Structural basis of the histone ubiquitination read–write mechanism of RYBP–PRC1
Maria Ciapponi, Elena Karlukova, Sven Schkölziger, Christian Benda, Jürg Müller
Abstract
Histone H2A monoubiquitination (H2Aub1) by the PRC1 subunit RING1B entails a positive feedback loop, mediated by the RING1B-interacting protein RYBP. We uncover that human RYBP-PRC1 binds unmodified nucleosomes via RING1B but H2Aub1-modified nucleosomes via RYBP. RYBP interactions with both ubiquitin and the nucleosome acidic patch create the high binding affinity that favors RYBP- over RING1B-directed PRC1 binding to H2Aub1-modified nucleosomes; this enables RING1B to monoubiquitinate H2A in neighboring unmodified nucleosomes.
Topics & Concepts
NucleosomeHistoneUbiquitinCell biologyHistone H2AChemistryProtein subunitBiochemistryBiologyDNAGeneUbiquitin and proteasome pathwaysRNA modifications and cancerinterferon and immune responses