The p21CIP1-CDK4-DREAM axis is a master regulator of genotoxic stress-induced cellular senescence

Author:

Schmidt Ariane1,Allmann Sebastian1,Schwarzenbach Christian1,Snyder Petra2,Chen Jia-Xuan3,Nagel Georg1,Schöneis Anna1,Rasenberger Birgit1,Beli Petra3,Loewer Alexander2,Hofmann Thomas G1ORCID,Tomicic Maja T1ORCID,Christmann Markus1ORCID

Affiliation:

1. Department of Toxicology, University Medical Center of the Johannes Gutenberg University of Mainz , Obere Zahlbacher Str. 67 , D-55131  Mainz , Germany

2. Department of Biology, Technical University Darmstadt , Schnittspahnstrasse 13, 64287  Darmstadt , Germany

3. Institute of Molecular Biology , Ackermannweg 4, 55128  Mainz , Germany

Abstract

Abstract Cellular senescence, a major driver of aging, can be stimulated by DNA damage, and is counteracted by the DNA repair machinery. Here we show that in p16INK4a-deficient cells, senescence induction by the environmental genotoxin B[a]P or ionizing radiation (IR) completely depends on p21CIP1. Immunoprecipitation-based mass spectrometry interactomics data revealed that during senescence induction and maintenance, p21CIP1 specifically inhibits CDK4 and thereby activates the DREAM complex. Genome-wide transcriptomics revealed striking similarities in the response induced by B[a]P and IR. Among the top 100 repressed genes 78 were identical between B[a]P and IR and 76 were DREAM targets. The DREAM complex transcriptionally silences the main proliferation-associated transcription factors E2F1, FOXM1 and B-Myb as well as multiple DNA repair factors. Knockdown of p21CIP1, E2F4 or E2F5 diminished both, repression of these factors and senescence. The transcriptional profiles evoked by B[a]P and IR largely overlapped with the profile induced by pharmacological CDK4 inhibition, further illustrating the role of CDK4 inhibition in genotoxic stress-induced senescence. Moreover, data obtained by live-cell time-lapse microscopy suggest the inhibition of CDK4 by p21CIP1 is especially important for arresting cells which slip through mitosis. Overall, we identified the p21CIP1/CDK4/DREAM axis as a master regulator of genotoxic stress-induced senescence.

Funder

Deutsche Forschungsgemeinschaft

Publisher

Oxford University Press (OUP)

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