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Aberrant allele frequencies of the SNPs located in microRNA target sites are potentially associated with human cancers

机译:位于microRNA目标位点的SNP的异常等位基因频率可能与人类癌症有关

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MicroRNAs (miRNAs) are a class of noncoding small RNAs that regulate gene expression by base pairing with target mRNAs at the 3 '-terminal untranslated regions (3 '-UTRs), leading to mRNA cleavage or translational repression. Single-nucleotide polymorphisms (SNPs) located at miRNA-binding sites (miRNA-binding SNPs) are likely to affect the expression of the miRNA target and may contribute to the susceptibility of humans to common diseases. We herein performed a genome-wide analysis of SNPs located in the miRNA-binding sites of the 3 '-UTR of various human genes. We found that miRNA-binding SNPs are negatively selected in respect to SNP distribution between the miRNA-binding 'seed' sequence and the entire 3 '-UTR sequence. Furthermore, we comprehensively defined the expression of each miRNA-binding SNP in cancers versus normal tissues through mining EST data-bases. Interestingly, we found that some miRNA-binding SNPs exhibit significant different allele frequencies between the human cancer EST libraries and the dbSNP database. More importantly, using human cancer specimens against the dbSNP database for case-control association studies, we found that twelve mIRNA-binding SNPs indeed display an aberrant allele frequency in human cancers. Hence, SNPs located in miRNA-binding sites affect miRNA target expression and function, and are potentially associated with cancers.
机译:MicroRNA(miRNA)是一类非编码小RNA,它们通过与3'-末端非翻译区(3'-UTR)上的靶标mRNA碱基配对来调节基因表达,从而导致mRNA切割或翻译抑制。位于miRNA结合位点(与miRNA结合的SNP)的单核苷酸多态性(SNP)可能会影响miRNA靶标的表达,并可能导致人类对常见疾病的敏感性。我们在本文中对位于各种人类基因3'-UTR的miRNA结合位点的SNP进行了全基因组分析。我们发现,就结合miRNA的“种子”序列和整个3'-UTR序列之间的SNP分布而言,结合miRNA的SNP被否定选择。此外,我们通过挖掘EST数据库全面定义了每种与miRNA结合的SNP在癌症与正常组织中的表达。有趣的是,我们发现在人类癌症EST文库和dbSNP数据库之间,一些与miRNA结合的SNP表现出明显不同的等位基因频率。更重要的是,使用针对dbSNP数据库的人类癌症标本进行病例对照关联研究,我们发现十二种结合mIRNA的SNP确实在人类癌症中表现出异常的等位基因频率。因此,位于miRNA结合位点的SNP会影响miRNA靶标的表达和功能,并可能与癌症相关。

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