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视网膜母细胞瘤蛋白家族成员与灵长类多瘤病毒大T抗原的相互作用。

Interaction of retinoblastoma protein family members with large T-antigen of primate polyomaviruses.

作者信息

White M K, Khalili K

机构信息

Center for Neurovirology, Department of Neuroscience, Temple University School of Medicine, Philadelphia, PA 19122, USA.

出版信息

Oncogene. 2006 Aug 28;25(38):5286-93. doi: 10.1038/sj.onc.1209618.

Abstract

The retinoblastoma gene product pRb and other members of the Rb family of pocket proteins have a central role in the regulation of cell cycle progression. Soon after its discovery, pRb was found to interact with the transforming oncoproteins of DNA tumor viruses and this led to rapid advances in our understanding of the mechanisms of viral transformation and cell cycle progression. DNA viruses of the polyomavirus family have small, circular, double-stranded DNA genomes contained within non-enveloped icosahedral capsids and are highly tumorigenic in experimental animals. At least three types of polyomavirus infect humans: JC virus (JCV), BK virus (BKV) and Simian Vacuolating virus-40. The early region of these viruses encodes the transforming proteins large T-antigen and small t-antigen, which are involved in viral replication and also promote transformation of cells in culture and oncogenesis in vivo. Binding of T-antigen to pRb promotes the activation of the E2F family of transcription factors, which induce the expression of cellular genes required for S phase. In the context of lytic infection, this cell cycle progression is necessary for viral replication because polyomaviruses rely on S phase-specific host factors for their DNA synthesis. In the context of cellular transformation and tumorigenesis, T-antigen/pRB interaction is an indispensable event.

摘要

视网膜母细胞瘤基因产物pRb和口袋蛋白Rb家族的其他成员在细胞周期进程的调控中起核心作用。pRb被发现后不久,人们就发现它能与DNA肿瘤病毒的转化癌蛋白相互作用,这使得我们对病毒转化机制和细胞周期进程的理解迅速取得进展。多瘤病毒家族的DNA病毒具有小的、环状的双链DNA基因组,包含在无包膜的二十面体衣壳内,在实验动物中具有高度致瘤性。至少有三种多瘤病毒感染人类:JC病毒(JCV)、BK病毒(BKV)和猴空泡病毒40。这些病毒的早期区域编码转化蛋白大T抗原和小t抗原,它们参与病毒复制,也促进培养细胞的转化和体内肿瘤发生。T抗原与pRb的结合促进转录因子E2F家族的激活,E2F家族诱导S期所需细胞基因的表达。在裂解感染的情况下,这种细胞周期进程对于病毒复制是必要的,因为多瘤病毒依赖S期特异性宿主因子进行DNA合成。在细胞转化和肿瘤发生的情况下,T抗原/pRB相互作用是一个不可或缺的事件。

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