A bidentate Polycomb Repressive-Deubiquitinase complex is required for efficient activity on nucleosomes

Foglizzo, M; Middleton, AJ; Burgess, AE; Crowther, JM; Dobson, RCJ; Murphy, JM; Day, CL; Mace, PD

Author(s): Foglizzo, M; Middleton, AJ; Burgess, AE; Crowther, JM; Dobson, RCJ; Murphy, JM; Day, CL; Mace, PD;
Details: Publication Year 2018-09-26,Volume 9,Issue #1,Page 3932
Journal Title: Nature Communications
Publication Type: Journal Article
Abstract: Attachment of ubiquitin to lysine 119 of Histone 2A (H2AK119Ub) is an epigenetic mark characteristic of repressed developmental genes, which is removed by the Polycomb Repressive-Deubiquitinase (PR-DUB) complex. Here we report the crystal structure of the Drosophila PR-DUB, revealing that the deubiquitinase Calypso and its activating partner ASX form a 2:2 complex. The bidentate Calypso-ASX complex is generated by dimerisation of two activated Calypso proteins through their coiled-coil regions. Disrupting the Calypso dimer interface does not affect inherent catalytic activity, but inhibits removal of H2AK119Ub as a consequence of impaired recruitment to nucleosomes. Mutating the equivalent surface on the human counterpart, BAP1, also compromises activity on nucleosomes. Together, this suggests that high local concentrations drive assembly of bidentate PR-DUB complexes on chromatin-providing a mechanistic basis for enhanced PR-DUB activity at specific genomic foci, and the impact of distinct classes of PR-DUB mutations in tumorigenesis.
Publisher: Springer Nature
Research Division(s): Cell Signalling And Cell Death
PubMed ID: 30258054
Publisher's Version: https://doi.org/10.1038/s41467-018-06186-1
Open Access at Publisher's Site: https://doi.org/10.1038/s41467-018-06186-1
NHMRC Grants: NHMRC/1105754,
Terms of Use/Rights Notice: Refer to copyright notice on published article.
Documents: Foglizzo M et al Nat Comm_2018.pdf - (3.40MB, application/pdf)

Creation Date: 2018-10-11 04:23:14

Last Modified: 2018-10-12 03:04:46