Literature DB >> 23788213

Genetic polymorphisms in DNA repair genes XRCC4 and XRCC5 and aflatoxin B1-related hepatocellular carcinoma.

Xi-Dai Long1, Dong Zhao, Chao Wang, Xiao-Ying Huang, Jin-Guang Yao, Yun Ma, Zhong-Hua Wei, Min Liu, Li-Xiao Zeng, Xiao-Qiang Mo, Jian-Jun Zhang, Feng Xue, Bo Zhai, Qiang Xia.   

Abstract

BACKGROUND: Genetic polymorphisms in DNA repair genes may influence individual variation in DNA repair capacity and may play an important role in carcinogenesis. We investigated the role of genetic polymorphisms at XRCC4 codon 247 (rs3734091, XRCC4P) and XRCC5 codon 180 (rs80309960, XRCC5P) in liver cancer (hepatocellular carcinoma) caused by aflatoxin B1 (AFB1).
METHODS: A hospital-based case-control study, including 1499 liver cancer cases and 2045 controls without any liver disease, was conducted in a high aflatoxin exposure area in the Guangxi region of China to assess the relationship between these two polymorphisms and aflatoxin-related liver cancer risk and prognosis. Genotypes, mRNA levels, and the hot-spot mutation of TP53 gene (TP53M) related to AFB1 exposure was tested using TaqMan-PCR technique. XRCC4 protein level was analyzed by immunohistochemistry.
RESULTS: For XRCC4P and XRCC5P, only XRCC4P modified liver cancer risk. Compared with the homozygote of XRCC4 codon 247 Ala alleles (XRCC4-AA), the genotypes of XRCC4 codon 247 Ser alleles (namely XRCC4-AS or -SS) increased liver cancer risk (odds ratio [OR] = 1.35 and 2.02, respectively). Significant interactive effects between risk genotypes (OR > 1) and aflatoxin exposure status were also observed in the joint effects analysis. Moreover, this polymorphism was associated not only with lower XRCC4 expression levels but also with higher AFB1-DNA adduct levels and increasing TP53M and portal vein tumor risk. Additionally, XRCC4P modified the recurrence-free survival and overall survival of cases, especially under conditions of high aflatoxin exposure.
CONCLUSION: XRCC4P may be a genetic modifier for the risk and outcome of hepatocellular carcinoma induced by AFB1 exposure.

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Year:  2013        PMID: 23788213     DOI: 10.1097/EDE.0b013e31829d2744

Source DB:  PubMed          Journal:  Epidemiology        ISSN: 1044-3983            Impact factor:   4.822


  26 in total

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Authors:  Andrea Hartwig; Michael Arand; Bernd Epe; Sabine Guth; Gunnar Jahnke; Alfonso Lampen; Hans-Jörg Martus; Bernhard Monien; Ivonne M C M Rietjens; Simone Schmitz-Spanke; Gerlinde Schriever-Schwemmer; Pablo Steinberg; Gerhard Eisenbrand
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3.  Genetic variations of CAV1 gene contribute to HCC risk: a case-control study.

Authors:  Xixue Zhao; Guozheng Pan; Qingzhong Yuan; Dongpo Mu; Jun Zhang; Tao Cui; Jian Zhang; Linghai Zhang
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4.  Interaction of DNA repair gene polymorphisms and aflatoxin B1 in the risk of hepatocellular carcinoma.

Authors:  Jin-Guang Yao; Xiao-Ying Huang; Xi-Dai Long
Journal:  Int J Clin Exp Pathol       Date:  2014-08-15

5.  Effect of transporter and DNA repair gene polymorphisms to lung cancer chemotherapy toxicity.

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6.  Genetic variations in the one-carbon metabolism pathway genes and susceptibility to hepatocellular carcinoma risk: a case-control study.

Authors:  Heng Zhang; Chunhe Liu; Yu-Chen Han; Zuohong Ma; Haiyan Zhang; Yinan Ma; Xiaofang Liu
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8.  Association of androgen receptor exon 1 CAG repeat length with risk of hepatocellular carcinoma: a case-control study.

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Review 9.  The clinical utilization of circulating cell free DNA (CCFDNA) in blood of cancer patients.

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10.  MicroRNA-24 modulates aflatoxin B1-related hepatocellular carcinoma prognosis and tumorigenesis.

Authors:  Yi-Xiao Liu; Xi-Dai Long; Zhi-Feng Xi; Yun Ma; Xiao-Ying Huang; Jin-Guang Yao; Chao Wang; Tian-Yu Xing; Qiang Xia
Journal:  Biomed Res Int       Date:  2014-04-08       Impact factor: 3.411

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