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. 2007 Oct;81(20):11341-51.
doi: 10.1128/JVI.00930-07. Epub 2007 Aug 8.

Genetic and phenotypic variation of foot-and-mouth disease virus during serial passages in a natural host

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Genetic and phenotypic variation of foot-and-mouth disease virus during serial passages in a natural host

C Carrillo et al. J Virol. 2007 Oct.

Abstract

Foot-and-mouth disease virus (FMDV), like other RNA viruses, exhibits high mutation rates during replication that have been suggested to be of adaptive value. However, even though genetic variation in RNA viruses and, more specifically, FMDV has been extensively examined during virus replication in a wide variety of in vitro cell cultures, very little is known regarding the generation and effects of genetic variability of virus replication in the natural host under experimental conditions and no genetic data are available regarding the effects of serial passage in natural hosts. Here, we present the results of 20 serial contact transmissions of the highly pathogenic, pig-adapted O Taiwan 97 (O Tw97) isolate of FMDV in swine. We examined the virus genomic consensus sequences for a total of 37 full-length viral genomes recovered from 20 in vivo passages. The characteristics and distributions of changes in the sequences during the series of pig infections were analyzed in comparison to the O Tw97 genomes recovered from serially infected BHK-21 cell cultures. Unexpectedly, a significant reduction of virulence upon pig passages was observed, and finally, interruption of the viral transmission chain occurred after the14th pig passage (T14). Virus was, however, isolated from the tonsils and nasal swabs of the asymptomatic T15 pigs at 26 days postcontact, consistent with a natural establishment of the carrier state previously described only for ruminants. Surprisingly, the region encoding the capsid protein VP1 (1D) did not show amino acid changes during in vivo passages. These data demonstrate that contact transmission of FMDV O Tw97 in pigs mimics the fitness loss induced by the bottleneck effect, which was previously observed by others during plaque-to-plaque FMDV passage in vitro, suggesting that unknown mechanisms of virulence recovery might be necessary during the evolution and perpetuation of FMDV in nature.

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Figures

FIG. 1.
FIG. 1.
Schematic representation of changes observed in the FMDV genome during passages in vivo and in vitro. White stars represent nucleotide changes fixed along the genome during passages. Black stars represent nonsynonymous fixed nucleotide changes. Data summary of in vivo and in vitro parameters of selective pressure: lnL, neperian log likelihood ratio value; tree branch length, number of nucleotide substitutions per codon; Ts/Tv, transition/transversion; dN/dS, number of nonsynonymous substitutions per nonsynonymous site/number of synonymous substitutions per synonymous site.

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