In silico screening and preclinical validation identify bavisant as a therapeutic candidate for multiple sclerosis

再髓鞘化 神经保护 生物信息学 多发性硬化 医学 神经科学 体内 药理学 髓鞘 临床试验 药物发现 生物信息学 特瑞氟米特 生物 芬戈莫德 计算生物学 系统药理学 药物重新定位 再生(生物学) 体外毒理学 格拉默
作者
Nadjet Gacem,Svetlana Bezukladova,Farina Windener,Tala Karam,Linda K Ottoboni,Elena Brambilla,Francesca Ruffini,Karthik Soman,Beatriz García-Díaz,M. Lévy,Qiao-Ling Cui,Alessia Formato,Cyrille Deboux,Jérémy Chazot,Radmila Panic,Stefanie Albrecht,Elif Nur Yılmaz,Raquel Guerrero González,Ivano Eberini,Stefania Olla
出处
期刊:Science Translational Medicine [American Association for the Advancement of Science]
卷期号:18 (833): eads0633-eads0633 被引量:3
标识
DOI:10.1126/scitranslmed.ads0633
摘要

Current treatments for multiple sclerosis (MS) are insufficient to delay the neurodegenerative process that is the main cause of disability progression in patients with MS. Therapeutics aimed at supporting myelin regeneration and neuroprotection are thus a major unmet medical need for the progressive forms of MS. To address this, we developed a strategy combining in silico screening of more than 1500 repurposed compounds with a validation pipeline of models, encompassing rodent and human in vitro assays as well as mouse models of demyelination/remyelination. From the initial library, 273 drugs were prioritized in silico on the basis of the predicted effects on myelination and neuroprotection, and among them, 160 were potentially nontoxic. We identified 32 molecules that exerted a promyelinating and a neuroprotective action on rodent and human oligodendroglia and neurons. Our data identified classes of compounds with potentially distinct mechanisms of action that may foster remyelination and neuroprotection. The therapeutic activity of one selected drug, the histamine receptor H3 antagonist bavisant, was further validated in mouse models of demyelination and axonal injury reproducing some key pathological features occurring in MS. Our in vivo studies demonstrated that bavisant promoted remyelination and neuroprotection when administered to LPC-treated, cuprizone-fed, or MOG-induced EAE mice, as well as in a human oligodendroglia chimeric mouse model of demyelination/remyelination. These findings provide proof-of-concept validation for bavisant as a candidate for neuroprotective clinical trials in MS.
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