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猿猴病毒 40 大 T 抗原的两个独立区域可增加 CBP/p300 水平,改变细胞组蛋白乙酰化模式,并使原代细胞永生化。

Two independent regions of simian virus 40 T antigen increase CBP/p300 levels, alter patterns of cellular histone acetylation, and immortalize primary cells.

机构信息

Department of Biological Sciences, University of Pittsburgh, Pittsburgh, Pennsylvania, USA.

出版信息

J Virol. 2013 Dec;87(24):13499-509. doi: 10.1128/JVI.02658-13. Epub 2013 Oct 2.

DOI:10.1128/JVI.02658-13
PMID:24089570
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3838271/
Abstract

Simian virus 40 (SV40) large T antigen (SVT) interferes with normal cell regulation and thus has been used to identify cellular components controlling proliferation and homeostasis. We have previously shown that SVT-mediated transformation requires interaction with the histone acetyltransferases (HATs) CBP/p300 and now report that the ectopic expression of SVT in several cell types in vivo and in vitro results in a significant increase in the steady-state levels of CBP/p300. Furthermore, SVT-expressing cells contain higher levels of acetylated CBP/p300, a modification that has been linked to increased HAT activity. Concomitantly, the acetylation levels of histone residues H3K56 and H4K12 are markedly increased in SVT-expressing cells. Other polyomavirus-encoded large T antigens also increase the levels of CBP/p300 and sustain a rise in the acetylation levels of H3K56 and H4K12. SVT does not affect the transcription of CBP/p300, but rather, alters their overall levels through increasing the loading of CBP/p300 mRNAs onto polysomes. Two distinct regions within SVT, one located in the amino terminus and one in the carboxy terminus, can independently alter both the levels of CBP/p300 and the loading of CBP/p300 transcripts onto polysomes. Within the amino-terminal fragment, a functional J domain is necessary for increasing CBP/p300 and specific histone acetylation levels, as well as for immortalizing primary cells. These studies uncover the action of polyomavirus T antigens on cellular CBP/p300 and suggest that additional mechanisms are used by T antigens to induce cell immortalization and transformation.

摘要

猿猴病毒 40(SV40)大 T 抗原(SVT)干扰正常细胞调节,因此被用于鉴定控制增殖和动态平衡的细胞成分。我们之前已经表明,SVT 介导的转化需要与组蛋白乙酰转移酶(HATs)CBP/p300 相互作用,现在我们报告说,SVT 在体内和体外的几种细胞类型中的异位表达导致 CBP/p300 的稳态水平显著增加。此外,SVT 表达细胞含有更高水平的乙酰化 CBP/p300,这种修饰与 HAT 活性的增加有关。同时,SVT 表达细胞中组蛋白残基 H3K56 和 H4K12 的乙酰化水平显著增加。其他多瘤病毒编码的大 T 抗原也增加了 CBP/p300 的水平,并维持 H3K56 和 H4K12 的乙酰化水平升高。SVT 不影响 CBP/p300 的转录,而是通过增加 CBP/p300 mRNA 加载到多核糖体上来改变它们的总体水平。SVT 中有两个不同的区域可以独立地改变 CBP/p300 的水平和 CBP/p300 转录物加载到多核糖体上,一个位于氨基末端,一个位于羧基末端。氨基末端片段中的一个功能 J 结构域对于增加 CBP/p300 和特定组蛋白乙酰化水平以及使原代细胞永生化是必需的。这些研究揭示了多瘤病毒 T 抗原对细胞 CBP/p300 的作用,并表明 T 抗原还使用其他机制诱导细胞永生化和转化。

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