期刊
MOLECULAR AND CELLULAR BIOLOGY
卷 32, 期 15, 页码 3107-3120出版社
AMER SOC MICROBIOLOGY
DOI: 10.1128/MCB.00362-12
关键词
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资金
- NSF-CMMB-IGERT
- NIH [AI083025, GM088252]
- NSF [0822613, 0843604]
- ACS [RSG-11-174-01-RMC]
- Div Of Molecular and Cellular Bioscience
- Direct For Biological Sciences [0843604] Funding Source: National Science Foundation
In eukaryotes, initiation of DNA replication requires the assembly of a multiprotein prereplicative complex (pre-RC) at the origins. We recently reported that a WD repeat-containing protein, origin recognition complex (ORC)-associated (ORCA/LRWDI), plays a crucial role in stabilizing ORC to chromatin. Here, we find that ORCA is required for the G(1)-to-S-phase transition in human cells. In addition to binding to ORC, ORCA associates with Cdt1 and its inhibitor, geminin. Single-molecule pulldown experiments demonstrate that each molecule of ORCA can bind to one molecule of ORC, one molecule of Cdt1, and two molecules of geminin. Further, ORCA directly interacts with the N terminus of Orc2, and the stability of ORCA is dependent on its association with Orc2. ORCA associates with Orc2 throughout the cell cycle, with Cdt1 during mitosis and G and with geminin in post-G(1) cells. Overexpression of geminin results in the loss of interaction between ORCA and Cdt1, suggesting that increased levels of geminin in post-G(1) cells titrate Cdt1 away from ORCA. We propose that the dynamic association of ORCA with pre-RC components modulates the assembly of its interacting partners on chromatin and facilitates DNA replication initiation.
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