The deubiquitylase USP9X controls ribosomal stalling

Clancy, Anne; Heride, Claire; Pinto-Fernández, Adán; Kayser-Bricker, Katherine J.; Wang, Weiping; Smith, Victoria; Elcocks, Hannah; Davis, Simon; Fessler, Shawn P.; McKinnon, Crystal; Katz, Marie; Hammonds, Tim; Jones, Neil P.; O’Connell, Jonathan C.; Follows, Bruce; Mischke, Steven; Caravella, Justin A.; Ioannidis, Stephanos; Dinsmore, Christopher J.; Kim, Sunkyu; Behrens, Axel; Komander, David; Kessler, Benedikt M.; Urbé, Sylvie; Clague, Michael J.

doi:10.1101/2020.04.15.042291

Cited by 3 publications

(3 citation statements)

References 45 publications

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“…In this case, a panel of 22 DUBs were quantified (Turnbull et al, 2017). The ABPP assay was used also to assess cellular target engagement and DUB selectivity in crude cell extracts for small molecule inhibitors against USP9X (Clancy et al, 2020), and USP28 (Ruiz et al, 2020).…”

Section: Introductionmentioning

confidence: 99%

ABPP-HT - High-Throughput Activity-Based Profiling of Deubiquitylating Enzyme Inhibitors in a Cellular Context

et al. 2021

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The potency and selectivity of a small molecule inhibitor are key parameters to assess during the early stages of drug discovery. In particular, it is very informative for characterizing compounds in a relevant cellular context in order to reveal potential off-target effects and drug efficacy. Activity-based probes are valuable tools for that purpose, however, obtaining cellular target engagement data in a high-throughput format has been particularly challenging. Here, we describe a new methodology named ABPP-HT (high-throughput-compatible activity-based protein profiling), implementing a semi-automated proteomic sample preparation workflow that increases the throughput capabilities of the classical ABPP workflow approximately ten times while preserving its enzyme profiling characteristics. Using a panel of deubiquitylating enzyme (DUB) inhibitors, we demonstrate the feasibility of ABPP-HT to provide compound selectivity profiles of endogenous DUBs in a cellular context at a fraction of time as compared to previous methodologies.

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Section: Introductionmentioning

confidence: 99%

ABPP-HT - High-Throughput Activity-Based Profiling of Deubiquitylating Enzyme Inhibitors in a Cellular Context

et al. 2021

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“…Although the state of DUB inhibitor discovery is relatively young, with only one DUB inhibitor having entered clinical trials, a number of potent and selective DUB inhibitors have recently been described and characterized, which we reviewed (Schauer et al, 2020b). Some of the most promising inhibitors include several small-molecule inhibitors of USP7 (XL188, ALM5, FT671) (Di Gavory et al, 2018;Kategaya et al, 2017;Lamberto et al, 2017;O'Dowd et al, 2018;Reverdy et al, 2012;Turnbull et al, 2017), USP28/25 (AZ1) (Wrigley et al, 2017), and USP9X (FT709) (Clancy et al, 2020). Notably, over a decade ago, development began on inhibitors for the SARS-CoV papainlike protease (PLpro), a protease in the SARS genome that has DUB activity, and subsequently second-generation inhibitors have been described (Baez-Santos et al, 2014;Ghosh et al, 2009Ghosh et al, , 2010Ratia et al, 2008).…”

Section: Introductionmentioning

confidence: 99%

Small molecules as tools for functional assessment of deubiquitinating enzyme function

Magin

Liu

Felix

et al. 2021

Cell Chemical Biology

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“…The copyright holder for this preprint (which this version posted May 18, 2021. ; https://doi.org/10.1101/2021.05.17.444542 doi: bioRxiv preprint 4 directed mutagenesis experiments show USP5 processes Met1 and Lys48-linked polyUb chains sequentially from the proximal end of Ub chains 2,31 . The USP domain is highly conserved making it difficult to develop selective catalytic inhibitors; to date, out of 56 human USPs, selective inhibitors have been reported for USP1, USP7, USP9x, USP14 and USP30 [32][33][34][35][36][37][38] . The ZnF-UBD domain is present in a limited number of proteins in the human genome: USP3, USP5, USP13, USP16, USP20, USP22, USP33, USP39, USP44, USP45, USP49, USP51, HDAC6, a histone deacetylase protein, and BRAP, a BRCA1associated protein [39][40][41] .…”

Section: Introductionmentioning

confidence: 99%

Structure Activity Relationship of USP5 Allosteric Inhibitors

Mann

et al. 2021

Preprint

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USP5 is a deubiquitinase that has been implicated in a range of diseases, including cancer, but no USP5-targeting chemical probe has been reported to date. Here, we present the progression of a chemical series that occupies the C-terminal ubiquitin-binding site of a poorly characterized zinc-finger ubiquitin binding domain (ZnF-UBD) of USP5 and allosterically inhibits the catalytic activity of the enzyme. Systematic exploration of the structure-activity relationship, complemented with crystallographic characterization of the ZnF-UBD bound to multiple ligands, led to the identification of 64, which binds to the USP5 ZnF-UBD with a KD of 2.8 μM. 64 is selective over the structurally similar ZnF-UBD domain of HDAC6 and inhibits USP5 catalytic activity in vitro with an IC50 of 26 μM. This study provides a chemical and structural framework for the discovery of a chemical probe to delineate USP5 function in cells.

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The deubiquitylase USP9X controls ribosomal stalling

Cited by 3 publications

References 45 publications

ABPP-HT - High-Throughput Activity-Based Profiling of Deubiquitylating Enzyme Inhibitors in a Cellular Context

ABPP-HT - High-Throughput Activity-Based Profiling of Deubiquitylating Enzyme Inhibitors in a Cellular Context

Small molecules as tools for functional assessment of deubiquitinating enzyme function

Structure Activity Relationship of USP5 Allosteric Inhibitors

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