Issue 3, 2024
From the journal:

RSC Medicinal Chemistry

Chemical tools for the Gid4 subunit of the human E3 ligase C-terminal to LisH (CTLH) degradation complex

Aliakbar Khalili Yazdi,a   Sumera Perveen, ORCID logo a   Cheng Dong, ORCID logo a   Xiaosheng Song, ORCID logo a   Aiping Dong, ORCID logo a   Magdalena M. Szewczyk, ORCID logo a   Matthew F. Calabrese, ORCID logo b   Agustin Casimiro-Garcia, ORCID logo c   Subramanyam Chakrapani,b   Matthew S. Dowling, ORCID logo b   Emel Ficici, ORCID logo b   Jisun Lee, ORCID logo b   Justin I. Montgomery,b   Thomas N. O'Connell,b   Grzegorz J. Skrzypek, ORCID logo b   Tuan P. Tran, ORCID logo b   Matthew D. Troutman,b   Feng Wang,b   Jennifer A. Young,b   Jinrong Min,a   Dalia Barsyte-Lovejoy, ORCID logo ad   Peter J. Brown, ORCID logo a   Vijayaratnam Santhakumar, ORCID logo a   Cheryl H. Arrowsmith, ORCID logo ade   Masoud Vedadi ORCID logo ad  and  Dafydd R. Owen ORCID logo *c  

* Corresponding authors

a Structural Genomics Consortium, University of Toronto, Toronto, ON, Canada

b Pfizer Research & Development, Groton, CT, USA

c Pfizer Research & Development, Cambridge, MA, USA
E-mail: dafydd.owen@pfizer.com

d Department of Pharmacology and Toxicology, University of Toronto, Toronto, ON, Canada

e Princess Margaret Cancer Centre and Department of Medical Biophysics, University of Toronto, Toronto, ON, Canada

Abstract

We have developed a novel chemical handle (PFI-E3H1) and a chemical probe (PFI-7) as ligands for the Gid4 subunit of the human E3 ligase CTLH degradation complex. Through an efficient initial hit-ID campaign, structure-based drug design (SBDD) and leveraging the sizeable Pfizer compound library, we identified a 500 nM ligand for this E3 ligase through file screening alone. Further exploration identified a vector that is tolerant to addition of a linker for future chimeric molecule design. The chemotype was subsequently optimized to sub-100 nM Gid4 binding affinity for a chemical probe. These novel tools, alongside the suitable negative control also identified, should enable the interrogation of this complex human E3 ligase macromolecular assembly.

Graphical abstract: Chemical tools for the Gid4 subunit of the human E3 ligase C-terminal to LisH (CTLH) degradation complex

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Article information

DOI
https://doi.org/10.1039/D3MD00633F
Article type
Research Article
Submitted
13 Nov 2023
Accepted
14 Jan 2024
First published
05 Mar 2024

RSC Med. Chem., 2024,15, 1066-1071

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Chemical tools for the Gid4 subunit of the human E3 ligase C-terminal to LisH (CTLH) degradation complex

A. K. Yazdi, S. Perveen, C. Dong, X. Song, A. Dong, M. M. Szewczyk, M. F. Calabrese, A. Casimiro-Garcia, S. Chakrapani, M. S. Dowling, E. Ficici, J. Lee, J. I. Montgomery, T. N. O'Connell, G. J. Skrzypek, T. P. Tran, M. D. Troutman, F. Wang, J. A. Young, J. Min, D. Barsyte-Lovejoy, P. J. Brown, V. Santhakumar, C. H. Arrowsmith, M. Vedadi and D. R. Owen, RSC Med. Chem., 2024, 15, 1066 DOI: 10.1039/D3MD00633F

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