Author
Listed:
- Tingjun Lei
(Sichuan University)
- Peixuan Zhang
(Sichuan University)
- Xudong Zhang
(Sichuan University)
- Xue Xiao
(Sichuan University)
- Jingli Zhang
(Hospital 363 of Aviation Industry Corporation of China)
- Tong Qiu
(Sichuan University)
- Qian Dai
(Sichuan University)
- Yujun Zhang
(Sichuan University)
- Ling Min
(Sichuan University)
- Qian Li
(Hospital 363 of Aviation Industry Corporation of China)
- Rutie Yin
(Sichuan University)
- Ping Ding
(Sichuan Cunde Therapeutics)
- Ni Li
(University of Chinese Academy of Sciences)
- Yi Qu
(Sichuan University)
- Dezhi Mu
(Sichuan University)
- Jun Qin
(University of Chinese Academy of Sciences)
- Xiaofeng Zhu
(Sichuan University)
- Zhi-Xiong Xiao
(Sichuan University)
- Qintong Li
(Sichuan University)
Abstract
The assembly of prereplicative complex (pre-RC) during G1 phase must be tightly controlled to sustain cell proliferation and maintain genomic stability. Mechanisms to prevent pre-RC formation in G2/M and S phases are well appreciated, whereas how cells ensure efficient pre-RC assembly during G1 is less clear. Here we report that cyclin K regulates pre-RC formation. We find that cyclin K expression positively correlates with cell proliferation, and knockdown of cyclin K or its cognate kinase CDK12 prevents the assembly of pre-RC in G1 phase. Mechanistically we uncover that cyclin K promotes pre-RC assembly by restricting cyclin E1 activity in G1. We identify a cyclin K-dependent, novel phosphorylation site in cyclin E1 that disrupts its interaction with CDK2. Importantly, this antagonistic relationship is largely recapitulated in cyclin E1-overexpressing tumors. We discuss the implications of our findings in light of recent reports linking cyclin K and CDK12 to human tumorigenesis.
Suggested Citation
Tingjun Lei & Peixuan Zhang & Xudong Zhang & Xue Xiao & Jingli Zhang & Tong Qiu & Qian Dai & Yujun Zhang & Ling Min & Qian Li & Rutie Yin & Ping Ding & Ni Li & Yi Qu & Dezhi Mu & Jun Qin & Xiaofeng Zh, 2018.
"Cyclin K regulates prereplicative complex assembly to promote mammalian cell proliferation,"
Nature Communications, Nature, vol. 9(1), pages 1-15, December.
Handle:
RePEc:nat:natcom:v:9:y:2018:i:1:d:10.1038_s41467-018-04258-w
DOI: 10.1038/s41467-018-04258-w
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