首页> 外文期刊>Retrovirology >Contribution of type W human endogenous retroviruses to the human genome: characterization of HERV-W proviral insertions and processed pseudogenes
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Contribution of type W human endogenous retroviruses to the human genome: characterization of HERV-W proviral insertions and processed pseudogenes

机译:W人类内源性逆转录病毒对人类基因组的贡献:Herv-W脱玻璃插入和加工假生素的表征

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Background Human endogenous retroviruses (HERVs) are ancient sequences integrated in the germ line cells and vertically transmitted through the offspring constituting about 8?% of our genome. In time, HERVs accumulated mutations that compromised their coding capacity. A prominent exception is HERV-W locus 7q21.2, producing a functional Env protein (Syncytin-1) coopted for placental syncytiotrophoblast formation. While expression of HERV-W sequences has been investigated for their correlation to disease, an exhaustive description of the group composition and characteristics is still not available and current HERV-W group information derive from studies published a few years ago that, of course, used the rough assemblies of the human genome available at that time. This hampers the comparison and correlation with current human genome assemblies. Results In the present work we identified and described in detail the distribution and genetic composition of 213 HERV-W elements. The bioinformatics analysis led to the characterization of several previously unreported features and provided a phylogenetic classification of two main subgroups with different age and structural characteristics. New facts on HERV-W genomic context of insertion and co-localization with sequences putatively involved in disease development are also reported. Conclusions The present work is a detailed overview of the HERV-W contribution to the human genome and provides a robust genetic background useful to clarify HERV-W role in pathologies with poorly understood etiology, representing, to our knowledge, the most complete and exhaustive HERV-W dataset up to date.
机译:背景技术人内源性逆转录病毒(HERVS)是整合在种系细胞中的古序列,并垂直传播通过构成我们基因组的约8μm的后代。及时,Hervs累积损害其编码能力的突变。突出的例外是Herv-W Locus 7Q21.2,产生函数env蛋白(Syncytin-1),用于胎直合胞胎细胞形成。虽然已经研究了Herv-W-W序列的表达,但它们与疾病的相关性,但仍然不可用的植物组成和特征的详尽描述,并且目前的Herv-W集团信息来自几年前发表的研究,当然,使用当时可用的人类基因组的粗糙组件。这妨碍了与当前人类基因组组件的比较和相关性。结果我们鉴定并详细描述了213赫沃-W元素的分布和遗传组成。生物信息学分析导致​​了几种先前未报告的特征的表征,并提供了具有不同年龄和结构特征的两个主要亚组的系统发育分类。还报道了患者插入和共同定位的新事实,伴随着疾病发展的序列。结论本作本作的详细概述了对人类基因组的贡献,并提供了一种有用的遗传背景,可阐明植物在病因良好的病因中,代表我们的知识,最完整和令人遗憾的腰部-w dataset最新。

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