Your search keyword '"Jiuping Ji"' showing total 2 results

1. Veliparib Alone or in Combination with Mitomycin C in Patients with Solid Tumors With Functional Deficiency in Homologous Recombination Repair.

Author

Villalona-Calero, Miguel A., Duan, Wenrui, Weiqiang Zhao, Shilo, Konstantin, Schaaf, Larry J., Thurmond, Jennifer, Westman, Judith A., Marshall, John, Li Xiaobai, Jiuping Ji, Rose, Jeffrey, Lustberg, Maryam, Bekaii-Saab, Tanios, Chen, Alice, Timmers, Cynthia, Zhao, Weiqiang, Xiaobai, Li, and Ji, Jiuping

Subjects

ANTINEOPLASTIC agents, APLASTIC anemia, COMPARATIVE studies, DIARRHEA, DRUG administration, FATIGUE (Physiology), GENEALOGY, GENETIC techniques, HETEROCYCLIC compounds, RESEARCH methodology, MEDICAL cooperation, GENETIC mutation, RESEARCH, RESEARCH funding, THROMBOCYTOPENIA, TUMORS, PILOT projects, EVALUATION research, RANDOMIZED controlled trials, BRCA genes, MITOMYCINS

Abstract

Background: BRCA germline mutations are being targeted for development of PARP inhibitors. BRCA genes collaborate with several others in the Fanconi Anemia (FA) pathway. We screened cancer patients' tumors for FA functional defects then aimed to establish the safety/feasibility of administering PARP inhibitors as monotherapy and combined with a DNA-breaking agent.Methods: Patients underwent FA functional screening for the presence (or lack) of tumor FancD2 nuclear foci formation on their archival tumor material, utilizing a newly developed method (Fanconi Anemia triple-stain immunofluorescence [FATSI]), performed in a Clinical Laboratory Improvement Amendments-certified laboratory. FATSI-negative patients were selected for enrollment in a two-arm dose escalation trial of veliparib, or veliparib/mitomycin-C (MMC).Results: One hundred eighty-five of 643 (28.7%) screened patients were FATSI-negative. Sixty-one received veliparib or veliparib/MMC through 14 dose levels. Moderate/severe toxicities included fatigue (DLT at veliparib 400mg BID), diarrhea, and thrombocytopenia. Recommended doses are 300mg BID veliparib and veliparib 200mg BID for 21 days following 10mg/m(2) MMC every 28 days. Six antitumor responses occurred, five in the combination arm (3 breast, 1 ovarian, 1 endometrial [uterine], and 1 non-small cell lung cancer). Two patients have received 36 and 60 cycles to date. BRCA germline analysis among 51 patients revealed five deleterious mutations while a targeted FA sequencing gene panel showed missense/nonsense mutations in 29 of 49 FATSI-negative tumor specimens.Conclusions: FATSI screening showed that a substantial number of patients' tumors have FA functional deficiency, which led to germline alterations in several patients' tumors. Veliparib alone or with MMC was safely administered to these patients and produced clinical benefit in some. However, a better understanding of resistance mechanisms in this setting is needed. [ABSTRACT FROM AUTHOR]

Published

2016

2. Phase l/lb Study of Olaparib and Carboplatin in BRCA1 or BRCA2 Mutation-Associated Breast or Ovarian Cancer With Biomarker Analyses.

Author

Jung-Min Lee, Hays, John L., Annunziata, Christina M., Noonan, Anne M., Minasian, Lori, Zujewski, Jo Anne, Minshu Yu, Gordon, Nicolas, Jiuping Ji, Sissung, Tristan M., Figg, William D., Azad, Nilofer, Wood, Bradford J., Doroshow, James, and Kohn, Elise C.

Subjects

OVARIAN cancer, GERM cells, BRCA genes, CARBOPLATIN, BIOMARKERS, PROTEOMICS, APOPTOSIS

Abstract

Background Olaparib has single-agent activity against breast/ovarian cancer (BrCa/OvCa) in germline BRCA1 or BRCA2 mutation carriers (gBRCAm). We hypothesized addition of olaparib to carboplatin can be administered safely and yield preliminary clinical activity. Methods Eligible patients had measurable or evaluable disease, gBRCAm, and good end-organ function. A 3 + 3 dose escalation tested daily oral capsule olaparib (100 or 200mg every 12 hours; dose levell or 2) with carboplatin area under the curve (AUC) on day 8 (AUC3 day 8), then every 21 days. For dose levels 3 to 6, patients were given olaparib days 1 to 7 at 200 and 400 mg every 12 hours, with carboplatin AUC3 to 5 on day 1 or 2 every 21 days; a maximum of eight combination cycles were permitted, after which daily maintenance of olaparib 400 mg every12 hours continued until progression. Dose-limiting toxicity was defined in the first two cycles. Peripheral blood mononuclear cells were collected for polymorphism analysis and polyADP-ribose incorporation. Paired tumor biopsies (before/after cycle 1) were obtained for biomarker proteomics and apoptosis endpoints. Results Forty-five women (37 OvCa/8 BrCa) were treated. Dose-limiting toxicity was not reached on the intermittent schedule. Expansion proceeded with olaparib 400 mg every 12 hours on days 1 to 7/carboplatin AUC5. Grade 3/4 adverse events included neutropenia (42.2%), thrombocytopenia (20.0%), and anemia (15.6%). Responses included 1 complete response (1 BrCa; 23 months) and 21 partial responses (50.0%; 15 OvCa; 6 BrCa; median = 16 [4 to > 45] in OvCa and 10 [6 to > 40] months in BrCa). Proteomic analysis suggests high pretreatment pS209-elF4E and FOX03a correlated with duration of response (two-sided P < .001; Pearson's R² = 0.94). Conclusions Olaparib capsules 400 mg every 12 hours on days 1 to 7/carboplatin AUC5 is safe and has activity in gBRCAm BrCa/OvCa patients. Exploratory translational studies indicate pretreatment tissue FOX03a expression may be predictive for response to therapy, requiring prospective validation. [ABSTRACT FROM AUTHOR]

Published

2014