Cell Reports (May 2016)
USP1 Regulates Cellular Senescence by Controlling Genomic Integrity
Abstract
Summary: Oncogene-induced senescence (OIS) is a potent barrier for the transformation of pre-cancerous cells. The molecular pathways involved in the execution of OIS are still incompletely understood, but they include chronic DNA damage signaling and post-translational modifications of key factors. Here, we show that OIS-associated transcriptional downregulation of deubiquitinating enzyme USP1 triggers and maintains a DNA damage checkpoint response with atypical DNA lesions that is dependent on functional FANCD2-FI-ATR-CHK1-p53-CDKN1A signaling. We find that a reduced USP1 level causes aberrant aggregation of its target FANCD2 concomitant with replication stress, accumulation, and colocalization of γ-H2Ax and p53-binding protein 1 (53BP1) in large and unusual sparse DNA damage foci and an increased number of polyploid cells and cells arrested in G2/M, as well as a sensitization of senescence-bypassing cells to DNA interstrand crosslinking-mediated cell death. Our study identifies USP1 as a key senescence regulator controlling genomic integrity and a promising target for anti-cancer therapy. : Ogrunc et al. identify the deubiquitinating enzyme USP1 as an active contributor to oncogene-induced senescence. They show that USP1 controls replisome dynamics and genome stability and that USP1 dysfunction induces aberrant aggregation of mono-ubiquitinated FANCD2 concomitant with a chronic DNA damage response and senescence induction.