Several tetratricopeptide repeat (TPR) motifs of FANCG are required for assembly of the BRCA2/D1-D2-G-X3 complex, FANCD2 monoubiquitylation and phleomycin resistance.

Wilson JB; Blom E; Cunningham R; Xiao Y; Kupfer GM; Jones NJ

首页> 外文期刊>Mutation Research: International Journal on Mutagenesis, Chromosome Breakage and Related Subjects >Several tetratricopeptide repeat (TPR) motifs of FANCG are required for assembly of the BRCA2/D1-D2-G-X3 complex, FANCD2 monoubiquitylation and phleomycin resistance.

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Several tetratricopeptide repeat (TPR) motifs of FANCG are required for assembly of the BRCA2/D1-D2-G-X3 complex, FANCD2 monoubiquitylation and phleomycin resistance.

机译：BRCA2 / D1-D2-G-X3复合物的组装，FANCD2单泛素化和磷脂酶抗性需要FANCG的几个四三肽重复（TPR）基序。

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The Fanconi anaemia (FA) FANCG protein is an integral component of the FA nuclear core complex that is required for monoubiquitylation of FANCD2. FANCG is also part of another protein complex termed D1-D2-G-X3 that contains FANCD2 and the homologous recombination repair proteins BRCA2 (FANCD1) and XRCC3. Formation of the D1-D2-G-X3 complex is mediated by serine-7 phosphorylation of FANCG and occurs independently of the FA core complex and FANCD2 monoubiquitylation. FANCG contains seven tetratricopeptide repeat (TPR) motifs that mediate protein-protein interactions and here we show that mutation of several of the TPR motifs at a conserved consensus residue ablates the in vivo binding activity of FANCG. Expression of mutated TPR1, TPR2, TPR5 and TPR6 in Chinese hamster fancg mutant NM3 fails to functionally complement its hypersensitivities to mitomycin C (MMC) and phleomycin and fails to restore FANCD2 monoubiquitylation. Using co-immunoprecipitation analysis, we demonstrate that these TPR-mutated FANCG proteins fail to interact with BRCA2, XRCC3, FANCA or FANCF. The interactions of other proteins in the D1-D2-G-X3 complex are also absent, including the interaction of BRCA2 with both the monoubiquitylated (FANCD2-L) and non-ubiquitylated (FANCD2-S) isoforms of FANCD2. Interestingly, a mutation of TPR7 (R563E), that complements the MMC and phleomycin hypersensitivity of human FA-G EUFA316 cells, fails to complement NM3, despite the mutated FANCG protein co-precipitating with FANCA, BRCA2 and XRCC3. Whilst interaction of TPR7-mutated FANCG with FANCF does appear to be reduced in NM3, FANCD2 is monoubiquitylated suggesting that sub-optimal interactions of FANCG in the core complex and the D1-D2-G-X3 complex are responsible for the observed MMC- and phleomycin-hypersensitivity, rather than a defect in FANCD2 monoubiquitylation. Our data demonstrate that FANCG functions as a mediator of protein-protein interactions and is vital for the assembly of multi-protein complexes including the FA core complex and the D1-D2-G-X3 complex.

机译：范可尼贫血（FA）FANCG蛋白是FANCD2单泛素化所需的FA核核心复合物的组成部分。 FANCG还是另一种称为D1-D2-G-X3的蛋白质复合物的一部分，该复合物包含FANCD2以及同源重组修复蛋白BRCA2（FANCD1）和XRCC3。 D1-D2-G-X3复合物的形成由FANCG的丝氨酸7磷酸化介导，并且独立于FA核心复合物和FANCD2单泛素化而发生。 FANCG包含七个介导蛋白质-蛋白质相互作用的四三肽重复（TPR）主题，在这里我们显示保守保守共有残基上的几个TPR主题的突变消除了FANCG的体内结合活性。在中国仓鼠fancg突变体NM3中突变TPR1，TPR2，TPR5和TPR6的表达无法在功能上补充其对丝裂霉素C（MMC）和细霉素的超敏性，并且无法恢复FANCD2单泛素化。使用免疫共沉淀分析，我们证明了这些TPR突变的FANCG蛋白无法与BRCA2，XRCC3，FANCA或FANCF相互作用。 D1-D2-G-X3复合物中也没有其他蛋白质的相互作用，包括BRCA2与FANCD2的单泛素化（FANCD2-L）和非泛素化（FANCD2-S）同种型的相互作用。有趣的是，尽管突变的FANCG蛋白与FANCA，BRCA2和XRCC3共同沉淀，TPR7（R563E）的突变补充了人类FA-G EUFA316细胞的MMC和细霉素超敏性，却未能补充NM3。尽管在NM3中，TPR7突变的FANCG与FANCF的相互作用似乎有所减少，但FANCD2是单泛素化的，这表明核心复合物和D1-D2-G-X3复合物中FANCG的次佳相互作用是所观察到的MMC-和phleomycin过敏，而不是FANCD2单泛素化的缺陷。我们的数据表明，FANCG充当蛋白质-蛋白质相互作用的介质，对于组装多种蛋白质复合物（包括FA核心复合物和D1-D2-G-X3复合物）至关重要。

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《Mutation Research: International Journal on Mutagenesis, Chromosome Breakage and Related Subjects》 |2010年第2期|共9页
作者
Wilson JB; Blom E; Cunningham R; Xiao Y; Kupfer GM; Jones NJ;
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1. Several tetratricopeptide repeat (TPR) motifs of FANCG are required for assembly of the BRCA2/D1-D2-G-X3 complex, FANCD2 monoubiquitylation and phleomycin resistance. [J] . Wilson JB, Blom E, Cunningham R, Mutation Research: International Journal on Mutagenesis, Chromosome Breakage and Related Subjects . 2010,第1a2期

机译：BRCA2 / D1-D2-G-X3复合物的组装，FANCD2单泛素化和磷脂酶抗性需要FANCG的几个四三肽重复（TPR）基序。
2. FANCG promotes formation of a newly identified protein complex containing BRCA2, FANCD2 and XRCC3 [J] . J B Wilson, K Yamamoto, A S Marriott, Oncogene . 2008,第26期

机译：FANCG促进含有BRCA2，FANCD2和XRCC3的新鉴定的蛋白质复合物的形成
3. Gα_(16) activates Ras by forming a complex with tetratricopeptide repeat 1 (TPR1) and Son of Sevenless (SOS) [J] . Liu A.M.F., Lo R.K.H., Lee M.M.K., Cellular Signalling . 2010,第10期

机译：Gα_（16）通过与四肽重复序列1（TPR1）和七人之子（SOS）形成复合物来激活Ras
4. The Role of Multiple Sequence Repeat Motifs in the Assembly of Multi-protein Complexes [C] . David Barford Macromolecular crystallography: deciphering the structure, function and dynamics of biological molecules . 2010

机译：多序列重复基序在多蛋白复合物装配中的作用
5. Several tetratricopeptide repeat (TPR) motifs of FANCG are required for assembly of the BRCA2/D1-D2-G-X3 complex FANCD2 monoubiquitylation and phleomycin resistance [O] . James B. Wilson, Eric Blom, Ryan Cunningham, -1

机译：组装BRCA2 / D1-D2-G-X3复合物FANCD2单相中素和富含霉素抗性所需的几种四氢肽重复（TPR）基序。
6. Several tetratricopeptide repeat (TPR) motifs of FANCG are required for assembly of the BRCA2/D1-D2-G-X3 complex, FANCD2 monoubiquitylation and phleomycin resistance [O] . James B. Wilson, Eric Blom, Ryan Cunningham, 2010

机译：组装BRCA2 / D1-D2-G-X3复合物，FANCD2单相中素和富含霉素抗性所需的几种四氢肽重复（TPR）基序。

Several tetratricopeptide repeat (TPR) motifs of FANCG are required for assembly of the BRCA2/D1-D2-G-X3 complex, FANCD2 monoubiquitylation and phleomycin resistance.

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