BRCA1/BARD1 intrinsically disordered regions facilitate chromatin recruitment and ubiquitylation

Author:

Witus Samuel R.,Tuttle Lisa M.ORCID,Li Wenjing,Zelter AlexORCID,Wang Meiling,Kermoade Klaiten E.,Wilburn Damien B.ORCID,Davis Trisha N.ORCID,Brzovic Peter S.,Zhao WeixingORCID,Klevit Rachel E.ORCID

Abstract

AbstractBRCA1/BARD1 is a tumor suppressor E3 ubiquitin (Ub) ligase with roles in DNA damage repair and in transcriptional regulation. BRCA1/BARD1 RING domains interact with nucleosomes to facilitate mono-ubiquitylation of distinct residues on the C-terminal tail of histone H2A. These enzymatic domains constitute a small fraction of the heterodimer, raising the possibility of functional chromatin interactions involving other regions such as the BARD1 C-terminal domains that bind nucleosomes containing the DNA damage signal H2A K15-Ub and H4 K20me0, or portions of the expansive intrinsically disordered regions found in both subunits. Herein, we reveal novel interactions that support robust H2A ubiquitylation activity mediated through a high-affinity, intrinsically disordered DNA-binding region of BARD1. These interactions support BRCA1/BARD1 recruitment to chromatin and sites of DNA damage in cells and contribute to their survival. We also reveal distinct BRCA1/BARD1 complexes that depend on the presence of H2A K15-Ub, including a complex where a single BARD1 subunit spans adjacent nucleosome units. Our findings identify an extensive network of multivalent BARD1- nucleosome interactions that serve as a platform for BRCA1/BARD1-associated functions on chromatin.

Publisher

Cold Spring Harbor Laboratory

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