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Phosphatidylserine clustering by the Ebola virus matrix protein is a critical step in viral budding

Monica L. Husby, Souad Amiar, Laura I. Prugar, Emily A. David, Caroline B. Plescia, Kathleen E. Huie, Jennifer M. Brannan, John M. Dye, Elsje Pienaar, Robert V. Stahelin

2022EMBO Reports35 citationsDOIOpen Access PDF

Abstract

Phosphatidylserine (PS) is a critical lipid factor in the assembly and spread of numerous lipid-enveloped viruses. Here, we describe the ability of the Ebola virus (EBOV) matrix protein eVP40 to induce clustering of PS and promote viral budding in vitro, as well as the ability of an FDA-approved drug, fendiline, to reduce PS clustering and subsequent virus budding and entry. To gain mechanistic insight into fendiline inhibition of EBOV replication, multiple in vitro assays were run including imaging, viral budding and viral entry assays. Fendiline lowers PS content in mammalian cells and PS in the plasma membrane, where the ability of VP40 to form new virus particles is greatly lower. Further, particles that form from fendiline-treated cells have altered particle morphology and cannot significantly infect/enter cells. These complementary studies reveal the mechanism by which EBOV matrix protein clusters PS to enhance viral assembly, budding, and spread from the host cell while also laying the groundwork for fundamental drug targeting strategies.

Topics & Concepts

Viral matrix proteinEbola virusBuddingVirologyBiologyVP40VirusComputational biologyCell biologyViral Infections and Outbreaks ResearchMosquito-borne diseases and controlSARS-CoV-2 and COVID-19 Research
Phosphatidylserine clustering by the Ebola virus matrix protein is a critical step in viral budding | Litcius