Published in

Microbiology Society, Journal of General Virology, 1(96), p. 64-73, 2015

DOI: 10.1099/vir.0.071639-0

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Triatoma virus structural polyprotein expression, processing and assembly into virus-like particles

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This paper is available in a repository.

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Abstract

In contrast to the current wealth of structural information concerning dicistrovirus particle structure very little is known about their morphogenetic pathways. Here we describe the expression of the two open reading frames encoded by Triatoma virus (TrV) genome. TrV, a member of the Cripavirus genus of the Dicistroviridae family, infects blood-sucking insects belonging to the Triatominae subfamily that act as vectors for the transmission of Trypanosoma cruzi, the etiological agent of the Chagas disease. We have established a baculovirus-based model for the expression of the NS (non structural) and P1 (structural) polyproteins. A preliminary characterization of the proteolytic processing of both polyprotein precursors has been performed using this system. We show that the proteolytic processing of the P1 polyprotein is strictly dependent upon the coexpression of the NS polyprotein, and that NS/P1 coexpression leads to the assembly of virus like particles (VLPs) exhibiting a morphology and a protein composition akin to natural TrV empty capsids. Remarkably, the unprocessed P1 polypeptide assembles into quasi-spherical structures conspicuously larger than VLPs produced in NS/P1-coexpressing cells likely representing a previously undescribed morphogenetic intermediate. This intermediate has not been found in members of the related Picornaviridae family currently used as a model for dicistrovirus studies, thus suggesting the existence of major differences in the assembly pathways of these two virus groups.