AUTHOR=Hoch Lucile , Bourg Nathalie , Degrugillier Fanny , Bruge Céline , Benabides Manon , Pellier Emilie , Tournois Johana , Mahé Gurvan , Maignan Nicolas , Dawe Jack , Georges Maxime , Papazian David , Subramanian Nik , Simon Stéphanie , Fanen Pascale , Delevoye Cédric , Richard Isabelle , Nissan Xavier 

TITLE=Dual Blockade of Misfolded Alpha-Sarcoglycan Degradation by Bortezomib and Givinostat Combination

JOURNAL=Frontiers in Pharmacology

VOLUME=13

YEAR=2022

URL=https://www.frontiersin.org/journals/pharmacology/articles/10.3389/fphar.2022.856804

DOI=10.3389/fphar.2022.856804

ISSN=1663-9812

ABSTRACT=<p>Limb-girdle muscular dystrophy type R3 (LGMD R3) is a rare genetic disorder characterized by a progressive proximal muscle weakness and caused by mutations in the <italic>SGCA</italic> gene encoding alpha-sarcoglycan (α-SG). Here, we report the results of a mechanistic screening ascertaining the molecular mechanisms involved in the degradation of the most prevalent misfolded R77C-α-SG protein. We performed a combinatorial study to identify drugs potentializing the effect of a low dose of the proteasome inhibitor bortezomib on the R77C-α-SG degradation inhibition. Analysis of the screening associated to artificial intelligence-based predictive ADMET characterization of the hits led to identification of the HDAC inhibitor givinostat as potential therapeutical candidate. Functional characterization revealed that givinostat effect was related to autophagic pathway inhibition, unveiling new theories concerning degradation pathways of misfolded SG proteins. Beyond the identification of a new therapeutic option for LGMD R3 patients, our results shed light on the potential repurposing of givinostat for the treatment of other genetic diseases sharing similar protein degradation defects such as LGMD R5 and cystic fibrosis.</p>