What question did this study set out to answer?

The aim is to develop high-affinity ligands for GID4 and understand their impact on its structure and function.

April 21, 2026

Cover Feature: Ligand‐Induced Conformational Plasticity of the CTLH E3 Ligase Receptor GID4 (ChemMedChem 7/2026)

Key Points

The aim is to develop high-affinity ligands for GID4 and understand their impact on its structure and function.
Utilized structure-based drug design to create ligands for GID4
Analyzed ligand-induced conformational states of GID4
Investigated clustering of ligand-GID4 complexes
Identified three distinct conformational states of GID4: closed, semi-open, and open
Demonstrated how ligand binding remaps the GID4 binding pocket
Highlighted the relationship between ligand structure and GID4 biological activity

Abstract

This study explores the development of high-affinity ligands for GID4 – the substrate receptor for the human CTLH E3 ligase. The cover image depicts the structural plasticity of GID4, highlighting three discrete conformational states—closed, semi-open, and open—induced by specific ligand binding. Through structure-based drug design, it was identified how these ligand-dependent shifts remodel the binding pocket. Analyzing how ligand-GID4 complexes cluster can clarify the links between chemical structure and biological activity, aiding the development of new ligands tailored for targeted protein degradation. More details can be found in the Research Article by Michal J. Walczak and co-workers (DOI: 10.1002/cmdc.202500849).

Bookmark

Cover Feature: Ligand‐Induced Conformational Plasticity of the CTLH E3 Ligase Receptor GID4 (ChemMedChem 7/2026)

Key Points

Abstract

Cite This Study