Litcius/Paper detail

KDM5A and KDM5B histone-demethylases contribute to HU-induced replication stress response and tolerance

Solenne Gaillard, Virginie Charasson, Cyril Ribeyre, Kader Salifou, Marie‐Jeanne Pillaire, Jean‐Sébastien Hoffmann, Angelos Constantinou, Didier Trouche, Marie Vandromme

2021Biology Open24 citationsDOIOpen Access PDF

Abstract

KDM5A and KDM5B histone-demethylases are overexpressed in many cancers and have been involved in drug tolerance. Here, we describe that KDM5A, together with KDM5B, contribute to replication stress (RS) response and tolerance. First, they positively regulate RRM2, the regulatory subunit of ribonucleotide reductase. Second, they are required for optimal levels of activated Chk1, a major player of the intra-S phase checkpoint that protects cells from RS. We also found that KDM5A is enriched at ongoing replication forks and associates with both PCNA and Chk1. Because RRM2 is a major determinant of replication stress tolerance, we developed cells resistant to HU, and show that KDM5A/B proteins are required for both RRM2 overexpression and tolerance to HU. Altogether, our results indicate that KDM5A/B are major players of RS management. They also show that drugs targeting the enzymatic activity of KDM5 proteins may not affect all cancer-related consequences of KDM5A/B overexpression.

Topics & Concepts

BiologyRibonucleotide reductaseHistoneDNA replicationReplication (statistics)GeneticsCell biologyProtein subunitCancer researchGeneVirologyDNA Repair MechanismsEpigenetics and DNA MethylationGenomics and Chromatin Dynamics