| Literature DB >> 26388029 |
Jianping Yin1, Allyn J Schoeffler2, Katherine Wickliffe3, Kim Newton3, Melissa A Starovasnik1, Erin C Dueber4, Seth F Harris5.
Abstract
Protein ubiquitination patterns are an important component of cellular signaling. The WD-repeat protein WDR48 (USP1-associated factor UAF-1) stimulates activity of ubiquitin-specific proteases USP1, USP12, and USP46. To understand how WDR48 exerts its effect on the USP scaffold, we determined structures of the ternary WDR48:USP46:ubiquitin complex. WDR48 interacts with the USP46 fingers subdomain via a relatively small, highly polar surface on the top center of the WDR48 β propeller. In addition, WDR48 has a novel ancillary domain and a C-terminal SUMO-like domain encircling the USP46-bound ubiquitin. Mutation of residues involved in the WDR48:USP46 interaction abrogated both binding and deubiquitinase activity of the complex. An analogous mutation in USP1 similarly blocked WDR48-dependent activation. Our data suggest a possible mechanism of deubiquitinase stimulation via stabilization and prolonged residence time of substrate. The unprecedented mode of interaction between the USP fingers domain and the WD-repeat β propeller serves as a prototypical example for this family of deubiquitinases.Entities:
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Year: 2015 PMID: 26388029 DOI: 10.1016/j.str.2015.08.010
Source DB: PubMed Journal: Structure ISSN: 0969-2126 Impact factor: 5.006