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首页> 外文期刊>BMC Genomics >Comprehensive search for intra- and inter-specific sequence polymorphisms among coding envelope genes of retroviral origin found in the human genome: genes and pseudogenes
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Comprehensive search for intra- and inter-specific sequence polymorphisms among coding envelope genes of retroviral origin found in the human genome: genes and pseudogenes

机译:全面搜索在人类基因组中发现的逆转录病毒起源的编码包膜基因之间的种内和种间序列多态性:基因和假基因

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Background The human genome carries a high load of proviral-like sequences, called Human Endogenous Retroviruses (HERVs), which are the genomic traces of ancient infections by active retroviruses. These elements are in most cases defective, but open reading frames can still be found for the retroviral envelope gene, with sixteen such genes identified so far. Several of them are conserved during primate evolution, having possibly been co-opted by their host for a physiological role. Results To characterize further their status, we presently sequenced 12 of these genes from a panel of 91 Caucasian individuals. Genomic analyses reveal strong sequence conservation (only two non synonymous Single Nucleotide Polymorphisms [SNPs]) for the two HERV-W and HERV-FRD envelope genes, i.e. for the two genes specifically expressed in the placenta and possibly involved in syncytiotrophoblast formation. We further show – using an ex vivo fusion assay for each allelic form – that none of these SNPs impairs the fusogenic function. The other envelope proteins disclose variable polymorphisms, with the occurrence of a stop codon and/or frameshift for most – but not all – of them. Moreover, the sequence conservation analysis of the orthologous genes that can be found in primates shows that three env genes have been maintained in a fully coding state throughout evolution including envW and envFRD. Conclusion Altogether, the present study strongly suggests that some but not all envelope encoding sequences are bona fide genes. It also provides new tools to elucidate the possible role of endogenous envelope proteins as susceptibility factors in a number of pathologies where HERVs have been suspected to be involved.
机译:背景技术人类基因组中载有高水平的前病毒样序列,称为人类内源性逆转录病毒(HERV),这是主动逆转录病毒感染古代病毒的基因组痕迹。这些元件在大多数情况下都是有缺陷的,但仍可以找到逆转录病毒包膜基因的开放阅读框,迄今已鉴定出十六种这样的基因。它们中有几个在灵长类动物进化过程中是保守的,它们的宿主可能因其生理作用而选择了它们。结果为了进一步表征它们的状态,我们目前对来自91个高加索人的一组基因中的12个进行了测序。基因组分析揭示了两个HERV-W和HERV-FRD包膜基因(即在胎盘中特异性表达并可能参与合体滋养层细胞形成的两个基因)的高度序列保守性(仅两个非同义的单核苷酸多态性[SNP])。我们进一步显示-使用每种等位基因形式的离体融合测定法-这些SNP均不损害融合功能。其他包膜蛋白具有可变的多态性,其中大多数(但不是全部)都出现终止密码子和/或移码。此外,对在灵长类动物中发现的直系同源基因的序列保守性分析表明,在整个进化过程中,包括envW和envFRD在内,三个env基因一直处于完全编码状态。结论总的来说,本研究强烈提示一些但不是全部的包膜编码序列是真正的基因。它还提供了新的工具来阐明内源性包膜蛋白在许多疑似涉及HERV的病理学中作为易感因素的可能作用。

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