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1
An N-terminal deletion mutant of simian virus 40 (SV40) large T antigen oligomerizes incorrectly on SV40 DNA but retains the ability to bind to DNA polymerase alpha and replicate SV40 DNA in vitro.猿猴病毒40(SV40)大T抗原的N端缺失突变体在SV40 DNA上错误地寡聚,但保留了与DNA聚合酶α结合并在体外复制SV40 DNA的能力。
J Virol. 1996 Jun;70(6):3509-16. doi: 10.1128/JVI.70.6.3509-3516.1996.
2
Stoichiometry and mechanism of assembly of SV40 T antigen complexes with the viral origin of DNA replication and DNA polymerase alpha-primase.SV40 T抗原复合物与病毒DNA复制起点及DNA聚合酶α-引发酶组装的化学计量学和机制
Biochemistry. 1998 Nov 3;37(44):15345-52. doi: 10.1021/bi9810959.
3
Mutation of the cyclin-dependent kinase phosphorylation site in simian virus 40 (SV40) large T antigen specifically blocks SV40 origin DNA unwinding.猴病毒40(SV40)大T抗原中细胞周期蛋白依赖性激酶磷酸化位点的突变特异性地阻断了SV40起始DNA的解旋。
J Virol. 1993 Aug;67(8):4992-5002. doi: 10.1128/JVI.67.8.4992-5002.1993.
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J Biol Chem. 1993 May 25;268(15):11018-27.
5
cdc2 phosphorylation of threonine 124 activates the origin-unwinding functions of simian virus 40 T antigen.苏氨酸124的cdc2磷酸化激活了猿猴病毒40 T抗原的解旋功能。
J Virol. 1993 Sep;67(9):5206-15. doi: 10.1128/JVI.67.9.5206-5215.1993.
6
Species-specific functional interactions of DNA polymerase alpha-primase with simian virus 40 (SV40) T antigen require SV40 origin DNA.DNA聚合酶α-引发酶与猿猴病毒40(SV40)T抗原的物种特异性功能相互作用需要SV40起始DNA。
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8
Two regions of simian virus 40 T antigen determine cooperativity of double-hexamer assembly on the viral origin of DNA replication and promote hexamer interactions during bidirectional origin DNA unwinding.猴病毒40 T抗原的两个区域决定了双六聚体在病毒DNA复制起点上组装的协同性,并在双向起点DNA解旋过程中促进六聚体相互作用。
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J Virol. 1998 Dec;72(12):9771-81. doi: 10.1128/JVI.72.12.9771-9781.1998.
10
Effects of T antigen and replication protein A on the initiation of DNA synthesis by DNA polymerase alpha-primase.T抗原与复制蛋白A对DNA聚合酶α-引发酶启动DNA合成的影响。
Mol Cell Biol. 1991 Apr;11(4):2108-15. doi: 10.1128/mcb.11.4.2108-2115.1991.

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Direct interaction between the N- and C-terminal portions of the herpes simplex virus type 1 origin binding protein UL9 implies the formation of a head-to-tail dimer.单纯疱疹病毒1型起始结合蛋白UL9的N端和C端部分之间的直接相互作用意味着形成了头对尾二聚体。
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The crystal structure of the SV40 T-antigen origin binding domain in complex with DNA.与DNA结合的SV40 T抗原起始结合结构域的晶体结构。
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本文引用的文献

1
Early events in eukaryotic DNA replication.真核生物DNA复制的早期事件。
Trends Cell Biol. 1992 Oct;2(10):298-303. doi: 10.1016/0962-8924(92)90119-8.
2
Interaction between T antigen and TEA domain of the factor TEF-1 derepresses simian virus 40 late promoter in vitro: identification of T-antigen domains important for transcription control.T抗原与转录增强因子TEF-1的TEA结构域之间的相互作用在体外可解除猿猴病毒40晚期启动子的抑制:鉴定对转录控制重要的T抗原结构域。
J Virol. 1996 Feb;70(2):1203-12. doi: 10.1128/JVI.70.2.1203-1212.1996.
3
The major transcriptional transactivation domain of simian virus 40 large T antigen associates nonconcurrently with multiple components of the transcriptional preinitiation complex.猿猴病毒40大T抗原的主要转录反式激活结构域与转录起始前复合物的多个组分非同时结合。
J Virol. 1996 Feb;70(2):1191-202. doi: 10.1128/JVI.70.2.1191-1202.1996.
4
Transcriptional activation by simian virus 40 large T antigen: interactions with multiple components of the transcription complex.猿猴病毒40大T抗原的转录激活:与转录复合物多个组分的相互作用
Mol Cell Biol. 1993 Feb;13(2):961-9. doi: 10.1128/mcb.13.2.961-969.1993.
5
Mutation of the cyclin-dependent kinase phosphorylation site in simian virus 40 (SV40) large T antigen specifically blocks SV40 origin DNA unwinding.猴病毒40(SV40)大T抗原中细胞周期蛋白依赖性激酶磷酸化位点的突变特异性地阻断了SV40起始DNA的解旋。
J Virol. 1993 Aug;67(8):4992-5002. doi: 10.1128/JVI.67.8.4992-5002.1993.
6
Biochemical analysis of mutants with changes in the origin-binding domain of simian virus 40 tumor antigen.对猿猴病毒40肿瘤抗原的起始结合结构域发生变化的突变体进行生化分析。
J Virol. 1993 Jul;67(7):4227-36. doi: 10.1128/JVI.67.7.4227-4236.1993.
7
An interaction between replication protein A and SV40 T antigen appears essential for primosome assembly during SV40 DNA replication.复制蛋白A与SV40 T抗原之间的相互作用对于SV40 DNA复制过程中的引发体组装似乎至关重要。
J Biol Chem. 1993 Feb 15;268(5):3389-95.
8
Initiation of simian virus 40 DNA replication requires the interaction of a specific domain of human DNA polymerase alpha with large T antigen.猿猴病毒40(Simian virus 40)DNA复制的起始需要人类DNA聚合酶α的一个特定结构域与大T抗原相互作用。
Mol Cell Biol. 1993 Feb;13(2):809-20. doi: 10.1128/mcb.13.2.809-820.1993.
9
Unusual properties of a replication-defective mutant SV40 large T antigen.
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10
The DNA-binding domain of simian virus 40 tumor antigen has multiple functions.猿猴病毒40肿瘤抗原的DNA结合结构域具有多种功能。
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猿猴病毒40(SV40)大T抗原的N端缺失突变体在SV40 DNA上错误地寡聚,但保留了与DNA聚合酶α结合并在体外复制SV40 DNA的能力。

An N-terminal deletion mutant of simian virus 40 (SV40) large T antigen oligomerizes incorrectly on SV40 DNA but retains the ability to bind to DNA polymerase alpha and replicate SV40 DNA in vitro.

作者信息

Weisshart K, Bradley M K, Weiner B M, Schneider C, Moarefi I, Fanning E, Arthur A K

机构信息

Institute for Biochemistry, Munich, Germany.

出版信息

J Virol. 1996 Jun;70(6):3509-16. doi: 10.1128/JVI.70.6.3509-3516.1996.

DOI:10.1128/JVI.70.6.3509-3516.1996
PMID:8648684
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC190225/
Abstract

A peptide encompassing the N-terminal 82 amino acids of simian virus 40 (SV40) large T antigen was previously shown to bind to the large subunit of DNA polymerase alpha-primase (I. Dornreiter, A. Höss, A. K. Arthur, and E. Fanning, EMBO J. 9:3329-3336, 1990). We report here that a mutant T antigen, T83-708, lacking residues 2 to 82 retained the ability to bind to DNA polymerase alpha-primase, implying that it carries a second binding site for DNA polymerase alpha-primase. The mutant protein also retained ATPase, helicase, and SV40 origin DNA-binding activity. However, its SV40 DNA replication activity in vitro was reduced compared with that of wild-type protein. The reduction in replication activity was accompanied by a lower DNA-binding affinity to SV40 origin sequences and aberrant oligomerization on viral origin DNA. Thus, the first 82 residues of SV40 T antigen are not strictly required for its interaction with DNA polymerase alpha-primase or for DNA replication function but may play a role in correct hexamer assembly and efficient DNA binding at the origin.

摘要

先前已表明,包含猿猴病毒40(SV40)大T抗原N端82个氨基酸的肽可与DNA聚合酶α-引发酶的大亚基结合(I. Dornreiter、A. Höss、A. K. Arthur和E. Fanning,《欧洲分子生物学组织杂志》9:3329 - 3336,1990年)。我们在此报告,缺失第2至82位残基的突变型T抗原T83 - 708仍保留与DNA聚合酶α-引发酶结合的能力,这意味着它带有DNA聚合酶α-引发酶的第二个结合位点。该突变蛋白还保留了ATP酶、解旋酶和SV40起始位点DNA结合活性。然而,与野生型蛋白相比,其体外SV40 DNA复制活性降低。复制活性的降低伴随着对SV40起始位点序列的DNA结合亲和力降低以及在病毒起始位点DNA上的异常寡聚化。因此,SV40 T抗原的前82个残基对于其与DNA聚合酶α-引发酶的相互作用或DNA复制功能并非严格必需,但可能在正确的六聚体组装以及在起始位点的有效DNA结合中发挥作用。