Abstract
BackgroundThe flaviviridae family comprises single-stranded RNA viruses that enter cells via clathrin-mediated pH-dependent endocytosis. Although the initial events of the virus entry have been already identified, data regarding intracellular virus trafficking and delivery to the replication site are limited. The purpose of this study was to map the transport route of Zika virus and to identify the fusion site within the endosomal compartment.MethodsTracking of viral particles in the cell was carried out with confocal microscopy. Immunostaining of two structural proteins of Zika virus enabled precise mapping of the route of the ribonucleocapsid and the envelope and, consequently, mapping the fusion site in the endosomal compartment. The results were verified using RNAi silencing and chemical inhibitors.ResultsAfter endocytic internalization, Zika virus is trafficked through the endosomal compartment to fuse in late endosomes. Inhibition of endosome acidification using bafilomycin A1 hampers the infection, as the fusion is inhibited; instead, the virus is transported to late compartments where it undergoes proteolytic degradation. The degradation products are ejected from the cell via slow recycling vesicles. Surprisingly, NH4Cl, which is also believed to block endosome acidification, shows a very different mode of action. In the presence of this basic compound, the endocytic hub is reprogrammed. Zika virus-containing vesicles never reach the late stage, but are rapidly trafficked to the plasma membrane via a fast recycling pathway after the clathrin-mediated endocytosis.Further, we also noted that, similarly as other members of the flaviviridae family, Zika virus undergoes furin- or furin-like-dependent activation during late steps of infection, while serine or cysteine proteases are not required for Zika virus maturation or entry.ConclusionsZika virus fusion occurs in late endosomes and is pH-dependent. These results broaden our understanding of Zika virus intracellular trafficking and may in future allow for development of novel treatment strategies. Further, we identified a novel mode of action for agents commonly used in studies of virus entry.Schematic representation of differences in ZIKV trafficking in the presence of Baf A1 and NH4Cl
Highlights
The flaviviridae family comprises single-stranded RNA viruses that enter cells via clathrin-mediated pHdependent endocytosis
Tracking of single virions revealed that they follow clathrin-mediated endocytosis to fuse within late endosomes
We noted that two compounds commonly used to block endocytosis –bafilomycin Bafilomycin A1 [(3Z (A1) and NH4Cl - have a very different activity than previously anticipated
Summary
The flaviviridae family comprises single-stranded RNA viruses that enter cells via clathrin-mediated pHdependent endocytosis. The initial events of the virus entry have been already identified, data regarding intracellular virus trafficking and delivery to the replication site are limited. Zika virus (ZIKV) is a (+)ssRNA mosquito-borne flavivirus that infects humans [1]. It originates from Africa, it hit the spotlight almost 60 years after its first discovery, due to massive outbreaks in Micronesia, the South Pacific Islands, and South America [2,3,4,5]. The initial events of ZIKV entry have been identified [10,11,12]; but data regarding its fate thereafter are limited. The dependence of ZIKV on endocytosis has been confirmed in a variety of cell models [15]
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