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UBE2T、范可尼贫血核心复合物和FANCD2被独立招募至染色质:FANCD2单泛素化调控的基础。

UBE2T, the Fanconi anemia core complex, and FANCD2 are recruited independently to chromatin: a basis for the regulation of FANCD2 monoubiquitination.

作者信息

Alpi Arno, Langevin Frederic, Mosedale Georgina, Machida Yuichi J, Dutta Anindya, Patel Ketan J

机构信息

Laboratory of Molecular Biology, Medical Research Council, Cambridge, United Kingdom.

出版信息

Mol Cell Biol. 2007 Dec;27(24):8421-30. doi: 10.1128/MCB.00504-07. Epub 2007 Oct 15.

DOI:10.1128/MCB.00504-07
PMID:17938197
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2169426/
Abstract

The Fanconi anemia (FA) nuclear core complex and the E2 ubiquitin-conjugating enzyme UBE2T are required for the S phase and DNA damage-restricted monoubiquitination of FANCD2. This constitutes a key step in the FA tumor suppressor pathway, and much attention has been focused on the regulation at this point. Here, we address the importance of the assembly of the FA core complex and the subcellular localization of UBE2T in the regulation of FANCD2 monoubiquitination. We establish three points. First, the stable assembly of the FA core complex can be dissociated of its ability to function as an E3 ubiquitin ligase. Second, the actual E3 ligase activity is not determined by the assembly of the FA core complex but rather by its DNA damage-induced localization to chromatin. Finally, UBE2T and FANCD2 access this subcellular fraction independently of the FA core complex. FANCD2 monoubiquitination is therefore not regulated by multiprotein complex assembly but by the formation of an active E2/E3 holoenzyme on chromatin.

摘要

范可尼贫血(FA)核心复合物和E2泛素结合酶UBE2T是FANCD2在S期和DNA损伤限制的单泛素化所必需的。这是FA肿瘤抑制途径中的关键步骤,并且此时的调控已备受关注。在此,我们探讨FA核心复合物的组装以及UBE2T的亚细胞定位在FANCD2单泛素化调控中的重要性。我们确立了三点。第一,FA核心复合物的稳定组装可与其作为E3泛素连接酶的功能解离。第二,实际的E3连接酶活性并非由FA核心复合物的组装决定,而是由其DNA损伤诱导的染色质定位决定。最后,UBE2T和FANCD2独立于FA核心复合物进入该亚细胞组分。因此,FANCD2单泛素化不是由多蛋白复合物组装调控,而是由染色质上活性E2/E3全酶的形成调控。

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