Program in Cell Cycle and Cancer Biology, Oklahoma Medical Research Foundation, Oklahoma City, Oklahoma 73104, USA.
J Biol Chem. 2012 Oct 5;287(41):34325-36. doi: 10.1074/jbc.M112.400192. Epub 2012 Aug 15.
Acetylation of the Smc3 subunit of cohesin is essential to establish functional cohesion between sister chromatids. Smc3 acetylation is catalyzed by members of the Eco family of acetyltransferases, although the mechanism by which acetylation is regulated and how it promotes cohesion are largely unknown. In vertebrates, the cohesin complex binds to chromatin during mitotic exit and is converted to a functional form during or shortly after DNA replication. The conserved proliferating cell nuclear antigen-interacting protein box motif in yeast Eco1 is required for function, and cohesin is acetylated during the S phase. This has led to the notion that acetylation of cohesin is stimulated by interaction of Eco1 with the replication machinery. Here we show that in vertebrates Smc3 acetylation occurs independently of DNA replication. Smc3 is readily acetylated before replication is initiated and after DNA replication is complete. However, we also show that functional acetylation occurs only in association with the replication machinery: disruption of the interaction between XEco2 and proliferating cell nuclear antigen prevents cohesion establishment while having little impact on the overall levels of Smc3 acetylation. These results demonstrate that Smc3 acetylation can occur throughout interphase but that only acetylation in association with the replication fork promotes sister chromatid cohesion. These data reveal how the generation of cohesion is limited to the appropriate time and place during the cell cycle and provide insight into the mechanism by which acetylation ensures cohesion.
着丝粒蛋白 Smc3 亚基的乙酰化对于在姐妹染色单体之间建立功能性黏合至关重要。Smc3 的乙酰化由 Eco 家族乙酰转移酶成员催化,但乙酰化的调控机制以及它如何促进黏合在很大程度上尚不清楚。在脊椎动物中,黏合复合物在有丝分裂末期与染色质结合,并在 DNA 复制期间或之后不久转化为功能性形式。酿酒酵母 Eco1 中的保守增殖细胞核抗原相互作用蛋白盒基序对于功能是必需的,并且在 S 期内黏合蛋白被乙酰化。这导致了这样一种观点,即 Eco1 与复制机制的相互作用刺激了黏合蛋白的乙酰化。在这里,我们表明在脊椎动物中,Smc3 的乙酰化独立于 DNA 复制发生。在复制开始之前和完成之后,Smc3 很容易被乙酰化。然而,我们还表明,功能乙酰化仅与复制机制相关:破坏 XEco2 和增殖细胞核抗原之间的相互作用会阻止黏合的建立,而对 Smc3 乙酰化的整体水平几乎没有影响。这些结果表明,Smc3 乙酰化可以在整个间期中发生,但只有与复制叉相关的乙酰化才能促进姐妹染色单体的黏合。这些数据揭示了黏合的产生如何在细胞周期的适当时间和地点受到限制,并为乙酰化确保黏合的机制提供了深入的了解。