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Mgm101: A double-duty Rad52-like protein

机译:Mgm101:双重Rad52样蛋白

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Mgm101 has well-characterized activity for the repair and replication of the mitochondrial genome. Recent work has demonstrated a further role for Mgm101 in nuclear DNA metabolism, contributing to an S-phase specific DNA interstrand cross-link repair pathway that acts redundantly with a pathway controlled by Pso2 exonuclease. Due to involvement of FANCM, FANCJ and FANCP homologues (Mph1, Chl1 and Slx4), this pathway has been described as a Fanconi anemia-like pathway. In this pathway, Mgm101 physically interacts with the DNA helicase Mph1 and the MutS (Msh2/Msh6) heterodimer, but its precise role is yet to be elucidated. Data presented here suggests that Mgm101 functionally overlaps with Rad52, supporting previous suggestions that, based on protein structure and biochemical properties, Mgm101 and Rad52 belong to a family of proteins with similar function. In addition, our data shows that this overlap extends to the function of both proteins at telomeres, where Mgm101 is required for telomere elongation during chromosome replication in rad52 defective cells. We hypothesize that Mgm101 could, in Rad52-like manner, preferentially bind single-stranded DNAs (such as at stalled replication forks, broken chromosomes and natural chromosome ends), stabilize them and mediate single-strand annealing-like homologous recombination event to prevent them from converting into toxic structures.
机译:Mgm101具有线粒体基因组修复和复制的良好特性。最近的工作证明了Mgm101在核DNA代谢中的进一步作用,有助于S期特异性DNA链间交联修复途径,该途径与Pso2核酸外切酶控制的途径多余地起作用。由于涉及FANCM,FANCJ和FANCP同源物(Mph1,Chl1和Slx4),因此该途径已被描述为类似于Fanconi贫血的途径。在此途径中,Mgm101与DNA解旋酶Mph1和MutS(Msh2 / Msh6)异二聚体发生物理相互作用,但其确切作用尚待阐明。此处提供的数据表明Mgm101在功能上与Rad52重叠,支持先前的建议,即基于蛋白质结构和生化特性,Mgm101和Rad52属于具有相似功能的蛋白质家族。此外,我们的数据表明,这种重叠延伸到端粒的两种蛋白质的功能,其中在rad52缺陷细胞中染色体复制过程中,端粒延长需要Mgm101。我们假设Mgm101可以以Rad52样的方式优先结合单链DNA(例如停滞的复制叉,断裂的染色体和天然染色体末端),稳定它们并介导单链退火样同源重组事件以防止它们从转化为有毒的结构。

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