Methotrimeprazine is a neuroprotective antiviral in JEV infection via adaptive ER stress and autophagy

Author:

Prajapat Surendra K,Mishra Laxmi,Khera Sakshi,Owusu Shadrack D,Ahuja Kriti,Sharma Puja,Choudhary Eira,Chhabra Simran,Kumar Niraj,Singh RajanORCID,Kaushal Prem SORCID,Mahajan DineshORCID,Banerjee Arup,Motiani Rajender KORCID,Vrati Sudhanshu,Kalia ManjulaORCID

Abstract

AbstractJapanese encephalitis virus (JEV) pathogenesis is driven by a combination of neuronal death and neuroinflammation. We tested 42 FDA-approved drugs that were shown to induce autophagy for antiviral effects. Four drugs were tested in the JE mouse model based on in vitro protective effects on neuronal cell death, inhibition of viral replication, and anti-inflammatory effects. The antipsychotic phenothiazines Methotrimeprazine (MTP) & Trifluoperazine showed a significant survival benefit with reduced virus titers in the brain, prevention of BBB breach, and inhibition of neuroinflammation. Both drugs were potent mTOR-independent autophagy flux inducers. MTP inhibited SERCA channel functioning, and induced an adaptive ER stress response in diverse cell types. Pharmacological rescue of ER stress blocked autophagy and antiviral effect. MTP did not alter translation of viral RNA, but exerted autophagy-dependent antiviral effect by inhibiting JEV replication complexes. Drug-induced autophagy resulted in reduced NLRP3 protein levels, and attenuation of inflammatory cytokine/chemokine release from infected microglial cells. Our study suggests that MTP exerts a combined antiviral and anti-inflammatory effect in JEV infection, and has therapeutic potential for JE treatment.

Funder

Department of Biotechnology, Ministry of Science and Technology, India

The Wellcome Trust DBT India Alliance

DST | Science and Engineering Research Board

Publisher

Springer Science and Business Media LLC

Subject

Molecular Medicine

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