期刊
MOLECULAR CELL
卷 44, 期 1, 页码 85-96出版社
CELL PRESS
DOI: 10.1016/j.molcel.2011.08.028
关键词
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资金
- Deutsche Forschungsgemeinschaft [FOR885, SFB635, HO 2541/4-1, SPP1384]
- Rubicon European Union Network of Excellence [SPP1384]
- Cancer Research UK [C303/A7399]
- Cancer Research UK CDA
- Wellcome Trust
- EMBO
Faithful transmission of genomic information requires tight spatiotemporal regulation of DNA replication factors. In the licensing step of DNA replication, CDT-1 is loaded onto chromatin to subsequently promote the recruitment of additional replication factors, including CDC-45 and GINS. During the elongation step, the CDC-45/GINS complex moves with the replication fork; however, it is largely unknown how its chromatin association is regulated. Here, we show that the chaperone-like ATPase CDC-48/p97 coordinates degradation of CDT-1 with release of the CDC-45/GINS complex. C. elegans embryos lacking CDC-48 or its cofactors UFD-1/NPL-4 accumulate CDT-1 on mitotic chromatin, indicating a critical role of CDC-48 in CDT-1 turnover. Strikingly, CDC-48(UFD-1/NPL-4)-deficient embryos show persistent chromatin association of CDC-45/GINS, which is a consequence of CDT-1 stabilization. Moreover, our data confirmed a similar regulation in Xenopus egg extracts, emphasizing a conserved coordination of licensing and elongation events during eukaryotic DNA replication by CDC-48/p97.
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