Issue 12, 2022
From the journal:

RSC Medicinal Chemistry

A ‘click’ chemistry approach to novel entinostat (MS-275) based class I histone deacetylase proteolysis targeting chimeras

Jasmine M. Cross,a   Megan E. Coulson, ORCID logo ab   Joshua P. Smalley,a   Wiktoria A. Pytel,ab   Ozair Ismail,a   Justin S. Trory, ORCID logo a   Shaun M. Cowley*b  and  James T. Hodgkinson ORCID logo *a  

* Corresponding authors

a Leicester Institute of Structural and Chemical Biology, School of Chemistry, University of Leicester, Leicester, UK
E-mail: JTHodgkinson@le.ac.uk

b Department of Molecular and Cell Biology, University of Leicester, Leicester, UK
E-mail: smc57@leicester.ac.uk

Abstract

Click chemistry was utilised to prepare a library of PROTACs based on entinostat a class I histone deacetylase (HDAC) inhibitor in clinical trials. A novel PROTAC JMC-137 was identified as a HDAC1/2 and HDAC3 degrader in HCT116 cells. However, potency was compromised compared to previously identified class I HDAC PROTACs highlighting the importance in the choice of HDAC ligand, functional group for linker attachment and positioning in PROTAC design.

Graphical abstract: A ‘click’ chemistry approach to novel entinostat (MS-275) based class I histone deacetylase proteolysis targeting chimeras

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Article information

DOI
https://doi.org/10.1039/D2MD00199C
Article type
Research Article
Submitted
28 Jun 2022
Accepted
05 Oct 2022
First published
01 Nov 2022
This article is Open Access
Creative Commons BY license

RSC Med. Chem., 2022,13, 1634-1639

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A ‘click’ chemistry approach to novel entinostat (MS-275) based class I histone deacetylase proteolysis targeting chimeras

J. M. Cross, M. E. Coulson, J. P. Smalley, W. A. Pytel, O. Ismail, J. S. Trory, S. M. Cowley and J. T. Hodgkinson, RSC Med. Chem., 2022, 13, 1634 DOI: 10.1039/D2MD00199C

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