Publication | Open Access
A Unique Role for the Host ESCRT Proteins in Replication of Tomato bushy stunt virus
183
Citations
42
References
2009
Year
Viral ReplicationViral Polymerase StructureGeneticsViral Polymerase MechanismMolecular BiologyUnique RolePlant PathologyPlant VirologyVirus StructureReplicase ComplexPlant-virus InteractionHost Escrt ProteinsVirus GenePlus-stranded Rna VirusesPlant VirusVirologyGene ExpressionViral RnaBiomolecular EngineeringMolecular VirologyNatural SciencesPathogenesisMicrobiologyMedicine
Plus-stranded RNA viruses replicate in infected cells by assembling viral replicase complexes consisting of viral- and host-coded proteins. Previous genome-wide screens with Tomato bushy stunt tombusvirus (TBSV) in a yeast model host revealed the involvement of seven ESCRT (endosomal sorting complexes required for transport) proteins in viral replication. In this paper, we show that the expression of dominant negative Vps23p, Vps24p, Snf7p, and Vps4p ESCRT factors inhibited virus replication in the plant host, suggesting that tombusviruses co-opt selected ESCRT proteins for the assembly of the viral replicase complex. We also show that TBSV p33 replication protein interacts with Vps23p ESCRT-I and Bro1p accessory ESCRT factors. The interaction with p33 leads to the recruitment of Vps23p to the peroxisomes, the sites of TBSV replication. The viral replicase showed reduced activity and the minus-stranded viral RNA in the replicase became more accessible to ribonuclease when derived from vps23Delta or vps24Delta yeast, suggesting that the protection of the viral RNA is compromised within the replicase complex assembled in the absence of ESCRT proteins. The recruitment of ESCRT proteins is needed for the precise assembly of the replicase complex, which might help the virus evade recognition by the host defense surveillance system and/or prevent viral RNA destruction by the gene silencing machinery.
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