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Targeting retinoic acid receptor alpha-corepressor interaction activates chaperone-mediated autophagy and protects against retinal degeneration

Nature Communications. 2019-09; 
Raquel Gomez-Sintes; Qisheng Xin; Juan Ignacio Jimenez-Loygorri; Mericka McCabe; Antonio Diaz; Thomas P. Garner; Xiomaris M. Cotto-Rios; Yang Wu; Shuxian Dong; Cara A. Reynolds; Bindi Patel; Pedro de la Villa; Fernando Macian; Patricia Boya; Evripidis Gavathiotis; Ana Maria Cuervo
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Peptide Synthesis at 4 C. Fluorescence polarization binding assays The fluorescein-tagged peptide of N-CoR1, FITC-Ahx-RLITLADHICQIITQDFAR (FITC-N-CoR1) was provided by Genscript at purity > 95%. Fluorescence polarization assays (FPA) were performed using established procedures 36 . Direct binding isotherms were generated by incubating Get A Quote

摘要

Chaperone-mediated autophagy activity, essential in the cellular defense against proteotoxicity, declines with age, and preventing this decline in experimental genetic models has proven beneficial. Here, we have identified the mechanism of action of selective chaperone-mediated autophagy activators previously developed by our group and have leveraged that information to generate orally bioavailable chaperone-mediated autophagy activators with favorable brain exposure. Chaperone-mediated autophagy activating molecules stabilize the interaction between retinoic acid receptor alpha - a known endogenous inhibitor of chaperone-mediated autophagy - and its co-repressor, nuclear receptor corepressor 1, resulting in ch... More

关键词

Chaperone-mediated autophagy, Mechanism of action, Retinal diseases