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

Jasmine M Cross; Megan E Coulson; Joshua P Smalley; Wiktoria A Pytel; Ozair Ismail; Justin S Trory; Shaun M Cowley; James T Hodgkinson

doi:10.1039/d2md00199c

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

RSC Med Chem. 2022 Nov 1;13(12):1634-1639. doi: 10.1039/d2md00199c. eCollection 2022 Dec 14.

Authors

Jasmine M Cross¹, Megan E Coulson^{1

2}, Joshua P Smalley¹, Wiktoria A Pytel^{1

2}, Ozair Ismail¹, Justin S Trory¹, Shaun M Cowley², James T Hodgkinson¹

Affiliations

¹ Leicester Institute of Structural and Chemical Biology, School of Chemistry, University of Leicester Leicester LE1 7RH UK JTHodgkinson@le.ac.uk.
² Department of Molecular and Cell Biology, University of Leicester Leicester LE1 7RH UK 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.

Grants and funding

MR/J009202/1/MRC_/Medical Research Council/United Kingdom