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Synthesis and Validation of the First Cell-Impermeable Hsp90α-Selective Inhibitors

Tyelor S. Reynolds, Brian S. J. Blagg

2023ACS Medicinal Chemistry Letters10 citationsDOIOpen Access PDF

Abstract

Hsp90α is an isoform of the heat shock protein 90 (Hsp90) family of molecular chaperones and mediates the folding and activation of ∼400 client proteins. However, inhibition of intracellular Hsp90α has caused detrimental side effects and significantly hindered the clinical development of Hsp90 inhibitors. As an alternative strategy, 14 Hsp90α-selective inhibitors were synthesized to introduce permanently charged moieties onto the solvent-exposed portion of the Hsp90α binding site to produce cell-impermeable extracellular Hsp90α-selective inhibitors. The resulting lead compounds were cell-permeable dimethylamine 14 ( NDNA3 ), with an affinity of 0.51 μM for Hsp90α and >196-fold selectivity over the other Hsp90 isoforms, and cell-impermeable quaternary ammonium 17 ( NDNA4 ), with an affinity of 0.34 μM for Hsp90α and >294-fold selectivity. The permanently charged analogs were determined to have low membrane permeability, to be nontoxic against Ovcar-8 and MCF-10A cells, to avoid disruption of hERG channel maturation, and not to induce the heat shock response or Hsp90α-dependent client degradation.

Topics & Concepts

Hsp90Heat shock proteinIntracellularExtracellularChemistryBiophysicsMembraneCell membraneCellBiochemistrySelectivityHsp90 inhibitorHsp70Cell biologyBiologyGeneCatalysisHeat shock proteins researchComputational Drug Discovery Methods
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