Molecular Glues That Inhibit Deubiquitylase Activity and Inflammatory Signalling

Overview

Journal bioRxiv

Date 2024 Sep 16

PMID 39282282

Authors

Francesca Chandler

Poli Adi Narayana Reddy

Smita Bhutda

Rebecca L Ross

Arindam Datta

Miriam Walden

Kieran Walker

Stefano Di Donato

Joel A Cassel

Michael A Prakesch

Ahmed Aman

Alessandro Datti

Lisa J Campbell

Martina Foglizzo

Lillie Bell

Daniel N Stein

James R Ault

Rima S Al-Awar

Antonio N Calabrese

Frank Sicheri

Francesco Del Galdo

Joseph M Salvino

Roger A Greenberg

Elton Zeqiraj

Affiliations

Soon will be listed here.

Abstract

Deubiquitylases (DUBs) are crucial in cell signalling and are often regulated by interactions within protein complexes. The BRCC36 isopeptidase complex (BRISC) regulates inflammatory signalling by cleaving K63-linked polyubiquitin chains on Type I interferon receptors (IFNAR1). As a Zn-dependent JAMM/MPN DUB, BRCC36 is challenging to target with selective inhibitors. We discovered first-in-class inhibitors, termed BRISC molecular glues (BLUEs), which stabilise a 16-subunit BRISC dimer in an autoinhibited conformation, blocking active sites and interactions with the targeting subunit SHMT2. This unique mode of action results in selective inhibition of BRISC over related complexes with the same catalytic subunit, splice variants and other JAMM/MPN DUBs. BLUE treatment reduced interferon-stimulated gene expression in cells containing wild type BRISC, and this effect was absent when using structure-guided, inhibitor-resistant BRISC mutants. Additionally, BLUEs increase IFNAR1 ubiquitylation and decrease IFNAR1 surface levels, offering a potential new strategy to mitigate Type I interferon-mediated diseases. Our approach also provides a template for designing selective inhibitors of large protein complexes by promoting, rather than blocking, protein-protein interactions.

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