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

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

doi:10.1039/d3md00633f

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

RSC Med Chem. 2024 Mar 5;15(3):1066-1071. doi: 10.1039/d3md00633f. eCollection 2024 Mar 20.

Authors

Aliakbar Khalili Yazdi¹, Sumera Perveen¹, Cheng Dong¹, Xiaosheng Song¹, Aiping Dong¹, Magdalena M Szewczyk¹, Matthew F Calabrese², Agustin Casimiro-Garcia³, Subramanyam Chakrapani², Matthew S Dowling², Emel Ficici², Jisun Lee², Justin I Montgomery², Thomas N O'Connell², Grzegorz J Skrzypek², Tuan P Tran², Matthew D Troutman², Feng Wang², Jennifer A Young², Jinrong Min¹, Dalia Barsyte-Lovejoy^{1

4}, Peter J Brown¹, Vijayaratnam Santhakumar¹, Cheryl H Arrowsmith^{1

4

5}, Masoud Vedadi^{1

4}, Dafydd R Owen³

Affiliations

¹ Structural Genomics Consortium, University of Toronto Toronto ON Canada.
² Pfizer Research & Development Groton CT USA.
³ Pfizer Research & Development Cambridge MA USA dafydd.owen@pfizer.com.
⁴ Department of Pharmacology and Toxicology, University of Toronto Toronto ON Canada.
⁵ Princess Margaret Cancer Centre and Department of Medical Biophysics, University of Toronto Toronto ON Canada.

PMID: 38516600
PMCID: PMC10953471 (available on 2025-03-05)
DOI: 10.1039/d3md00633f

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.