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通过免疫分离对SV40染色质和大T抗原的多聚(ADP-核糖基化)进行体内表征。

In vivo characterization of the poly(ADP-ribosylation) of SV40 chromatin and large T antigen by immunofractionation.

作者信息

Baksi K, Alkhatib H, Smulson M E

机构信息

Department of Biochemistry, School of Medicine, Georgetown University, Washington, D.C. 20007.

出版信息

Exp Cell Res. 1987 Sep;172(1):110-23. doi: 10.1016/0014-4827(87)90098-x.

Abstract

We have confirmed the poly(ADP-ribosylation) of large T antigen of SV40 by using antibodies to both large T antigen and poly(ADP-ribose) and consequently have begun to characterize how this post-translational nuclear modification of the viral protein modulates its biological functions. SV40 minichromosomal subpopulation containing replicative intermediate DNA was shown to have a significantly higher affinity for anti-poly(ADP-Rib)-Sepharose than viral chromatin fractions containing mature minichromosomal DNA. An anti-large T-Sepharose column was used to isolate T antigen from crude extracts by two different approaches: (1) large T antigen was labeled with [35S]methionine in vivo and the infected cell extract was immunofractionated to isolate large T antigen and (2) large T antigen from infected cell extracts was immunofractionated followed by immunostaining. Using these techniques, 1-10% of the total T antigen from infected cells was found to be poly(ADP-ribosylated). Minichromosome preparations per se were also subjected to immunofractionation on anti-large T-Sepharose. The high level of retention of poly(ADP-ribosylated) species of minichromosomes on this matrix suggested that this post-translational modification of viral chromatin may be related to those steps in viral replication and transcription under regulation by large T antigen.

摘要

我们通过使用针对大T抗原和聚(ADP - 核糖)的抗体,证实了SV40大T抗原的聚(ADP - 核糖基化),因此已开始研究病毒蛋白的这种翻译后核修饰如何调节其生物学功能。含有复制中间体DNA的SV40微型染色体亚群对抗聚(ADP - 核糖)-琼脂糖的亲和力明显高于含有成熟微型染色体DNA的病毒染色质组分。使用抗大T - 琼脂糖柱通过两种不同方法从粗提物中分离T抗原:(1)大T抗原在体内用[35S]甲硫氨酸标记,感染细胞提取物经免疫分离以分离大T抗原;(2)感染细胞提取物中的大T抗原经免疫分离后进行免疫染色。使用这些技术,发现感染细胞中总T抗原的1 - 10%被聚(ADP - 核糖基化)。微型染色体制剂本身也在抗大T - 琼脂糖上进行免疫分离。微型染色体的聚(ADP - 核糖基化)物种在该基质上的高保留水平表明,病毒染色质的这种翻译后修饰可能与大T抗原调控的病毒复制和转录步骤有关。

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