at the time." Abbott Labs., 471 F.3d at 1367. "The general principle that a newly-discovered property of the prior art cannot support a patent on that same art is not avoided if the patentee explicitly claims that property." Id. at 1368. Because Kimura teaches administering the same compound to subjects that are encompassed by the claim language, it carries out a process within the scope of claims 1, 10, and 12. Appellant also argues that without the teaching of the Applicant's invention, one having ordinary skill in the art would not be able to conceive that TSG enhances EPO formation. Similarly, without the teaching of the Applicant's invention, one having ordinary skill in the art would not be able to reasonably associate TSG with kidney function and the expression of hepatocyte growth factor. (Br. 10.) While the Examiner relied on Appellant's Specification as evidence that the rats treated with TSG in Kimura are subjects in need of enhanced expression of hepatocyte growth factor, we do not agree with Appellant's position that this reliance was improper. Claims are given their broadest reasonable interpretation in light of the Specification. In re Hyatt, 211 F .3d 1367, 1372 (Fed. Cir. 2000). Thus, it is proper to refer to the Specification 9 Appeal 2014-003135 Application 12/343,922 in interpreting the claim language. See In re Morris, 127 F.3d 1048, 1054 (Fed. Cir. 1997) ("the PTO applies to the verbiage of the proposed claims the broadest reasonable meaning ... , taking into account whatever enlightenment by way of definitions or otherwise that may be afforded by the written description contained in the applicant's Specification."). Claims 2 and 3 fall with claim 1, claim 11 falls with claim 10, and claim 13 falls with claim 12. 37 C.F.R. Â§ 41.37(c)(l)(iv). III The Examiner has rejected claims 1-3 and 8-13 as anticipated by Wu as evidenced by Kim and Hayat. The Examiner finds that Wu discloses methanol extracts from P. multiflorum Thunb. and Kim provides evidence that TSG is present in such extracts. (Ans. 5-6.) The Examiner finds that "Wu furthermore discloses that these extracts can be administered to subjects in need of proliferation of various cell types including erythrocytes, (i.e. erythropoiesis) and additionally to treat diseases including" liver cirrhosis and anemia. (Id. at 6.) The Examiner finds that Appellant's Specification provides evidence that liver cirrhosis is a disease to be treated by regulating expression of hepatocyte growth factor and anemia is a disease benefitting from Epo treatment (and therefore also enhanced Epo formation). (Id.) We agree with the Examiner's findings. Wu discloses "extract products from the root of Polygonum multiflorum Thunb., which have been proved to be biologically active in promoting the proliferation and/or growth of hepatocytes and bone marrow cells." (Wu ,-i 53.) Wu's extracts are made by methanol extraction of P. multiflorum Thunb. root material, optionally 10 Appeal 2014-003135 Application 12/343,922 followed by other extraction steps. (Id. at iii! 54-58, 67-79.) Wu discloses that its extracts are used to treat a subject in need of erythrocyte proliferation (a.k.a. erythropoiesis), subjects having liver cirrhosis, and subjects having anemia. (Id. at iJ 82-84.) Kim discloses analysis of methanol extracts of P. multiflorum Thunb. root material. (Kim 1225-1226, Extraction and Isolation.) Kim discloses that the extracts contained compound 3, which Kim identifies as TSG. (Id. at 1227, right col.) Kim also discloses that TSG is a known constituent of P. multiflorum root extracts. (Id. at 1225, abstract.) We agree that Kim supports a reasonable conclusion that the extracts disclosed by Wu contained TSG, based on the similarity of the extraction procedures disclosed by Wu and Kim. The Examiner notes that Appellant's Specification states that subjects with liver cirrhosis are subjects in need of enhanced expression of hepatocyte growth factor and subjects having anemia are subjects in need of enhanced Epo formation. (Spec. 4:1-5, 5:1-3, 10.) Therefore, we agree with the Examiner that Wu discloses methods meeting the limitations of claims 1, 8, and 12. As evidenced by Hayat, Epo formation is one function of the kidney, and therefore subjects in need of enhanced Epo formation are also subjects in need of enhanced kidney function, as recited in claim 10. Appellant argues that the rejection based on Wu is erroneous for the same reason as the rejection based on Wang. (Br. 11.) This argument is unpersuasive for the reasons previously discussed. Appellant also argues that "Kim clearly discloses that various compounds, not only TSG, are present in the methanol extract of Polygonum 11 Appeal 2014-003135 Application 12/343,922 multiflorum. Therefore, the Office has failed to provide any reasonable support for position that TSG is the active component." (Id.) Similarly, Appellant argues that "the Office fails to afford a reasonable support for that it must be the TSG which acts in Wu's extract as an active component responsible for the observed effects, even in view of the disclosure of Kim." (Id. at 12.) This argument is also unpersuasive. Kim identifies nine compounds in its extracts, including compound 3, which is identified as TSG. (Kim 1225, abstract; 1227, right col.) Kim also discloses that extraction with methanol, followed by ethyl acetate, and separation into six fractions (id. at 1226, left col.), resulted in a fraction containing "compounds 1 (25 mg), 2 (120 mg), 3 (5.3 g), 4 (8 mg), 7 (50 mg), and 8 (49 mg)." (Id. at 1226, left col.) At 5.3 grams, the amount of compound 3 in the fraction is far greater than any of the other compounds, which are all present in milligram quantities. Based on Kim, therefore, it is reasonable to conclude that Wu's methanol extracts contained TSG "in an effective amount," as recited in the claims. Finally, Appellant argues that "[ n Jo prior art teaches that compounds for promoting the proliferation of hepatocytes and bone marrow cells must be useful for enhancing erythropoietin formation, erythropoiesis, kidney function or expression of hepatocyte growth factor." (Br. 12.) This argument fails for reasons similar to those discussed above. The anticipation issue turns on whether Wu discloses administering the same compound, to the same subjects, in the amount recited in the claims. For the reasons discussed previously, we conclude that it does. The fact that the 12 Appeal 2014-003135 Application 12/343,922 claims recite effects of carrying out the prior art process that were not disclosed in the prior art does not render the claimed methods different from those disclosed by Wu. See Perricone v. Medicis Pharm. Corp., 432 F.3d 1368, 1377 (Fed. Cir. 2005) ("In some cases, [an] inherent property corresponds to a claimed new benefit or characteristic of an invention otherwise in the prior art. In those cases, the new realization alone does not render the old invention patentable."). Claims 2 and 3 fall with claim 1, claim 9 falls with claim 8, claim 11 falls with claim 10, and claim 13 falls with claim 12. 37 C.F.R. Â§ 41.37(c)(l)(iv). SUMMARY We affirm the rejection of claims 1, 2, 7, 10, and 11 under 35 U.S.C. Â§ 102(b) as anticipated by Wang, as evidenced by Chong and Hayat. Because anticipation is the epitome of obviousness, In re McDaniel, 293 F.3d 1379, 1385 (Fed. Cir. 2002), we also affirm the alternative rejection of these claims under 35 U.S.C. Â§ 103(a). We reverse both of these rejections with respect to claims 12 and 13. We affirm the rejection of claims 1-3 and 10-13 under 35 U.S.C. Â§ 102(b) as anticipated by Kimura, as evidenced by Y azihan and Hayat. Because anticipation is the epitome of obviousness, 293 F.3d at 1385, we also affirm the alternative rejection of these claims under 35 U.S.C. Â§ 103(a). We affirm the rejection of claims 1-3 and 8-13 under 35 U.S.C. Â§ 102(b) as anticipated by Wu, as evidenced by Kim and Hayat. 13 Appeal 2014-003135 Application 12/343,922 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§ l.136(a). AFFIRMED 14