School of Environmental Science and Engineering, Kochi University of Technology, 185 Miyanokuchi, Tosayamada, Kami, Kochi 782-8502, Japan.
Genetics. 2021 Mar 3;217(1):1-11. doi: 10.1093/genetics/iyaa001.
DNA replication in eukaryotes is a multi-step process that consists of three main reactions: helicase loading (licensing), helicase activation (firing), and nascent DNA synthesis (elongation). Although the contributions of some chromatin regulatory factors in the licensing and elongation reaction have been determined, their functions in the firing reaction remain elusive. In the budding yeast Saccharomyces cerevisiae, Sld3, Sld7, and Cdc45 (3-7-45) are rate-limiting in the firing reaction and simultaneous overexpression of 3-7-45 causes untimely activation of late and dormant replication origins. Here, we found that 3-7-45 overexpression not only activated dormant origins in the silenced locus, HMLα, but also exerted an anti-silencing effect at this locus. For these, interaction between Sld3 and Esa1, a conserved histone acetyltransferase, was responsible. Moreover, the Sld3-Esa1 interaction was required for the untimely activation of late origins. These results reveal the Sld3-Esa1 interaction as a novel level of regulation in the firing reaction.
真核生物的 DNA 复制是一个多步骤的过程,包括三个主要反应:解旋酶加载(许可)、解旋酶激活(引发)和新生 DNA 合成(延伸)。尽管已经确定了一些染色质调节因子在许可和延伸反应中的作用,但它们在引发反应中的功能仍然难以捉摸。在芽殖酵母酿酒酵母中,Sld3、Sld7 和 Cdc45(3-7-45)在引发反应中是限速的,并且 3-7-45 的同时过表达会导致晚期和休眠复制起点的过早激活。在这里,我们发现 3-7-45 的过表达不仅激活了沉默位点 HMLα 中的休眠起点,而且在该位点还产生了抗沉默效应。对于这些,Sld3 和 Esa1(一种保守的组蛋白乙酰转移酶)之间的相互作用是负责的。此外,Sld3-Esa1 相互作用对于晚期起源的过早激活是必需的。这些结果揭示了 Sld3-Esa1 相互作用是引发反应中的一个新的调节水平。
