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Vimentin binding is critical for infection by the virulent strain of Japanese encephalitis virus
77
Citations
42
References
2011
Year
Vimentin ExpressionViral PathogenesisImmunologyMolecular BiologyViral Structural ProteinVirus StructureInfection ControlJapanese Encephalitis VirusVimentin ContributesVirologyFlavivirusVimentin BindingMolecular VirologyPathogenesisVirulent StrainDifferent Vimentin DependencyMicrobiologyVirus-host InteractionMedicineViral Immunity
Japanese encephalitis virus (JEV), a mosquito-borne flavivirus, causes acute encephalitis with high mortality in humans. We used a pair of virulent (RP-9) and attenuated (RP-2ms) variants of JEV to pull down the cell surface molecules bound with JEV particle; their identities were revealed by LC-MS/MS analysis. One major protein bound with RP-9 and weakly with RP-2ms was identified as the intermediate filament protein vimentin. Infection of RP-9 but not that of RP-2ms was blocked by anti-vimentin antibodies and by recombinant-expressed vimentin proteins. Knockdown of vimentin expression reduced the levels of viral binding and viral production of RP-9, but not that of RP-2ms. The different vimentin dependency for JEV infection could be attributed to the major structural envelope protein, as the recombinant RP-9 with an E-E138K mutation became resistant to anti-vimentin blockage. Furthermore, RP-2ms mainly depended on cell surface glycosaminoglycans for viral binding and it became vimentin-dependent only when binding to glycosaminoglycans was blocked. Thus, we suggest that vimentin contributes to virulent JEV infection and might be a new target to intervene in this deadly infection.
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