Therapeutic targeting of Lyn kinase to treat chorea-acanthocytosis

Author:

Peikert Kevin,Federti Enrica,Matte Alessandro,Constantin Gabriela,Pietronigro Enrica Caterina,Fabene Paolo Francesco,Defilippi Paola,Turco Emilia,Del Gallo Federico,Pucci Pietro,Amoresano Angela,Illiano Anna,Cozzolino Flora,Monti Maria,Garello Francesca,Terreno Enzo,Alper Seth Leo,Glaß Hannes,Pelzl Lisann,Akgün Katja,Ziemssen Tjalf,Ordemann Rainer,Lang Florian,Brunati Anna Maria,Tibaldi Elena,Andolfo Immacolata,Iolascon Achille,Bertini Giuseppe,Buffelli Mario,Zancanaro Carlo,Lorenzetto Erika,Siciliano Angela,Bonifacio Massimiliano,Danek Adrian,Walker Ruth Helen,Hermann Andreas,De Franceschi LuciaORCID

Abstract

AbstractChorea-Acanthocytosis (ChAc) is a devastating, little understood, and currently untreatable neurodegenerative disease caused by VPS13A mutations. Based on our recent demonstration that accumulation of activated Lyn tyrosine kinase is a key pathophysiological event in human ChAc cells, we took advantage of Vps13a−/− mice, which phenocopied human ChAc. Using proteomic approach, we found accumulation of active Lyn, γ-synuclein and phospho-tau proteins in Vps13a−/− basal ganglia secondary to impaired autophagy leading to neuroinflammation. Mice double knockout Vps13a−/− Lyn−/− showed normalization of red cell morphology and improvement of autophagy in basal ganglia. We then in vivo tested pharmacologic inhibitors of Lyn: dasatinib and nilotinib. Dasatinib failed to cross the mouse brain blood barrier (BBB), but the more specific Lyn kinase inhibitor nilotinib, crosses the BBB. Nilotinib ameliorates both Vps13a−/− hematological and neurological phenotypes, improving autophagy and preventing neuroinflammation. Our data support the proposal to repurpose nilotinib as new therapeutic option for ChAc patients.

Funder

NA advocay

Zentrum für Regenerative Therapien Dresden

Else Kröner-Fresenius-Stiftung

Universität Rostock

Kurt-Eberhard-Bode-Stiftung für Medizinische und Naturwissenschaftliche Forschung

European Research Council

Publisher

Springer Science and Business Media LLC

Subject

Cellular and Molecular Neuroscience,Clinical Neurology,Pathology and Forensic Medicine

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