11871057 - (D) (P.T.A.B. Jun. 25, 2019)

Ex Parte Kwong

Patent Trials and Appeals BoardJun 25, 2019

11871057 - (D) (P.T.A.B. Jun. 25, 2019)

UNITED STA TES p A TENT AND TRADEMARK OFFICE APPLICATION NO. FILING DATE 11/871,057 10/11/2007 23579 7590 06/25/2019 Pabst Patent Group LLP 1545 PEACHTREE STREET NE SUITE 320 ATLANTA, GA 30309 FIRST NAMED INVENTOR Yok-LamKwong 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. UHK00230 6065 EXAMINER CHOI, FRANK I ART UNIT PAPER NUMBER 1616 MAIL DATE DELIVERY MODE 06/25/2019 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 YOK-LAM KWONG Appeal2018-001094 Application 11/871,057 1 Technology Center 1600 Before DONALD E. ADAMS, ERIC B. GRIMES, and FRANCISCO C. PRATS, Administrative Patent Judges. ADAMS, Administrative Patent Judge. DECISION ON APPEAL This Appeal2 under 35 U.S.C. Â§ 134(a) involves claims 1, 3, 5, 7, and 11-13 (App. Br. 3). Examiner entered a rejection under 35 U.S.C. Â§ 103(a). We have jurisdiction under 35 U.S.C. Â§ 6(b). We AFFIRM. 1 Appellant identifies "The University of Hong Kong" as the real party in interest (Appellant's May 1, 2017 Appeal Brief (App. Br.) 2). 2 This Appeal is related to Appeal 2012-005618 (Application 11/871,068), Decision on Appeal reversing the rejections of record entered May 12, 2014 and Appeal 2012-008942 (Application 11/549,347), Decision on Appeal affirming the rejection of record entered May 9, 2014. Appeal2018-001094 Application 11/871,057 STATEMENT OF THE CASE Appellant's disclosure "relates to methods of inhibiting certain cancers by affecting expression, translation, and biological activity of cancers expressing receptor tyrosine kinases using arsenic trioxide" (Spec. 1:8-10). Appellant's claims 1, 3, and 11 are representative and reproduced below: 1. A method for promoting cytokine receptor or receptor tyrosine kinase degradation in cancer cells comprising orally administering to a patient with epidermal growth factor or cytokine dependent cancer cells that have been tested for dependency on tyrosine kinase receptors for signaling, proliferation, survival, metastasis and differentiation, wherein the cancer cells are not head and neck squamous cell carcinoma, acute promyelocytic leukemia, and multiple myeloma, an amount of arsenic trioxide in a pharmaceutically acceptable carrier for enteral administration which is effective to inhibit proliferation of the cancer cells. (App. Br. 26.) (Id.) (Id.) 3. The method of claim 1, wherein the cancer is an epithelial growth factor receptor dependent cancer. 11. The method of claim 1 wherein the arsenic trioxide is present in an amount from 5 to 10 mg. 2 Appeal2018-001094 Application 11/871,057 Claims 1, 3, 5, 7, and 11-13 stand rejected under 35 U.S.C. Â§ 103(a) as unpatentable over the combination of Warrell, 3 Kwong, 4 Rojewski, 5 Appellant's Admission, Cui, 6 Soresi, 7 and Cheung. 8 ISSUE Does the preponderance of evidence relied upon by Examiner support a conclusion of obviousness? FACTUAL FINDINGS (FF) FF 1. We adopt Examiner's findings concerning the scope and content of the prior art (Final Act. 9 2---6), and provide the following findings for emphasis. 3 Warrell, Jr. et al., US 6,723,351 B2, issued Apr. 20, 2004. 4 Yok-Lam Kwong, Arsenic trioxide in the treatment of haematological malignancies, 3 EXPERT OPIN. DRUG SAF. 589-597 (2004). 5 Rojewski et al., Dual effects of arsenic trioxide (As203) on non-acute promyelocytic leukaemia myeloid cell lines: induction of apoptosis and inhibition of proliferation, 116 BRITISH JOURNAL OF HAEMATOLOGY 555- 563 (2002). 6 Cui et al., Effects of Arsenic Trioxide on the Expression of Gene Protein Related to Vascular Endothelium Induced by Liver Cancer, SmnE HUAREN XIAOHUAZAZHI (2005) (as translated in PT02010-4450 (July 9, 2010)). 7 Soresi et al., Interleukin-6 and its soluble receptor in patients with liver cirrhosis and hepatocellular carcinoma, 12 WORLD J. GASTROENTEROLOGY 2563-2568 (2006). 8 Cheung et al., Arsenic Trioxide Targets the Interleukin-6 Cascade in Multiple Myeloma by Promoting Lysosomal Degradation of the Interleukin- 6 Receptor Complex, 106 BLOOD, Abstract 5159 (2005). 9 Examiner's November 1, 2016 Final Office Action. 3 Appeal2018-001094 Application 11/871,057 FF 2. Warrell "relates to methods and compositions for the treatment of leukemia, lymphoma, and certain other cancers" (Warrell 1: 12-14; see generally Final Act. 3). FF 3. Warrell provides a method for treatment of solid tumors, including metastasises [sic], in humans comprising the administration of a therapeutically effective and non-lethal amount of arsenic trioxide ... to the human. Solid tumors that can be treated by the methods of [Warrell' s] invention include but are not limited to: cancer of the digestive tract, oesophagus, liver, stomach, and colon; skin; brain; bone; breast; lung; and soft tissues, including but not limited to various sarcomas, and preferably prostate cancer. (Warrell 6: 58---67; see id. at 4: 41--42 (Warrell's use of the term "'arsenic compound' refers to a pharmaceutically acceptable form of arsenic trioxide (As203)"); see Final Act. 3.) FF 4. Warrell's disclosure "encompasses a composition suitable for oral delivery; comprising arsenic trioxide ... and a pharmaceutically acceptable excipient or carrier" (Warrell 4: 7-10; see also id. at 5: 18-22 (describing oral administration as a suitable mode of administering Warrell' s arsenic compound); id. at 9: 20--44 (describing oral formulations ofWarrell's arsenic compound); id. at 11: 3-52 (describing oral administration of Warrell's arsenic compound, including, inter alia, powder, capsule, and tablet formulations); see Final Act. 3). FF 5. Warrell discloses, "[i]n general, the daily dose ranges of arsenic trioxide for the conditions described [by Warrell] are generally from about 0.05 to about 5 mg per kg body weight administered in divided doses administered parenterally or orally or topically," wherein "[a] preferred total 4 Appeal2018-001094 Application 11/871,057 daily dose is from about 2.5 to about 40 mg of arsenic trioxide" (Warrell 10: 25-31; see Final Act. 3). FF 6. Kwong discloses that a standard oral dose of arsenic trioxide is 10 mg/day, wherein, "current practice is to use half the standard dose (5 mg/day) for patients with impaired renal function," because "[r]enal excretion is a major route of elimination of arsenic" and "[i]n patients with impaired renal function, the dose of arsenic trioxide should be adjusted" (Kwong 593; see Final Act. 3; Ans. 10 6; cf Spec. 15: 3-5 (Appellant discloses that the "dose of oral As203 is typically adjusted according to age and kidney function. In one embodiment, the dose range of As203 varies from 1 to 10 mg, typically about 5 to 10 mg")). FF 7. Kwong discloses that although arsenic trioxide "is a well-known poison ... at therapeutic doses, arsenic trioxide has much fewer side effects . . . than standard chemotherapy" (Kwong 591; see id. at 591-593; see Final Act. 3). FF 8. Kwong discloses "that oral arsenic trioxide is comparable with intravenous arsenic trioxide in its clinical profile and efficacy" (Kwong 591; see Final Act. 3). FF 9. Cui discloses that As203 has an inhibiting effect on the EGFR expression in liver cancer cells. EGFR plays an important part in the process of the emergence and development of human liver cancer. ... [B]y regulating down the expression of EGFR protein in liver cancer cells, As203 injections may affect the EGFR mediated signal transduction paths, thereby inhibiting the proliferation and migration of the tumor, inhibiting the formation of newly 10 Examiner's September 11, 2017 Answer. 5 Appeal2018-001094 Application 11/871,057 generated vessels in the tumor, and achieving the goal of curing the tumor and preventing it from metastasizing and recurring. Since there is a relatedness among the expressions of EGFR and its ligands those of E-CD, integrin and other factors, as soon as a change occurs in the expression of a certain factor, or a common change in their interaction, this can have a major impact on the emergence, development, and metastasizing of tumors. The results of [Cui's] study have demonstrated that As203 injections have a certain regulating effect on the expression of all of these factors; however, it remains to be studied how they are interrelated. (Cui Â§ 3.4 ( endnotes and emphasis omitted); see Final Act. 4 ( citing Spec. 1: 12-14; 2: 1-2, and 3: 1-2) (the "epidermal growth factor receptor (EGFR) is [a] tyrosine kinase receptor"); Ans. 7-9.) FF 10. Warrell discloses: It should be noted that the attending physician would know how to and when to terminate, interrupt or adjust therapy to lower dosage due to toxicity, or bone marrow, liver or kidney dysfunctions. Conversely, the attending physician would also know how to and when to adjust treatment to higher levels if the clinical response is not adequate (precluding toxic side effects). (Warrell 10: 63 - 11: 2; see Final Act. 3.) FF 11. Kwong discloses that, because "oral arsenic trioxide achieves a lower peak plasma arsenic level, the prolongation of QT interval, which depends on the plasma arsenic, might be expected to be less serious. This has in fact been found when oral arsenic trioxide is used clinically" (Kwong 592; see Final Act. 3; Ans. 6). 6 Appeal2018-001094 Application 11/871,057 ANALYSIS The combination of prior art relied upon by Examiner makes obvious a method of treating, inter alia, liver cancer, in a human, by orally administering "a therapeutically effective and non-lethal amount of arsenic trioxide ... to the human" (FF 1--4). The evidence of record establishes that liver cancer is an EGFR dependent cancer, wherein arsenic trioxide injections have a regulating effect on "EGFR mediated signal transduction paths, thereby inhibiting the proliferation and migration of the tumor, inhibiting the formation of newly generated vessels in the tumor, and," thereby resulting in "achieving the goal of curing the tumor and preventing it from metastasizing and recurring" (FF 9). With regard to arsenic trioxide injections, the evidence of record establishes "that oral arsenic trioxide is comparable with intravenous arsenic trioxide in its clinical profile and efficacy" (FF 8). In this regard, the evidence of record establishes that although arsenic trioxide "is a well- known poison ... at therapeutic doses, arsenic trioxide has much fewer side effects ... than standard chemotherapy" (FF 7). In addition, the combination of prior art relied upon by Examiner suggests that a therapeutically effective and non-lethal amount of arsenic trioxide for oral administration to a human for the treatment of, inter alia, liver cancer is "generally from about 0.05 to about 5 mg per kg body weight administered in divided doses administered parenterally or orally or topically" and, more specifically, the oral administration of arsenic trioxide at a dose of 10 mg/day to patients without impaired renal function (FF 5---6). Thus, we find no error in Examiner's conclusion that the combination of Warrell, Kwong, Rojewski, Appellant's Admission, Cui, Soresi, and 7 Appeal2018-001094 Application 11/871,057 Cheung, make obvious Appellant's claimed invention (see Final Act. 6; FF 1-9). Claim 1: Initially, we note that argument by counsel cannot take the place of evidence. In re Cole, 326 F.2d 769, 773 (CCPA 1964). Therefore, we are not persuaded by counsel's unsupported assertions (see generally App. Br. 7-9). We recognize Appellant's contention that "Appellant discovered that arsenic trioxide suppresses cancer cell growth by targeting receptor tyrosine kinases and cytokine receptors for degradation" and "that oral administration of arsenic trioxide [was] effective in treating cancer characterized by their dependency on tyrosine kinase receptors for signaling, proliferation, survival, metastasis and differentiation" (App. Br. 12; see id. (Appellant discloses that "the common mechanism linking the activity of arsenic trioxide in different cell types was not known prior to Appellant's filing, showing that this had been determined by extensive experimentation"); see Reply Br. 2-3; cf FF 1-9)). It is, however, "elementary that the mere recitation of a newly discovered function or property, inherently possessed by things in the prior art, does not cause a claim drawn to those things to distinguish over the prior art." In re Swinehart, 439 F.2d 210, 212-13 (CCPA 1971); Atlas Powder Co. v. Ireco Inc., 190 F.3d 1342, 1347 (Fed. Cir. 1999) ("[T]he discovery of a previously unappreciated property of a prior art composition, or of a scientific explanation for the prior art's functioning, does not render the old composition patentably new to the discoverer."). 8 Appeal2018-001094 Application 11/871,057 A reference disclosure is not limited only to its preferred embodiments, but is available for all that it discloses and suggests to one of ordinary skill in the art. In re Lamberti, 545 F.2d 747, 750 (CCPA 1976); see also In re Susi, 440 F.2d 442,446 n.3 (CCPA 1971) (disclosed examples and preferred embodiments do not constitute a teaching away from a broader disclosure or non-preferred embodiments). Therefore, we are not persuaded by Appellant's contention that despite Warrell's extensive disclosure of oral arsenic trioxide formulations for use in the treatment of cancer, including liver cancer, a "person of ordinary skill in the art reading the disclosure of Warrell would not have reasonably expected an oral formulation to be both safe and effective for treating solid tumors" (see App. Br. 9; see also id. at 17 (Appellant contends that "even though Warrell states that arsenic trioxide can be administered orally, this statement is not supported by the examples."); Reply Br. 4; cf FF 5). Appellant's contention also fails to account for Kwong's disclosure of the oral administration of arsenic trioxide for the treatment of cancer (FF 6). Notwithstanding Appellant's unsupported assertion that "arsenic trioxide has been administered systemically (i.v.) to treat cancer, but with such debilitating side effects that it was a drug of last resort," the evidence on this record makes clear that although arsenic trioxide "is a well-known poison," the administration of arsenic trioxide "at therapeutic doses ... has much fewer side effects ... than standard chemotherapy" and "that oral arsenic trioxide is comparable with intravenous arsenic trioxide in its clinical profile and efficacy" (see App. Br. 7; see also id. at 9-10 and 12; Reply Br. 3--4; cf FF 7-8). For the same reasons we are not persuaded by Appellant's contention that the combination of Warrell, Kwong, Rojewski, Appellant's 9 Appeal2018-001094 Application 11/871,057 Admission, Cui, Soresi, and Cheung does not make obvious the oral administration of arsenic trioxide for the treatment of cancer (see FF 1-10; cf App. Br. 16-17). The evidence of record establishes that liver cancer is an EGFR dependent cancer, wherein arsenic trioxide injections have a regulating effect on "EGFR mediated signal transduction paths, thereby inhibiting the proliferation and migration of the tumor, inhibiting the formation of newly generated vessels in the tumor, and," thereby result in "achieving the goal of curing the tumor and preventing it from metastasizing and recurring" (FF 9). Appellant does not dispute that EGFR is a tyrosine kinase receptor (see FF 11-12; cf FF 9). For the reasons set forth above, we are not persuaded by Appellant's contention that "[n]one of the cited art leads one to arsenic trioxide for the selective killing of cells expressing tyrosine kinases associated with cancer cells" (App. Br. 14 (emphasis omitted); see also id. at 18; Reply Br. 7-9; cf FF 1-10). Therefore, we are not persuaded by Appellant's unsupported assertion that: [S]afe and effective use of an oral formulation of arsenic trioxide in treating epidermal growth factor ... dependent cancer cells that have been tested for dependency on tyrosine kinase receptors for signaling, proliferation, survival, metastasis and differentiation, wherein the cancer cells are not head and neck squamous cell carcinoma, acute promyelocytic leukemia, and multiple myeloma ... is unexpected. (App. Br. 9-10; see also id. at 16-17; cf FF 1-9.) For the reasons set for the above, we are not persuaded by Appellant's contention that: Without Appellant's teaching of the route of administration, and the common mechanism linking the activity of arsenic trioxide in different cell types, it would not have been predictable to one of ordinary skill in the art at the time the application was filed, based on the prior art, that arsenic 10 Appeal2018-001094 Application 11/871,057 trioxide could be administered orally, to produce a level that would be effective to treat cancers in patients, wherein the cancer cells are dependent on receptor tyrosine kinases and/ or cytokine receptors for signaling, proliferation, survival, metastasis and differentiation, and wherein the cancer cells are not head and neck squamous cell carcinoma, acute promyelocytic leukemia, and multiple myeloma. (App. Br. 13.) Warrell "provides a method for treatment of solid tumors, including [hematological and non-hematological malignancies] ... , in humans comprising the administration of a therapeutically effective and non-lethal amount of arsenic trioxide ... to the human" (see FF 3). Warrell discloses, "[i]n general, the daily dose ranges of arsenic trioxide for the conditions described [by Warrell] are generally from about 0.05 to about 5 mg per kg body weight administered in divided doses administered parenterally or orally or topically," wherein "[a] preferred total daily dose is from about 2.5 to about 40 mg of arsenic trioxide" (FF 5). In this regard, we note that Kwong discloses that a standard oral dose of arsenic trioxide is 10 mg/ day (FF 6). Therefore, we are not persuaded by Appellant's contention that Kwong's disclosure of the treatment of hematological malignancies is unrelated and fails to support Warrell' s disclosure of the treatment of hematological and non-hematological malignancies, which include those, such as liver cancer, that are epidermal growth factor dependent, by orally administering arsenic trioxide at dosages that encompass Kwong's standard oral arsenic trioxide dosage (see App. Br. 10; see also id. at 13 (Appellant contends that "[p]rior to Appellant's discovery, it was not known that arsenic trioxide targets receptor tyrosine kinases and cytokine receptors in non-hematological cancer cells, or that an oral dose would be effective to 11 Appeal2018-001094 Application 11/871,057 treat these non-hematological cancer cells"); Reply Br. 4--7; cf FF 5---6; see generally FF 1-9). For the foregoing reasons, we are not persuaded by Appellant's contentions relating to arsenic toxicity (App. Br. 14 (citing ATSDR Guide 11 and Ratnaike 12); see also App. Br. 15 and 19; cf FF IO (Warrell discloses that those of ordinary skill in this art understand how to minimize toxic side effects)). As discussed above, Warrell in combination with Kwong, Rojewski, Appellant's Admission, Cui, Soresi, and Cheung "provides a method for treatment of solid tumors, including [hematological and non-hematological malignancies, such as liver cancer] ... , in humans comprising the [oral] administration of a therapeutically effective and non-lethal amount of arsenic trioxide ... to the human" (see FF 3). The evidence of record also supports a conclusion that liver cancer is an EGFR dependent cancer, wherein arsenic trioxide injections have a regulating effect on "EGFR mediated signal transduction paths, thereby inhibiting the proliferation and migration of the tumor, inhibiting the formation of newly generated vessels in the tumor, and," thereby result in "achieving the goal of curing the tumor and preventing it from metastasizing and recurring" (FF 9). Therefore, we are not persuaded by Appellant's contentions relating to whether "tyrosine 11 Medical Management Guidelines for Arsenic Trioxide (As203), in Agency for Toxic Substances & Disease Registry, CAS#: 1327-53-3, UN#: 1561 (2014), available at https://www.atsdr.cdc.gov/MMG/MMG.asp?id=1200&tid=279. 12 Ratnaike, Acute and chronic arsenic toxicity, 79 POSTGRAD MED. J. 391---6 (2003). 12 Appeal2018-001094 Application 11/871,057 receptors were found in significantly different levels and types depending on the type of cancer" (App. Br. 19 (citing Miiller-Tidow 13 and Johnson 14)). Warrell discloses that those of ordinary skill in the art understand how to minimize the toxic side effects associated with oral arsenic trioxide administration (FF 10). Nevertheless, Appellant contends that its claimed invention is not prima facie obvious over the combination of Warrell, Kwong, Rojewski, Appellant's Admission, Cui, Soresi, and Cheung, because Weingart 15 suggests that practitioners may not orally administer chemotherapeutic drugs in a safe and effective manner (see App. Br. 15-16 ("Weingart states that safeguards in routine use for infusion chemotherapy have not been adopted for oral chemotherapy")). Because Examiner established an evidentiary basis on this record to support a conclusion of obviousness, we are not persuaded by Appellant's contentions regarding safety. The use of drugs in medicine is frequently a matter of balancing risks to save a life. And Congress has given the responsibility to the FDA, not to the Patent Office, to determine in the first instance whether drugs are sufficiently safe for use that they can be introduced in the commercial market, under the conditions 13 Miiller-Tidow et al., High-Throughput Analysis of Genome-Wide Receptor Tyrosine Kinase Expression in Human Cancers Identifies Potential Novel Drug Targets, 10 CLINICAL CANCER RESEARCH 1241-1249 (2004). 14 Johnson, Screening Methods in Antineoplastic Drug Discovery, 82 JOURNAL OF THE NATIONAL CANCER INSTITUTE 1082-1083 (1990). 15 Weingart et al., Oral chemotherapy safety practices at US cancer centres: questionnaire survey, BMJ, doi: 10.1136/bmj.39069.489757.55 (published 12 January 2007). 13 Appeal2018-001094 Application 11/871,057 prescribed, recommended, or suggested in the proposed labeling thereof .... In re Anthony, 414 F.2d 1383, 1395 (CCPA 1969). For the foregoing reasons, we are not persuaded by Appellant's contentions regarding each ofRojewski, Cui, Soresi, Cheung, and Kwong individually, which fail to account for the combined disclosures of Warrell, Kwong, Rojewski, Appellant's Admission, Cui, Soresi, and Cheung (see App. Br. 20; see also Reply Br. 5---6 and 9-10; cf FF 1-10). See In re Merck & Co., 800 F.2d 1091, 1097 (Fed. Cir. 1986) ("Non-obviousness cannot be established by attacking references individually where the rejection is based upon the teachings of a combination of references. . . . [The reference] must be read, not in isolation, but for what it fairly teaches in combination with the prior art as a whole."); see also Ans. 5 (citing In re Keller, 642 F.2d 413, 425 (CCPA 1981)). Unexpected Results: We are not persuaded by Appellant's contention that "[i]t was not known prior to Appellant's experimental results that orally administered arsenic trioxide is effective and significantly safer than intravenously administered arsenic trioxide" (App. Br. 18 (citing Siu 16); cf FF 7-8 and 11; Ans. 10). Warrell "provides a method for treatment of solid tumors, including metastasises [sic], in humans comprising the [oral] administration of a therapeutically effective and non-lethal amount of arsenic trioxide ... to the 16 Siu et al., Effects of oral arsenic trioxide therapy on QT intervals in patients with acute promyelocytic leukemia: implications for long-term cardiac safety, 108 BLOOD 103-106 (2006). 14 Appeal2018-001094 Application 11/871,057 human" (FF 3). Kwong, as Appellant recognizes, also discloses the oral administration of arsenic trioxide for the treatment of cancer (see App. Br. 19 (Appellant expressly states that "Kwong describes oral administration of arsenic trioxide to treat leukemias"); see also id. at 10). Therefore, we are not persuaded by Appellant's contention that "Appellant was the first to develop an oral formulation of arsenic trioxide and demonstrate efficacy of systemic cancer treatment with this formulation" (App. Br. 21; cf FF 1-5). Thus, Appellant failed to establish an evidentiary basis on this record to support Appellant's contention that those in the art tried and failed to solve the problem addressed by Appellant. For the reasons discussed above, Warrell and Kwong alone or in combination support a conclusion that the oral administration of arsenic trioxide for the treatment of cancer was well-known in this art prior to the date of Appellant's claimed invention (see FF 1-8; see also App. Br. 19 (Appellant expressly states that "Kwong describes oral administration of arsenic trioxide to treat leukemias")). In addition, Kwong discloses that "at therapeutic doses, arsenic trioxide has much fewer side effects ... than standard chemotherapy" (FF 7). Therefore, we are not persuaded by 15 Appeal2018-001094 Application 11/871,057 Appellant's contention regarding a long-felt but unmet need in this art (see App. Br. 21-22 (citing Au 2011, 17 Au 2012, 18 and Gill 19; cf Ans. 10). For the reasons discussed above, we are not persuaded by Appellant's contention that "[ s ]ince publication of the data described in this application and that which it claims priority to, the oral route has become a route of choice for administration of arsenic trioxide, precisely because it's safer and more efficacious in contrast to intravenous administration" (App. Br. 22; cf FF 1-8; see also App. Br. 19 (Appellant expressly states that "Kwong describes oral administration of arsenic trioxide to treat leukemias" prior to the date of Appellant's claimed invention); Ans. 11). For the foregoing reasons, we are not persuaded by Appellant's contention that Examiner's conclusion of obviousness is based on improper hindsight reasoning (see App. Br. 22; see also Reply Br. 10-11; cf Ans. 11- 12). Claim 3: Warrell discloses the oral administration of arsenic trioxide for the treatment of cancer, including liver cancer (FF 3). In addition, the evidence of record establishes that liver cancer is an EGFR dependent cancer, wherein 17 Au et al., Oral arsenic trioxide-based maintenance regimens for first complete remission of acute promyelocytic leukemia: a 10-year follow-up study, 118 BLOOD 6535-6543 (2011). 18 Au et al., Oral Arsenic Trioxide for relapsed Acute Promyelocytic Leukemia in Pediatric Patients, 58 PEDIATR BLOOD CANCER 630-632 (2012). 19 Gill et al., Oral arsenic trioxide-based regimen as salvage treatment for relapsed or refractory mantle cell lymphoma, 25 ANN ONCOL 1391-1397 (2014). 16 Appeal2018-001094 Application 11/871,057 arsenic trioxide injections have a regulating effect on "EGFR mediated signal transduction paths, thereby inhibiting the proliferation and migration of the tumor, inhibiting the formation of newly generated vessels in the tumor, and," thereby result in "achieving the goal of curing the tumor and preventing it from metastasizing and recurring" (FF 9). Therefore, for the reasons set forth above, we are not persuaded by Appellant's contention that the evidence of record fails to suggest an EGFR dependent cancer and "[t]here is no reason why one of ordinary skill in the art would expect success in using an orally administered dose of arsenic trioxide to treat cancers that is an epithelial growth factor receptor dependent cancer" (see App. Br. 23; see also Reply Br. 12-13; cf FF 1-11). Claim 11: For the reasons set forth above, we are not persuaded by Appellant's contentions that "none of the cited references disclose or suggest that 5 to 10 mg of arsenic trioxide administered orally would be effective for treating a patient with epidermal growth factor ... dependent cancer cells" and "[t]here is no reason why one of ordinary skill in the art would expect success in using an orally administered dose of arsenic trioxide at 5 to 10 mg to treat cancer" (see App. Br. 23-24; see also Reply Br. 13; cf FF 1-11). CONCLUSION The preponderance of evidence relied upon by Examiner supports a conclusion of obviousness. 17 Appeal2018-001094 Application 11/871,057 The rejection of claims 1, 3, and 11 under 35 U.S.C. Â§ 103(a) as unpatentable over the combination of Warrell, Kwong, Rojewski, Appellant's Admission, Cui, Soresi, and Cheung is affirmed. Appellant provides the following claim groupings: (a) claims 1 and 12; (b) claims 3, 5, and 7; and (c) claims 11 and 13 (App. Br. 5; see also Reply Br. 2). Therefore, Appellant's claims 5, 7, 12, and 13, fall with Appellant's claims 1, 3, and 11, respectively. 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 18