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Long-term balancing selection maintains trans-specific polymorphisms in the human TRIM5 gene.

机译:长期平衡选择在人类TRIM5基因中维持反式多态性。

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The human TRIM5 genes encodes a retroviral restriction factor (TRIM5alpha). Evolutionary analyses of this gene in mammals have revealed a complex and multifaceted scenario, suggesting that TRIM5 has been the target of exceptionally strong selective pressures, possibly exerted by recurrent waves of retroviral infections. TRIM5 displays inter-individual expression variability in humans and high levels of TRIM5 mRNA have been associated with a reduced risk of HIV-1 infection. We resequenced TRIM5 in chimpanzees and identified two polymorphisms in intron 1 that are shared with humans. Analysis of the gene region encompassing the two trans-specific variants in human populations identified exceptional nucleotide diversity levels and an excess of polymorphism compared to fixed divergence. Most tests rejected the null hypothesis of neutral evolution for this region and haplotype analysis revealed the presence of two deeply separated clades. Calculation of the time to the most recent common ancestor (TMRCA) for TRIM5 haplotypes yielded estimates ranging between 4 and 7 million years. Overall, these data indicate that long-term balancing selection, an extremely rare process outside MHC genes, has maintained trans-specific polymorphisms in the first intron of TRIM5. Bioinformatic analyses indicated that variants in intron 1 may affect transcription factor-binding sites and, therefore, TRIM5 transcriptional activity. Data herein confirm an extremely complex evolutionary history of TRIM5 genes in primates and open the possibility that regulatory variants in the gene modulate the susceptibility to HIV-1.
机译:人类TRIM5基因编码逆转录病毒限制因子(TRIM5alpha)。在哺乳动物中对该基因进行的进化分析揭示了一个复杂而多方面的情况,表明TRIM5已成为极强的选择性压力(可能由逆转录病毒感染的反复发作所施加)的目标。 TRIM5在人类中表现出个体间的表达差异,并且高水平的TRIM5 mRNA与降低HIV-1感染的风险有关。我们在黑猩猩中对TRIM5进行了重新测序,并确定了与人类共有的内含子1中的两个多态性。对涵盖人类群体中两个反式变异的基因区域的分析确定了异常的核苷酸多样性水平和与固定的多样性相比过量的多态性。大多数测试都拒绝了该区域中性进化的零假设,而单倍型分析揭示了两个深深分离的进化枝的存在。对TRIM5单倍体到最近的祖先(TMRCA)的时间进行计算得出的估计值介于4到700万年之间。总体而言,这些数据表明,长期平衡选择是MHC基因之外极为罕见的过程,在TRIM5的第一个内含子中保持了反式多态性。生物信息学分析表明,内含子1中的变体可能影响转录因子结合位点,从而影响TRIM5转录活性。本文中的数据证实了灵长类动物中TRIM5基因的进化过程极为复杂,并开启了该基因中的调控变异体调节HIV-1敏感性的可能性。

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