N‐Glycosylation‐Induced Pathologic Protein Conformations as a Tool to Guide the Selection of Biologically Active Small Molecules

Author:

Magni Andrea1,Sciva Cristiano12,Castelli Matteo1,Digwal Chander S.3,Rodina Anna3,Sharma Sahil3,Ochiana Stefan3,Patel Hardik J.3,Shah Smit3,Chiosis Gabriela34,Moroni Elisabetta2,Colombo Giorgio1ORCID

Affiliation:

1. Department of Chemistry University of Pavia 27100 Pavia Italy

2. Institute of Chemical Sciences and Technologies (SCITEC) Italian National Research Council (CNR) 20131 Milano Italy

3. Chemical Biology Program Memorial Sloan Kettering Cancer Center New York, NY 10065 USA

4. Department of Medicine Memorial Sloan Kettering Cancer Center New York, NY 10065 USA

Abstract

AbstractPost‐translational modifications such as protein N‐glycosylation, significantly influence cellular processes. Dysregulated N‐glycosylation, exemplified in Grp94, a member of the Hsp90 family, leads to structural changes and the formation of epichaperomes, contributing to pathologies. Targeting N‐glycosylation‐induced conformations offers opportunities for developing selective chemical tools and drugs for these pathologic forms of chaperones. We here demonstrate how a specific Grp94 conformation induced by N‐glycosylation, identified previously via molecular dynamics simulations, rationalizes the distinct behavior of similar ligands. Integrating dynamic ligand unbinding information with SAR development, we differentiate ligands productively engaging the pathologic Grp94 conformers from those that are not. Additionally, analyzing binding site stereoelectronic properties and QSAR models using cytotoxicity data unveils relationships between chemical, conformational properties, and biological activities. These findings facilitate the design of ligands targeting specific Grp94 conformations induced by abnormal glycosylation, selectively disrupting pathogenic protein networks while sparing normal mechanisms.

Publisher

Wiley

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