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猿猴病毒40 DNA体外复制的物种特异性需要人DNA聚合酶α的多种功能。

Species specificity of simian virus 40 DNA replication in vitro requires multiple functions of human DNA polymerase alpha.

作者信息

Smith Richard W P, Steffen Claudia, Grosse Frank, Nasheuer Heinz-Peter

机构信息

Abteilung Biochemie, Institut für Molekulare Biotechnologie, D-07745 Jena, Germany.

出版信息

J Biol Chem. 2002 Jun 7;277(23):20541-8. doi: 10.1074/jbc.M201908200. Epub 2002 Apr 1.

Abstract

Human cell extracts support the replication of SV40 DNA, whereas mouse cell extracts do not. Species specificity is determined at the level of initiation of DNA replication, and it was previously found that this requires the large subunit, p180, of DNA polymerase alpha-primase to be of human origin. Furthermore, a functional interaction between SV40 large T antigen (TAg) and p180 is essential for viral DNA replication. In this study we determined that the N-terminal regions of human p180, which contain the TAg-binding sites, can be replaced with those of murine origin without losing the ability to support SV40 DNA replication in vitro. The same substitutions do not prevent SV40 TAg from stimulating the activity of DNA polymerase alpha-primase on single-stranded DNA in the presence of replication protein A. Furthermore, biophysical studies show that the interactions of human and murine DNA polymerase alpha-primase with SV40 TAg are of a similar magnitude. These studies strongly suggest that requirement of SV40 DNA replication for human DNA polymerase alpha depends neither on the TAg-binding site being of human origin nor on the strength of the binary interaction between SV40 TAg and DNA polymerase alpha-primase but rather on sequences in the C-terminal region of human p180.

摘要

人类细胞提取物支持SV40 DNA的复制,而小鼠细胞提取物则不支持。物种特异性在DNA复制起始水平上确定,此前发现这需要DNA聚合酶α-引发酶的大亚基p180为人类来源。此外,SV40大T抗原(TAg)与p180之间的功能相互作用对于病毒DNA复制至关重要。在本研究中,我们确定人类p180的N端区域(包含TAg结合位点)可以被鼠源区域取代,而不会丧失体外支持SV40 DNA复制的能力。相同的替换并不妨碍SV40 TAg在复制蛋白A存在的情况下刺激DNA聚合酶α-引发酶对单链DNA的活性。此外,生物物理研究表明,人类和小鼠DNA聚合酶α-引发酶与SV40 TAg的相互作用程度相似。这些研究强烈表明,SV40 DNA复制对人类DNA聚合酶α的需求既不取决于TAg结合位点为人类来源,也不取决于SV40 TAg与DNA聚合酶α-引发酶之间二元相互作用的强度,而是取决于人类p180 C端区域的序列。

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