Mitotic Stress Is an Integral Part of the Oncogene-Induced Senescence Program That Promotes Multinucleation and Cell Cycle Arrest

Overview

Journal Cell Rep

Publisher Cell Press

Specialties Biology
Cell Biology
Molecular Biology

Date 2015 Aug 25

PMID 26299965

Citations 39

Authors

Dina Dikovskaya

John J Cole

Susan M Mason

Colin Nixon

Saadia A Karim

Lynn McGarry

William Clark

Rachael N Hewitt

Morgan A Sammons

Jiajun Zhu

Dimitris Athineos

Joshua D G Leach

Francesco Marchesi

John van Tuyn

Stephen W Tait

Claire Brock

Jennifer P Morton

Hong Wu

Shelley L Berger

Karen Blyth

Peter D Adams

Affiliations

Soon will be listed here.

Abstract

Oncogene-induced senescence (OIS) is a tumor suppression mechanism that blocks cell proliferation in response to oncogenic signaling. OIS is frequently accompanied by multinucleation; however, the origin of this is unknown. Here, we show that multinucleate OIS cells originate mostly from failed mitosis. Prior to senescence, mutant H-RasV12 activation in primary human fibroblasts compromised mitosis, concordant with abnormal expression of mitotic genes functionally linked to the observed mitotic spindle and chromatin defects. Simultaneously, H-RasV12 activation enhanced survival of cells with damaged mitoses, culminating in extended mitotic arrest and aberrant exit from mitosis via mitotic slippage. ERK-dependent transcriptional upregulation of Mcl1 was, at least in part, responsible for enhanced survival and slippage of cells with mitotic defects. Importantly, mitotic slippage and oncogene signaling cooperatively induced senescence and key senescence effectors p21 and p16. In summary, activated Ras coordinately triggers mitotic disruption and enhanced cell survival to promote formation of multinucleate senescent cells.

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