Iizuka Masayoshi, Matsui Tomoko, Takisawa Haruhiko, Smith M Mitchell
Department of Microbiology, University of Virginia Health System, P.O. Box 800734, Charlottesville, VA 22908-0734, USA.
Mol Cell Biol. 2006 Feb;26(3):1098-108. doi: 10.1128/MCB.26.3.1098-1108.2006.
The initiation of DNA replication is tightly regulated in eukaryotic cells to ensure that the genome is precisely duplicated once and only once per cell cycle. This is accomplished by controlling the assembly of a prereplicative complex (pre-RC) which involves the sequential binding to replication origins of the origin recognition complex (ORC), Cdc6/Cdc18, Cdt1, and the minichromosome maintenance complex (Mcm2-Mcm7, or Mcm2-7). Several mechanisms of pre-RC regulation are known, including ATP utilization, cyclin-dependent kinase levels, protein turnover, and Cdt1 binding by geminin. Histone acetylation may also affect the initiation of DNA replication, but at present neither the enzymes nor the steps involved are known. Here, we show that Hbo1, a member of the MYST histone acetyltransferase family, is a previously unrecognized positive regulatory factor for pre-RC assembly. When Hbo1 expression was inhibited in human cells, Mcm2-7 failed to associate with chromatin even though ORC and Cdc6 loading was normal. When Xenopus egg extracts were immunodepleted of Xenopus Hbo1 (XHbo1), chromatin binding of Mcm2-7 was lost, and DNA replication was abolished. The binding of Mcm2-7 to chromatin in XHbo1-depleted extracts could be restored by the addition of recombinant Cdt1.
在真核细胞中,DNA复制的起始受到严格调控,以确保基因组在每个细胞周期中精确复制一次且仅复制一次。这是通过控制前复制复合体(pre-RC)的组装来实现的,该复合体涉及依次与复制起点结合的起点识别复合体(ORC)、Cdc6/Cdc18、Cdt1以及微型染色体维持复合体(Mcm2-Mcm7,或Mcm2-7)。已知pre-RC调控的几种机制,包括ATP利用、细胞周期蛋白依赖性激酶水平、蛋白质周转以及geminin对Cdt1的结合。组蛋白乙酰化也可能影响DNA复制的起始,但目前涉及的酶和步骤均未知。在此,我们表明,MYST组蛋白乙酰转移酶家族成员Hbo1是一种此前未被认识的pre-RC组装的正调控因子。当人类细胞中Hbo1的表达受到抑制时,尽管ORC和Cdc6的加载正常,但Mcm2-7未能与染色质结合。当非洲爪蟾卵提取物中的非洲爪蟾Hbo1(XHbo1)被免疫去除后,Mcm2-7与染色质的结合丧失,DNA复制被阻断。通过添加重组Cdt1,可以恢复XHbo1缺失提取物中Mcm2-7与染色质的结合。
