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本文引用的文献

1
The intrinsic DNA helicase activity of Methanobacterium thermoautotrophicum delta H minichromosome maintenance protein.嗜热自养甲烷杆菌δH微小染色体维持蛋白的内在DNA解旋酶活性。
J Biol Chem. 2000 May 19;275(20):15049-59. doi: 10.1074/jbc.M000398200.
2
Sequential MCM/P1 subcomplex assembly is required to form a heterohexamer with replication licensing activity.需要依次进行MCM/P1亚复合物组装以形成具有复制许可活性的异源六聚体。
J Biol Chem. 2000 Jan 28;275(4):2491-8. doi: 10.1074/jbc.275.4.2491.
3
Biochemical analysis of the intrinsic Mcm4-Mcm6-mcm7 DNA helicase activity.对内在的Mcm4-Mcm6-Mcm7 DNA解旋酶活性的生化分析。
Mol Cell Biol. 1999 Dec;19(12):8003-15. doi: 10.1128/MCB.19.12.8003.
4
Stat protein transactivation domains recruit p300/CBP through widely divergent sequences.信号转导和转录激活因子(Stat)蛋白的反式激活结构域通过差异很大的序列招募p300/CBP。
J Biol Chem. 1999 Sep 3;274(36):25343-9. doi: 10.1074/jbc.274.36.25343.
5
MCM proteins are associated with RNA polymerase II holoenzyme.微小染色体维持(MCM)蛋白与RNA聚合酶II全酶相关联。
Mol Cell Biol. 1999 Sep;19(9):6154-63. doi: 10.1128/MCB.19.9.6154.
6
The regulation of replication origin activation.复制起点激活的调控。
Curr Opin Genet Dev. 1999 Feb;9(1):62-8. doi: 10.1016/s0959-437x(99)80009-4.
7
Ser727-dependent recruitment of MCM5 by Stat1alpha in IFN-gamma-induced transcriptional activation.Stat1α 在 IFN-γ 诱导的转录激活中通过 Ser727 依赖性方式募集 MCM5。
EMBO J. 1998 Dec 1;17(23):6963-71. doi: 10.1093/emboj/17.23.6963.
8
How cells respond to interferons.细胞如何对干扰素作出反应。
Annu Rev Biochem. 1998;67:227-64. doi: 10.1146/annurev.biochem.67.1.227.
9
MCM proteins: evolution, properties, and role in DNA replication.微小染色体维持蛋白:进化、特性及其在DNA复制中的作用
Biochim Biophys Acta. 1998 Jun 16;1398(2):113-36. doi: 10.1016/s0167-4781(98)00033-5.
10
Three-dimensional structure of the Stat3beta homodimer bound to DNA.与DNA结合的Stat3β同二聚体的三维结构。
Nature. 1998 Jul 9;394(6689):145-51. doi: 10.1038/28101.

鉴定MCM5中对MCM复合物组装以及响应干扰素-γ时Stat1介导的转录激活至关重要的两个残基。

Identification of two residues in MCM5 critical for the assembly of MCM complexes and Stat1-mediated transcription activation in response to IFN-gamma.

作者信息

DaFonseca C J, Shu F, Zhang J J

机构信息

Department of Pathology, Weill Medical College of Cornell University, 1300 York Avenue, New York, NY 10021, USA.

出版信息

Proc Natl Acad Sci U S A. 2001 Mar 13;98(6):3034-9. doi: 10.1073/pnas.061487598. Epub 2001 Mar 6.

DOI:10.1073/pnas.061487598
PMID:11248027
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC30602/
Abstract

In response to IFN-gamma, the latent cytoplasmic Stat1 (signal transducer and activator of transcription) proteins translocate into the nucleus and activate transcription. We showed previously that Stat1 recruits a group of nuclear proteins, among them MCM5 (minichromosome maintenance) and MCM3, for transcription activation. MCM5 directly interacts with the transcription activation domain (TAD) of Stat1 and enhances Stat1-mediated transcription activation. In this report, we identified two specific residues (R732, K734) in MCM5 that are required for the direct interaction between Stat1 and MCM5 both in vitro and in vivo. MCM5 containing mutations of R732/K734 did not enhance Stat1-mediated transcription activation in response to IFN-gamma. In addition, it also failed to form complexes with other MCM proteins in vivo, suggesting that these two residues may be important for an interaction domain in MCM5. Furthermore, MCM5 bearing mutations in its ATPase and helicase domains did not enhance Stat1 activity. In vitro binding assays indicate that MCM3 does not interact directly with Stat1, suggesting that the presence of MCM3 in the group of Stat1TAD-interacting proteins is due to the association of MCM3 with MCM5. Finally, gel filtration analyses of nuclear extracts from INF-gamma-treated cells demonstrate that there is a MCM5/3 subcomplex coeluting with Stat1. Together, these results strongly suggest that Stat1 recruits a MCM5/3 subcomplex through direct interaction with MCM5 in the process of IFN-gamma-induced gene activation.

摘要

在对干扰素-γ的应答中,潜伏的细胞质信号转导子和转录激活子1(Stat1)蛋白转位进入细胞核并激活转录。我们之前表明,Stat1招募一组核蛋白,其中包括微小染色体维持蛋白5(MCM5)和MCM3,用于转录激活。MCM5直接与Stat1的转录激活结构域(TAD)相互作用,并增强Stat1介导的转录激活。在本报告中,我们鉴定出MCM5中的两个特定残基(R732、K734),它们是Stat1与MCM5在体外和体内直接相互作用所必需的。含有R732/K734突变的MCM5不能增强Stat1介导的对干扰素-γ的转录激活。此外,它在体内也无法与其他MCM蛋白形成复合物,这表明这两个残基可能对MCM5中的一个相互作用结构域很重要。此外,在其ATP酶和螺旋酶结构域中带有突变的MCM5不能增强Stat1活性。体外结合试验表明,MCM3不直接与Stat1相互作用,这表明Stat1 TAD相互作用蛋白组中MCM3的存在是由于MCM3与MCM5的关联。最后,对干扰素-γ处理细胞的核提取物进行凝胶过滤分析表明,有一个MCM5/3亚复合物与Stat1共洗脱。总之,这些结果强烈表明,在干扰素-γ诱导的基因激活过程中,Stat1通过与MCM5的直接相互作用招募一个MCM5/3亚复合物。