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新型人多瘤病毒的结构评估为其发病机制提供了线索。

Structural evaluation of new human polyomaviruses provides clues to pathobiology.

机构信息

Department of Microbiology and Molecular Cell Biology, Eastern Virginia Medical School, Norfolk, VA 23501, USA.

出版信息

Trends Microbiol. 2010 May;18(5):215-23. doi: 10.1016/j.tim.2010.01.001. Epub 2010 Feb 20.

Abstract

In the past three years, remarkable discoveries have added three new human polyomaviruses (KI virus (KIV), WU virus (WUV) and Merkel cell virus (MCV)) to a class that previously had only two disease-causing members (BK virus (BKV) and JC virus (JCV)) identified. Two monkey polyomaviruses, simian virus (SV)40 and B-cell lymphotropic polyomavirus (LPV) are also present in humans. KIV and WUV lack the agnoprotein coding sequence and regulatory micro (mi)RNA clusters of BKV, JCV and SV40. MCV lacks the agnoprotein sequence but generates miRNAs. KIV, WUV and MCV are all widespread in humans. Although they have distinctive tissue tropisms, all these viruses are probably acquired in childhood. Of these viruses, only MCV has thus far been strongly linked to cancer. Marshalled evidence from diverse sources implicates MCV as an etiological agent of Merkel cell carcinoma. This review compares the structural features of the new and previously known polyomaviruses, with the aim of identifying approaches to molecular pathology.

摘要

在过去的三年中,已经发现了三种新的人类多瘤病毒(KI 病毒(KIV)、WU 病毒(WUV)和 Merkel 细胞病毒(MCV)),使以前只有两种致病成员(BK 病毒(BKV)和 JC 病毒(JCV))的一类病毒增加到了五种。两种猴多瘤病毒,猿猴病毒 40 型(SV40)和 B 细胞淋巴组织增生性多瘤病毒(LPV)也存在于人类中。KIV 和 WUV 缺乏 BKV、JCV 和 SV40 的 agnoprotein 编码序列和调节微(mi)RNA 簇。MCV 缺乏 agnoprotein 序列,但能产生 miRNA。KIV、WUV 和 MCV 在人类中都广泛存在。尽管它们具有不同的组织嗜性,但所有这些病毒可能都是在儿童时期获得的。在这些病毒中,只有 MCV 迄今与癌症有很强的关联。从不同来源收集的证据表明,MCV 是 Merkel 细胞癌的病因。这篇综述比较了新的和以前已知的多瘤病毒的结构特征,目的是确定分子病理学的方法。

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