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DNA 腺嘌呤甲基化是复制每个细胞周期中霍乱弧菌两个染色体所必需的。

DNA adenine methylation is required to replicate both Vibrio cholerae chromosomes once per cell cycle.

机构信息

Center for Cancer Research, National Cancer Institute, Bethesda, Maryland, United States of America.

出版信息

PLoS Genet. 2010 May 6;6(5):e1000939. doi: 10.1371/journal.pgen.1000939.

Abstract

DNA adenine methylation is widely used to control many DNA transactions, including replication. In Escherichia coli, methylation serves to silence newly synthesized (hemimethylated) sister origins. SeqA, a protein that binds to hemimethylated DNA, mediates the silencing, and this is necessary to restrict replication to once per cell cycle. The methylation, however, is not essential for replication initiation per se but appeared so when the origins (oriI and oriII) of the two Vibrio cholerae chromosomes were used to drive plasmid replication in E. coli. Here we show that, as in the case of E. coli, methylation is not essential for oriI when it drives chromosomal replication and is needed for once-per-cell-cycle replication in a SeqA-dependent fashion. We found that oriII also needs SeqA for once-per-cell-cycle replication and, additionally, full methylation for efficient initiator binding. The requirement for initiator binding might suffice to make methylation an essential function in V. cholerae. The structure of oriII suggests that it originated from a plasmid, but unlike plasmids, oriII makes use of methylation for once-per-cell-cycle replication, the norm for chromosomal but not plasmid replication.

摘要

DNA 腺嘌呤甲基化被广泛用于控制许多 DNA 转化,包括复制。在大肠杆菌中,甲基化用于沉默新合成的(半甲基化)姐妹起始点。与半甲基化 DNA 结合的 SeqA 蛋白介导沉默,这对于将复制限制在每个细胞周期一次是必要的。然而,甲基化本身对于复制起始并不是必需的,但当使用两个霍乱弧菌染色体的 oriI 和 oriII 作为起点来驱动大肠杆菌中的质粒复制时,情况似乎如此。在这里,我们表明,与大肠杆菌的情况一样,当 oriI 驱动染色体复制时,甲基化对于 oriI 不是必需的,并且以 SeqA 依赖性方式需要在每个细胞周期中复制一次。我们发现 oriII 也需要 SeqA 才能进行一次细胞周期的复制,此外,还需要完全甲基化才能有效结合起始子。对起始子结合的需求可能足以使甲基化成为霍乱弧菌的必需功能。oriII 的结构表明它起源于质粒,但与质粒不同的是,oriII 利用甲基化来进行一次细胞周期的复制,这是染色体复制的常态,而不是质粒复制的常态。

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