Zika virus prM protein contains cholesterol binding motifs required for virus entry and assembly

Author:

Goellner SarahORCID,Enkavi GirayORCID,Prasad VibhuORCID,Denolly Solène,Eu Sungmin,Mizzon GiuliaORCID,Witte LeanderORCID,Kulig WaldemarORCID,Uckeley Zina M.,Lavacca Teresa M.ORCID,Haselmann Uta,Lozach Pierre-Yves,Brügger BrittaORCID,Vattulainen IlpoORCID,Bartenschlager RalfORCID

Abstract

AbstractFor successful infection of host cells and virion production, enveloped viruses, including Zika virus (ZIKV), extensively rely on cellular lipids. However, how virus protein–lipid interactions contribute to the viral life cycle remains unclear. Here, we employ a chemo-proteomics approach with a bifunctional cholesterol probe and show that cholesterol is closely associated with the ZIKV structural protein prM. Bioinformatic analyses, reverse genetics alongside with photoaffinity labeling assays, and atomistic molecular dynamics simulations identified two functional cholesterol binding motifs within the prM transmembrane domain. Loss of prM–cholesterol association has a bipartite effect reducing ZIKV entry and leading to assembly defects. We propose a model in which membrane-resident M facilitates cholesterol-supported lipid exchange during endosomal entry and, together with cholesterol, creates a platform promoting virion assembly. In summary, we identify a bifunctional role of prM in the ZIKV life cycle by mediating viral entry and virus assembly in a cholesterol-dependent manner.

Funder

Deutsche Forschungsgemeinschaft

Helmholtz Association

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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