Carboplatin/taxane-induced gastrointestinal toxicity: a pharmacogenomics study on the SCOTROC1 trial

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作者
Y J He
S J Winham
J M Hoskins
S Glass
J Paul
R Brown
A Motsinger-Reif
H L McLeod
机构
[1] Xiang-Ya Hospital,Department of Clinical Pharmacology
[2] Central South University,Department of Statistics
[3] Pharmacogenetics Research institute,Department of Surgery and Cancer
[4] Central South University,undefined
[5] Institute for Pharmacogenomics and Individualized Therapy,undefined
[6] University of North Carolina,undefined
[7] Moffitt Cancer Center,undefined
[8] DeBartolo Family Personalized Medicine Institute,undefined
[9] Bioinformatics Research Center,undefined
[10] North Carolina State University,undefined
[11] Health Sciences Research,undefined
[12] Mayo Clinic,undefined
[13] Cancer Research UK Clinical Trials Unit,undefined
[14] Beatson West of Scotland Cancer Centre,undefined
[15] Institute of Cancer Sciences,undefined
[16] University of Glasgow,undefined
[17] Imperial College London,undefined
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摘要
Carboplatin/taxane combination is first-line therapy for ovarian cancer. However, patients can encounter treatment delays, impaired quality of life, even death because of chemotherapy-induced gastrointestinal (GI) toxicity. A candidate gene study was conducted to assess potential association of genetic variants with GI toxicity in 808 patients who received carboplatin/taxane in the Scottish Randomized Trial in Ovarian Cancer 1 (SCOTROC1). Patients were randomized into discovery and validation cohorts consisting of 404 patients each. Clinical covariates and genetic variants associated with grade III/IV GI toxicity in discovery cohort were evaluated in replication cohort. Chemotherapy-induced GI toxicity was significantly associated with seven single-nucleotide polymorphisms in the ATP7B, GSR, VEGFA and SCN10A genes. Patients with risk genotypes were at 1.53 to 18.01 higher odds to develop carboplatin/taxane-induced GI toxicity (P<0.01). Variants in the VEGF gene were marginally associated with survival time. Our data provide potential targets for modulation/inhibition of GI toxicity in ovarian cancer patients.
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页码:243 / 248
页数:5
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