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USP11 mediates repair of DNA–protein cross-links by deubiquitinating SPRTN metalloprotease

Megan C. Perry, Meghan Biegert, Sai Sundeep Kollala, Halle J. Mallard, Grace Su, Manohar Kodavati, Natasha F. Kreiling, Alexander Holbrook, Gargi Ghosal

2021Journal of Biological Chemistry25 citationsDOIOpen Access PDF

Abstract

DNA-protein cross-links (DPCs) are toxic DNA lesions that interfere with DNA metabolic processes such as replication, transcription, and recombination. USP11 deubiquitinase participates in DNA repair, but the role of USP11 in DPC repair is not known. SPRTN is a replication-coupled DNA-dependent metalloprotease that cleaves proteins cross-linked to DNA to promote DPC repair. SPRTN function is tightly regulated by a monoubiquitin switch that controls SPRTN auto-proteolysis and chromatin accessibility during DPC repair. Previously, VCPIP1 and USP7 deubiquitinases have been shown to regulate SPRTN. Here, we identify USP11 as an SPRTN deubiquitinase. USP11 interacts with SPRTN and cleaves monoubiquitinated SPRTN in cells and in vitro. USP11 depletion impairs SPRTN deubiquitination and promotes SPRTN auto-proteolysis in response to formaldehyde-induced DPCs. Loss of USP11 causes an accumulation of unrepaired DPCs and cellular hypersensitivity to treatment with DPC-inducing agents. Our findings show that USP11 regulates SPRTN auto-proteolysis and SPRTN-mediated DPC repair to maintain genome stability.

Topics & Concepts

Deubiquitinating enzymeMetalloproteinaseDNAChemistryCell biologyUbiquitinMatrix metalloproteinaseBiologyBiochemistryGeneUbiquitin and proteasome pathwaysDNA Repair MechanismsCancer-related Molecular Pathways
USP11 mediates repair of DNA–protein cross-links by deubiquitinating SPRTN metalloprotease | Litcius