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A Novel Functional TagSNP Rs7560488 in the DNMT3A1 Promoter Is Associated with Susceptibility to Gastric Cancer by Modulating Promoter Activity

机译:DNMT3A1启动子中的新型功能性TagSNP Rs7560488通过调节启动子活性与胃癌易感性相关

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摘要

DNA-methyltransferase (DNMT)-3A which contains DNMT3A1 and DNMT3A2 isoforms have been suggested to play a crucial role in carcinogenesis and showed aberrant expression in most cancers. Accumulated evidences also indicated that single nucleotide polymorphisms (SNP) in DNMT genes were associated with susceptibility to different tumors. We hypothesized that genetic variants in DNMT3A1 promoter region are associated with gastric cancer risk. We selected the tagSNPs from the HapMap database for the Chinese and genotyped in a case-control study to evaluate the association with gastric cancer (GC) in a Chinese population. We identified that the functional tagSNP rs7560488 T>C associated with a significantly increased risk of GC. In vitro functional analysis by luciferase reporter assay and EMSA indicated that the tagSNP rs7560488 T>C substantially altered transcriptional activity of DNMT3A1 gene via influencing the binding of some transcriptional factors, although a definite transcriptional factor remains to be established. Compared with TT homozygotes, subjects who were TC heterozygotes and CC homozygotes exhibited a reduced expression of DNMT3A1. Furthermore, stratified analysis showed that individuals who harbor TC or CC genotypes less than 60 years old were more susceptible to GC. Our results suggest that the genetic variations in the DNMT3A1 promoter contribute to the susceptibility to GC and also provide an insight that tagSNP rs7560488 T>C may be a promising biomarker for predicting GC genetic susceptibility and a valuable information in GC pathogenesis.
机译:含有DNMT3A1和DNMT3A2亚型的DNA-甲基转移酶(DNMT)-3A被认为在致癌作用中起关键作用,并在大多数癌症中表现出异常表达。累积的证据还表明,DNMT基因中的单核苷酸多态性(SNP)与不同肿瘤的易感性相关。我们假设DNMT3A1启动子区域的遗传变异与胃癌风险相关。我们从HapMap数据库中为中国人选择了tagSNPs,并在一项病例对照研究中进行了基因分型,以评估与中国人群胃癌(GC)的关联。我们发现功能性标签SNP rs7560488 T> C与GC风险显着增加相关。荧光素酶报告基因分析和EMSA的体外功能分析表明,tagSNP rs7560488 T> C通过影响某些转录因子的结合,实质上改变了DNMT3A1基因的转录活性,尽管仍有待确定的转录因子。与TT纯合子相比,TC杂合子和CC纯合子的DNMT3A1表达降低。此外,分层分析显示,携带TC或CC基因型小于60岁的个体更易患GC。我们的结果表明,DNMT3A1启动子的遗传变异有助于GC的易感性,也为tagSNP rs7560488 T> C可能是预测GC遗传易感性的有前途的生物标志物和在GC发病机理中提供有价值的信息提供了见解。

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