A Degron Blocking Strategy Towards Improved CRL4<sup>CRBN</sup> Recruiting PROTAC Selectivity**-Reference-Cited by-同舟云学术

A Degron Blocking Strategy Towards Improved CRL4^CRBN Recruiting PROTAC Selectivity**

Published:2023-10-10 Issue:23 Volume:24 Page:
ISSN:1439-4227
Container-title:ChemBioChem
language:en
Short-container-title:ChemBioChem

Author:

Bouguenina Habib¹^ORCID,Scarpino Andrea¹,O'Hanlon Jack A.¹,Warne Justin¹,Wang Hannah Z.¹,Wah Hak Laura Chan¹,Sadok Amine¹²,McAndrew P. Craig¹,Stubbs Mark¹,Pierrat Olivier A.¹,Hahner Tamas¹,Cabry Marc P.¹,Le Bihan Yann‐Vaï¹,Mitsopoulos Costas¹,Sialana Fernando J.¹³,Roumeliotis Theodoros I.¹³,Burke Rosemary¹,van Montfort Rob L. M.¹,Choudhari Jyoti³,Chopra Rajesh¹⁴,Caldwell John J.¹,Collins Ian¹

Affiliation:

1. Centre for Cancer Drug Discovery Institute of Cancer Research 15 Cotswold Road, Sutton London SM2 5NG UK

2. Monte Rosa Therapeutics AG Aeschenvorstadt 36 4051 Basel Switzerland

3. Functional Proteomics Group The Institute of Cancer Research Chester Beatty Laboratories London SW3 6JB UK

4. Apple Tree Partners The Gridiron Building, Suite 6.05, 1 St Pancras Square London N1 C 4AG UK

Abstract

AbstractSmall molecules inducing protein degradation are important pharmacological tools to interrogate complex biology and are rapidly translating into clinical agents. However, to fully realise the potential of these molecules, selectivity remains a limiting challenge. Herein, we addressed the issue of selectivity in the design of CRL4CRBN recruiting PROteolysis TArgeting Chimeras (PROTACs). Thalidomide derivatives used to generate CRL4CRBN recruiting PROTACs have well described intrinsic monovalent degradation profiles by inducing the recruitment of neo‐substrates, such as GSPT1, Ikaros and Aiolos. We leveraged structural insights from known CRL4CRBN neo‐substrates to attenuate and indeed remove this monovalent degradation function in well‐known CRL4CRBN molecular glues degraders, namely CC‐885 and Pomalidomide. We then applied these design principles on a previously published BRD9 PROTAC (dBRD9‐A) and generated an analogue with improved selectivity profile. Finally, we implemented a computational modelling pipeline to show that our degron blocking design does not impact PROTAC‐induced ternary complex formation. We believe that the tools and principles presented in this work will be valuable to support the development of targeted protein degradation.

Funder

Cancer Research UK

Publisher

Wiley

Subject

Organic Chemistry,Molecular Biology,Molecular Medicine,Biochemistry

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