| Literature DB >> 29056420 |
Alexandra Pozhidaeva1, Gabrielle Valles1, Feng Wang2, Jian Wu2, David E Sterner2, Phuong Nguyen2, Joseph Weinstock2, K G Suresh Kumar2, Jean Kanyo3, Dennis Wright4, Irina Bezsonova5.
Abstract
USP7 is a deubiquitinating enzyme that plays a pivotal role in multiple oncogenic pathways and therefore is a desirable target for new anti-cancer therapies. However, the lack of structural information about the USP7-inhibitor interactions has been a critical gap in the development of potent inhibitors. USP7 is unique among USPs in that its active site is catalytically incompetent, and is postulated to rearrange into a productive conformation only upon binding to ubiquitin. Surprisingly, we found that ubiquitin alone does not induce an active conformation in solution. Using a combination of nuclear magnetic resonance, mass spectrometry, computational modeling, and cell-based assays, we found that DUB inhibitors P22077 and P50429 covalently modify the catalytic cysteine of USP7 and induce a conformational switch in the enzyme associated with active site rearrangement. This work represents the first experimental insights into USP7 activation and inhibition and provides a structural basis for rational development of potent anti-cancer therapeutics.Entities:
Keywords: DUB inhibition; DUBs; NMR; USP7; covalent inhibitors; cysteine peptidase; mass spectrometry; ubiquitin binding
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Year: 2017 PMID: 29056420 DOI: 10.1016/j.chembiol.2017.09.004
Source DB: PubMed Journal: Cell Chem Biol ISSN: 2451-9448 Impact factor: 8.116