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一种新的MCM修饰循环调节DNA复制起始。

A new MCM modification cycle regulates DNA replication initiation.

作者信息

Wei Lei, Zhao Xiaolan

机构信息

Molecular Biology Program, Memorial Sloan Kettering Cancer Center, New York, New York, USA.

Gerstner Sloan Kettering Graduate School of Biomedical Sciences, Memorial Sloan Kettering Cancer Center, New York, New York, USA.

出版信息

Nat Struct Mol Biol. 2016 Mar;23(3):209-16. doi: 10.1038/nsmb.3173. Epub 2016 Feb 8.

Abstract

The MCM DNA helicase is a central regulatory target during genome replication. MCM is kept inactive during G1, and it initiates replication after being activated in S phase. During this transition, the only known chemical change to MCM is the gain of multisite phosphorylation that promotes cofactor recruitment. Because replication initiation is intimately linked to multiple biological cues, additional changes to MCM can provide further regulatory points. Here, we describe a yeast MCM SUMOylation cycle that regulates replication. MCM subunits undergo SUMOylation upon loading at origins in G1 before MCM phosphorylation. MCM SUMOylation levels then decline as MCM phosphorylation levels rise, thus suggesting an inhibitory role of MCM SUMOylation during replication. Indeed, increasing MCM SUMOylation impairs replication initiation, partly through promoting the recruitment of a phosphatase that decreases MCM phosphorylation and activation. We propose that MCM SUMOylation counterbalances kinase-based regulation, thus ensuring accurate control of replication initiation.

摘要

MCM DNA解旋酶是基因组复制过程中的核心调控靶点。MCM在G1期保持无活性状态,在S期被激活后启动复制。在这一转变过程中,已知MCM唯一的化学变化是多位点磷酸化增加,这促进了辅因子的募集。由于复制起始与多种生物学信号密切相关,MCM的其他变化可能提供更多的调控点。在此,我们描述了一种调节复制的酵母MCM SUMO化循环。MCM亚基在G1期于复制起点加载后、MCM磷酸化之前发生SUMO化。随着MCM磷酸化水平升高,MCM SUMO化水平随后下降,因此表明MCM SUMO化在复制过程中具有抑制作用。确实,增加MCM SUMO化会损害复制起始,部分原因是促进了一种磷酸酶的募集,该磷酸酶会降低MCM磷酸化和激活水平。我们提出,MCM SUMO化可平衡基于激酶的调控,从而确保对复制起始进行精确控制。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/29a6/4823995/3211c7453131/nihms771419f1.jpg

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