Breaking Bad Proteins—Discovery Approaches and the Road to Clinic for Degraders

Author:

Bouvier Corentin1ORCID,Lawrence Rachel2,Cavallo Francesca2,Xolalpa Wendy3ORCID,Jordan Allan2ORCID,Hjerpe Roland2,Rodriguez Manuel S.145

Affiliation:

1. Laboratoire de Chimie de Coordination LCC-UPR 8241-CNRS, 31077 Toulouse, France

2. Sygnature Discovery, Bio City, Pennyfoot St., Nottingham NG1 1GR, UK

3. Departamento de Ingeniería Celular y Biocatálisis, Instituto de Biotecnología, Universidad Nacional Autónoma de México, Cuernavaca 62209, Morelos, Mexico

4. Pharmadev, UMR 152, Université de Toulouse, IRD, UT3, 31400 Toulouse, France

5. B Molecular, Centre Pierre Potier, Canceropôle, 31106 Toulouse, France

Abstract

Proteolysis-targeting chimeras (PROTACs) describe compounds that bind to and induce degradation of a target by simultaneously binding to a ubiquitin ligase. More generally referred to as bifunctional degraders, PROTACs have led the way in the field of targeted protein degradation (TPD), with several compounds currently undergoing clinical testing. Alongside bifunctional degraders, single-moiety compounds, or molecular glue degraders (MGDs), are increasingly being considered as a viable approach for development of therapeutics, driven by advances in rational discovery approaches. This review focuses on drug discovery with respect to bifunctional and molecular glue degraders within the ubiquitin proteasome system, including analysis of mechanistic concepts and discovery approaches, with an overview of current clinical and pre-clinical degrader status in oncology, neurodegenerative and inflammatory disease.

Funder

COST

Telethon

JANUS

CONACyT-SRE

ARC foundation

La ligue contre le Cancer

Consejo Nacional de Ciencia y Tecnología

Publisher

MDPI AG

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