| Literature DB >> 17854076 |
Zhongning Lin1, Xuemei Zhang, Jingsheng Tuo, Yongli Guo, Bridgett Green, Chi-Chao Chan, Wen Tan, Ying Huang, Wenhua Ling, Fred F Kadlubar, Dongxin Lin, Baitang Ning.
Abstract
Cockayne syndrome B protein (ERCC6) plays an essential role in DNA repair. However, the Cockayne syndrome caused by the ERCC6 defect has not been linked to cancer predisposition; likely due to the fact that cells with severe disruption of the ERCC6 function are sensitive to lesion-induced apoptosis, thus reducing the chance of tumorigenesis. The biological function and cancer susceptibility of a common variant rs3793784:C>G (c.-6530C>G) in the ERCC6 was examined. We show that the c.-6530C allele has lower binding affinity of Sp1 by EMSA and displays a lower transcriptional activity in vitro and in vivo. We then examined the contribution of this polymorphism to the risk of lung cancer in a case-control study with 1,000 cases and 1,000 controls. The case-control analysis revealed a 1.76-fold (P= x 10(-9)) excess risk of developing lung cancer for the c.-6530CC carriers compared with noncarriers. The c.-6530CC interacts with smoking to intensify lung cancer risk, with the odds ratio (OR)=9 for developing lung cancer among heavy smokers. Our data constituted strong evidence that ERCC6 rs3793784:C>G alters its transcriptional activity and may confer personalized susceptibility to lung cancer. Published 2007, Wiley-Liss, Inc.Entities:
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Year: 2008 PMID: 17854076 PMCID: PMC2441604 DOI: 10.1002/humu.20610
Source DB: PubMed Journal: Hum Mutat ISSN: 1059-7794 Impact factor: 4.878