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逆转录病毒起源的人类基因调查:具有完整包膜蛋白编码能力的基因的鉴定与转录组分析

Survey of human genes of retroviral origin: identification and transcriptome of the genes with coding capacity for complete envelope proteins.

作者信息

de Parseval Nathalie, Lazar Vladimir, Casella Jean-François, Benit Laurence, Heidmann Thierry

机构信息

Unité des Rétrovirus Endogènes et Eléments Rétroïdes des Eucaryotes Supérieurs, UMR 8122 CNRS, France.

出版信息

J Virol. 2003 Oct;77(19):10414-22. doi: 10.1128/jvi.77.19.10414-10422.2003.

DOI:10.1128/jvi.77.19.10414-10422.2003
PMID:12970426
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC228468/
Abstract

Sequences of retroviral origin occupy approximately 8% of the human genome. Most of these "retroviral" genes have lost their coding capacities since their entry into our ancestral genome millions of years ago, but some reading frames have remained open, suggesting positive selection. The complete sequencing of the human genome allowed a systematic search for retroviral envelope genes containing an open reading frame and resulted in the identification of 16 genes that we have characterized. We further showed, by quantitative reverse transcriptase PCR using specifically devised primers which discriminate between coding and noncoding elements, that all 16 genes are expressed in at least some healthy human tissues, albeit at highly different levels. All envelope genes disclose significant expression in the testis, three of them have a very high level of expression in the placenta, and a fourth is expressed in the thyroid. Besides their primary role as key molecules for viral entry, the envelope genes of retroviruses can induce cell-cell fusion, elicit immunosuppressive effects, and even protect against infection, and as such, endogenous retroviral envelope proteins have been tentatively identified in several reports as being involved in both normal and pathological processes. The present study provides a comprehensive survey of candidate genes and tools for a precise evaluation of their involvement in these processes.

摘要

逆转录病毒起源的序列占据了人类基因组的约8%。自从数百万年前进入我们的祖先基因组以来,这些“逆转录病毒”基因中的大多数已经丧失了编码能力,但一些阅读框仍然开放,这表明存在正选择。人类基因组的全序列测定使得能够系统地搜索含有开放阅读框的逆转录病毒包膜基因,并鉴定出了我们已进行特征描述的16个基因。我们还通过使用专门设计的能区分编码和非编码元件的引物进行定量逆转录酶PCR进一步表明,所有这16个基因在至少一些健康人体组织中都有表达,尽管表达水平差异很大。所有包膜基因在睾丸中均有显著表达,其中三个在胎盘中表达水平非常高,还有一个在甲状腺中表达。除了作为病毒进入的关键分子的主要作用外,逆转录病毒的包膜基因还可诱导细胞间融合、引发免疫抑制作用,甚至预防感染,因此,在几份报告中已初步确定内源性逆转录病毒包膜蛋白参与正常和病理过程。本研究提供了对候选基因的全面调查以及用于精确评估它们在这些过程中所起作用的工具。

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本文引用的文献

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Characterization of the low-copy HERV-Fc family: evidence for recent integrations in primates of elements with coding envelope genes.低拷贝HERV-Fc家族的特征:具有编码包膜基因的元件在灵长类动物中近期整合的证据。
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