Isoform-selective Hsp90 inhibition rescues model of hereditary open-angle glaucoma.
Andrew R StothertAmirthaa SuntharalingamXiaolan TangVincent M CrowleySanket J MishraJack M WebsterBryce A NordhuesDustin J E HuardChristopher L PassagliaRaquel L LiebermanBrian S J BlaggLaura J BlairJohn Koren IiiChad A DickeyPublished in: Scientific reports (2017)
The heat shock protein 90 (Hsp90) family of molecular chaperones regulates protein homeostasis, folding, and degradation. The ER-resident Hsp90 isoform, glucose-regulated protein 94 (Grp94), promotes the aggregation of mutant forms of myocilin, a protein associated with primary open-angle glaucoma. While inhibition of Grp94 promotes the degradation of mutant myocilin in vitro, to date no Grp94-selective inhibitors have been investigated in vivo. Here, a Grp94-selective inhibitor facilitated mutant myocilin degradation and rescued phenotypes in a transgenic mouse model of hereditary primary open-angle glaucoma. Ocular toxicities previously associated with pan-Hsp90 inhibitors were not evident with our Grp94-selective inhibitor, 4-Br-BnIm. Our study suggests that selective inhibition of a distinct Hsp90 family member holds translational promise for ocular and other diseases associated with cell stress and protein misfolding.
Keyphrases
- heat shock protein
- heat shock
- endoplasmic reticulum stress
- heat stress
- mouse model
- protein protein
- cell surface
- amino acid
- transcription factor
- single cell
- binding protein
- small molecule
- blood pressure
- stem cells
- metabolic syndrome
- mesenchymal stem cells
- wild type
- machine learning
- mass spectrometry
- artificial intelligence
- blood glucose