Management of Hsp90-Dependent Protein Folding by Small Molecules Targeting the Aha1 Co-Chaperone

Overview

Journal Cell Chem Biol

Publisher Cell Press

Specialty Biochemistry

Date 2020 Feb 5

PMID 32017918

Citations 12

Authors

Jay K Singh

Darren M Hutt

Bradley Tait

Naihsuan C Guy

Jeffrey C Sivils

Nina R Ortiz

Ashley N Payan

Shravan Kumar Komaragiri

Jazzmin Jovonna Owens

David Culbertson

Laura J Blair

Chad Dickey

Szu Yu Kuo

Dan Finley

H Jane Dyson

Marc B Cox

Jaideep Chaudhary

Jason E Gestwicki

William E Balch

Affiliations

Soon will be listed here.

Abstract

Hsp90 plays an important role in health and is a therapeutic target for managing misfolding disease. Compounds that disrupt co-chaperone delivery of clients to Hsp90 target a subset of Hsp90 activities, thereby minimizing the toxicity of pan-Hsp90 inhibitors. Here, we have identified SEW04784 as a first-in-class inhibitor of the Aha1-stimulated Hsp90 ATPase activity without inhibiting basal Hsp90 ATPase. Nuclear magnetic resonance analysis reveals that SEW84 binds to the C-terminal domain of Aha1 to weaken its asymmetric binding to Hsp90. Consistent with this observation, SEW84 blocks Aha1-dependent Hsp90 chaperoning activities, including the in vitro and in vivo refolding of firefly luciferase, and the transcriptional activity of the androgen receptor in cell-based models of prostate cancer and promotes the clearance of phosphorylated tau in cellular and tissue models of neurodegenerative tauopathy. We propose that SEW84 provides a novel lead scaffold for developing therapeutic approaches to treat proteostatic disease.

Citing Articles

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