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人嗜T淋巴细胞病毒基因调控:因为大小很重要,转录是不够的。

HTLV gene regulation: because size matters, transcription is not enough.

作者信息

Journo Chloé, Douceron Estelle, Mahieux Renaud

机构信息

Equipe Oncogenèse Rétrovirale, INSERM-U758 Virologie Humaine, 69364 Lyon Cedex 07, France.

出版信息

Future Microbiol. 2009 May;4(4):425-40. doi: 10.2217/fmb.09.13.

Abstract

Despite being discovered in animals in the early 20th century, the scientific interest in retroviruses was boosted with the discovery of human retroviruses (human T-leukemia/lymphoma virus [HTLV] and HIV), which are responsible for significant morbidity and mortality. HTLV was identified more than 25 years ago as the etiological agent of adult T-cell leukemia/lymphoma. It was then shown to be a complex retrovirus, given that it not only encodes the characteristic retroviral Gag, Pol and Env proteins, but also regulatory and accessory proteins. Since the first studies documenting the role of these proteins in viral expression, the picture has become increasingly more complex. Indeed, owing to the limited size of its genome that contains overlapping open-reading frames, HTLV has evolved unique ways to regulate its expression. Retroviral expression was originally thought to be mainly controlled through the regulation of transcription from the 5 long-terminal repeats, but we now know that the 3 long-terminal repeats also serve as promoters. Regulation of splicing and mRNA export, and post-translational modifications of viral protein also play a major role. This review discusses the latest insights gained into the field of HTLV gene expression.

摘要

尽管逆转录病毒在20世纪初就已在动物中被发现,但随着人类逆转录病毒(人类T淋巴细胞白血病/淋巴瘤病毒[HTLV]和HIV)的发现,科学界对逆转录病毒的兴趣得到了提升,这些病毒会导致严重的发病率和死亡率。25年前,HTLV被确定为成人T细胞白血病/淋巴瘤的病原体。后来发现它是一种复杂的逆转录病毒,因为它不仅编码逆转录病毒特有的Gag、Pol和Env蛋白,还编码调节蛋白和辅助蛋白。自首次研究记录这些蛋白在病毒表达中的作用以来,情况变得越来越复杂。事实上,由于其基因组大小有限且包含重叠的开放阅读框,HTLV进化出了独特的方式来调节其表达。逆转录病毒的表达最初被认为主要通过对5'长末端重复序列转录的调控来控制,但我们现在知道3'长末端重复序列也可作为启动子。剪接和mRNA输出的调控以及病毒蛋白的翻译后修饰也起着重要作用。本综述讨论了HTLV基因表达领域的最新见解。

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