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人内源性逆转录病毒K族:生物学活性最强的人类内源性逆转录病毒家族。

HERV-K: the biologically most active human endogenous retrovirus family.

作者信息

Tönjes R R, Löwer R, Boller K, Denner J, Hasenmaier B, Kirsch H, König H, Korbmacher C, Limbach C, Lugert R, Phelps R C, Scherer J, Thelen K, Löwer J, Kurth R

机构信息

Paul-Ehrlich-Institut, Langen, Germany.

出版信息

J Acquir Immune Defic Syndr Hum Retrovirol. 1996;13 Suppl 1:S261-7. doi: 10.1097/00042560-199600001-00039.

Abstract

The human genome contains a wide variety of endogenous retrovirus-like sequences. The human endogenous retrovirus type K (HERV-K) family comprises 30-50 members per haploid genome in humans and is highly conserved in Old World monkeys and apes. Some proviruses are displaying open reading frames (ORF) with coding capacity for viral particles. HERV-K sequences most likely code for the previously described human teratocarcinoma-derived virus (HTDV) and correlated expression of HERV-K Gag has been demonstrated by immunoelectron microscopy studies. Protease, but not yet reverse transcriptase (RT), enzymatic activity was demonstrated for recombinant HERV-K proteins. However, an ultrasensitive RT assay revealed specific polymerase activity associated with the HTDV particles. HERV-K transcription is specifically regulated by viral long terminal repeats and RNA is expressed at low steady-state levels in a variety of human tissues and tumours. In teratocarcinoma cell lines, HERV-K is highly expressed in a complex pattern showing full-length as well as subgenomic envelope (env) and two alternatively spliced small transcripts. The doubly spliced 1.8-kb mRNA codes for cORF protein which resembles Rev of HIV-1 and is located in the nucleolus. In addition, the cORF sequence acts as a leader and is essential for effective expression of glycosylated HERV-K Env protein. Although HERV-K sequences code for all necessary retroviral proteins, infectious particles could not yet be demonstrated. The putative implication of HERV sequences in pathophysiological processes, for example, testicular malignancies, remains to be elucidated.

摘要

人类基因组包含各种各样的内源性逆转录病毒样序列。人类内源性逆转录病毒K型(HERV-K)家族在人类单倍体基因组中包含30 - 50个成员,在旧世界猴和猿中高度保守。一些前病毒显示出具有病毒颗粒编码能力的开放阅读框(ORF)。HERV-K序列很可能编码先前描述的人类畸胎瘤衍生病毒(HTDV),免疫电子显微镜研究已证实HERV-K Gag的相关表达。重组HERV-K蛋白显示出蛋白酶活性,但尚未显示出逆转录酶(RT)活性。然而,一种超灵敏的RT检测揭示了与HTDV颗粒相关的特异性聚合酶活性。HERV-K转录受病毒长末端重复序列特异性调控,RNA在多种人类组织和肿瘤中以低稳态水平表达。在畸胎瘤细胞系中,HERV-K以复杂模式高度表达,显示出全长以及亚基因组包膜(env)和两种选择性剪接的小转录本。双重剪接的1.8 kb mRNA编码类似于HIV-1 Rev的cORF蛋白,其位于核仁中。此外,cORF序列起引导作用,对于糖基化HERV-K Env蛋白的有效表达至关重要。尽管HERV-K序列编码所有必需的逆转录病毒蛋白,但尚未证明有感染性颗粒。HERV序列在病理生理过程(例如睾丸恶性肿瘤)中的假定作用仍有待阐明。

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