posted on 2019-11-11, 22:44authored byMandeep K. Mann, Ivan Franzoni, Renato Ferreira de Freitas, Wolfram Tempel, Scott Houliston, Leanna Smith, Masoud Vedadi, Cheryl H. Arrowsmith, Rachel J. Harding, Matthieu Schapira
USP5 disassembles unanchored polyubiquitin
chains to recycle free monoubiquitin, and is one of the 12 ubiquitin
specific proteases featuring a zinc finger ubiquitin-binding domain
(ZnF-UBD). This distinct structural module has been associated with
substrate positioning or allosteric modulation of catalytic activity,
but its cellular function remains unclear. We screened a chemical
library focused on the ZnF-UBD of USP5, crystallized hits in complex
with the protein, and generated a preliminary structure–activity
relationship, which enables the development of more potent and selective
compounds. This work serves as a framework for the discovery of a
chemical probe to delineate the function of USP5 ZnF-UBD in proteasomal
degradation and other ubiquitin signaling pathways in health and disease.