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Merck
CN

A new MCM modification cycle regulates DNA replication initiation.

Nature structural & molecular biology (2016-02-09)
Lei Wei, Xiaolan Zhao
摘要

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.

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Millipore
抗-V5 琼脂糖亲和凝胶 小鼠抗, purified immunoglobulin, clone V5-10
Sigma-Aldrich
过氧化物酶抗过氧化物酶可溶性复合物 兔抗, affinity isolated antibody, buffered aqueous solution