The complete genomic sequence of very virulent infectious bursal disease virus (vvIBDV) Gx strain was determined, including the sequences of segment A, encoding the precursor polyprotein, and segment B, encoding the viral RNA polymerase (VP1) and 5′- and 3′-untranslating regions. Alignment of segment A of Gx with the sequences of 12 other vvIBDV strains showed 97.5% to 99.0% amino acid identity, whereas alignment of segment B of Gx with nine other vvIBDV strains revealed high sequence divergence, ranging from 10.3% to 11%. Phylogenetic analysis of segments A and B showed that they were in different branches, indicating that the reassortment occurred in this strain and that segment A and segment B derived from different pathotype strains. The mutant spectrum analysis of quasispecies virus demonstrated that the mean minimum mutation frequency in VP1 was 8.78-fold higher than in the polyprotein. The most frequent mutations were in the first 1986 nucleotides (nonsynonymous mutations) and the last 660 nucleotides (synonymous mutations), indicating that the 219 amino acid residues in the C-terminal of the VP1 form a functional region.
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1 December 2007
Direct Evidence of Reassortment and Mutant Spectrum Analysis of a Very Virulent Infectious Bursal Disease Virus
Hong-Lei Gao,
Xiao-Mei Wang,
Yu-Long Gao,
Chao-Yang Fu
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Avian Diseases
Vol. 51 • No. 4
December 2007
Vol. 51 • No. 4
December 2007
functional region
quasispecies
reassortment
very virulent infectious bursal disease virus