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p53与DNA聚合酶α竞争结合SV40 T抗原。

p53 and DNA polymerase alpha compete for binding to SV40 T antigen.

作者信息

Gannon J V, Lane D P

机构信息

Imperial Cancer Research Fund, Clare Hall Laboratories, Herts, UK.

出版信息

Nature. 1987;329(6138):456-8. doi: 10.1038/329456a0.

Abstract

The large T antigen (T) of simian virus 40 is a multifunctional protein required for both viral DNA replication and cellular transformation. T antigen forms specific protein complexes with the host protein p53 in both virus-infected and transformed cells. p53 has recently been shown to be an oncogene, but its normal function is not clear. We previously established a radioimmunoassay to study the newly described complex between T antigen and DNA polymerase alpha, and have noted a similarity between the antigenic changes induced in T by the binding of both p53 and polymerase. We now extend this analysis to a larger collection of anti-T antibodies and formally establish that p53 and DNA polymerase alpha can compete for binding to the SV40 T antigen. At a critical concentration of the three components it is possible to detect a trimeric complex of T, p53 and DNA polymerase alpha. Our observations have important implications for the control by these nuclear oncogenes of viral and cellular DNA synthesis and viral host range in both normal and transformed cells. We present a model for the action of p53 in growth control.

摘要

猴病毒40的大T抗原(T)是一种多功能蛋白,对于病毒DNA复制和细胞转化均不可或缺。在病毒感染细胞和转化细胞中,T抗原均会与宿主蛋白p53形成特定的蛋白复合物。p53最近被证明是一种癌基因,但其正常功能尚不清楚。我们之前建立了一种放射免疫分析法,以研究新描述的T抗原与DNA聚合酶α之间的复合物,并注意到p53和聚合酶与T结合所诱导的抗原变化之间存在相似性。我们现在将这种分析扩展到更多种类的抗T抗体,并正式确定p53和DNA聚合酶α可以竞争与SV40 T抗原的结合。在三种成分的临界浓度下,可以检测到T、p53和DNA聚合酶α的三聚体复合物。我们的观察结果对于这些核癌基因在正常细胞和转化细胞中对病毒和细胞DNA合成以及病毒宿主范围的控制具有重要意义。我们提出了一个p53在生长控制中的作用模型。

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