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Stress-mediated exit to quiescence restricted by increasing persistence in CDK4/6 activation.


ABSTRACT: Mammalian cells typically start the cell-cycle entry program by activating cyclin-dependent protein kinase 4/6 (CDK4/6). CDK4/6 activity is clinically relevant as mutations, deletions, and amplifications that increase CDK4/6 activity contribute to the progression of many cancers. However, when CDK4/6 is activated relative to CDK2 remained incompletely understood. Here, we developed a reporter system to simultaneously monitor CDK4/6 and CDK2 activities in single cells and found that CDK4/6 activity increases rapidly before CDK2 activity gradually increases, and that CDK4/6 activity can be active after mitosis or inactive for variable time periods. Markedly, stress signals in G1 can rapidly inactivate CDK4/6 to return cells to quiescence but with reduced probability as cells approach S phase. Together, our study reveals a regulation of G1 length by temporary inactivation of CDK4/6 activity after mitosis, and a progressively increasing persistence in CDK4/6 activity that restricts cells from returning to quiescence as cells approach S phase.

SUBMITTER: Yang HW 

PROVIDER: S-EPMC7213986 | biostudies-literature | 2020 Apr

REPOSITORIES: biostudies-literature

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Stress-mediated exit to quiescence restricted by increasing persistence in CDK4/6 activation.

Yang Hee Won HW   Cappell Steven D SD   Jaimovich Ariel A   Liu Chad C   Chung Mingyu M   Daigh Leighton H LH   Pack Lindsey R LR   Fan Yilin Y   Regot Sergi S   Covert Markus M   Meyer Tobias T  

eLife 20200407


Mammalian cells typically start the cell-cycle entry program by activating cyclin-dependent protein kinase 4/6 (CDK4/6). CDK4/6 activity is clinically relevant as mutations, deletions, and amplifications that increase CDK4/6 activity contribute to the progression of many cancers. However, when CDK4/6 is activated relative to CDK2 remained incompletely understood. Here, we developed a reporter system to simultaneously monitor CDK4/6 and CDK2 activities in single cells and found that CDK4/6 activi  ...[more]

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