Núñez J I, Baranowski E, Molina N, Ruiz-Jarabo C M, Sánchez C, Domingo E, Sobrino F
Centro de Biología Molecular Severo Ochoa, Universidad Autónoma de Madrid, 28049 Madrid, Spain.
J Virol. 2001 Apr;75(8):3977-83. doi: 10.1128/JVI.75.8.3977-3983.2001.
The genetic changes selected during the adaptation of a clonal population of foot-and-mouth disease virus (FMDV) to the guinea pig have been analyzed. FMDV clone C-S8c1 was adapted to the guinea pig by serial passage in the animals until secondary lesions were observed. Analysis of the virus directly recovered from the lesions developed by the animals revealed the selection of variants with two amino acid substitutions in nonstructural proteins, I(248)-->T in 2C and Q(44)-->R in 3A. On further passages, an additional mutation, L(147)-->P, was selected in an important antigenic site located in the G-H loop of capsid protein VP1. The amino acid substitution Q(44)-->R in 3A, either alone or in combination with the replacement I(248)-->T in 2C, was sufficient to give FMDV the ability to produce lesions. This was shown by using infectious transcripts which generated chimeric viruses with the relevant amino acid substitutions. Clinical symptoms produced by the artificial chimeras were similar to those produced by the naturally adapted virus. These results obtained with FMDV imply that one or very few replacements in nonstructural viral proteins, which should be within reach of the mutant spectra of replicating viral quasispecies, may result in adaptation of a virus to a new animal host.
对口蹄疫病毒(FMDV)克隆群体适应豚鼠过程中选择的基因变化进行了分析。FMDV克隆C-S8c1通过在动物体内连续传代来适应豚鼠,直至观察到继发性病变。对直接从动物产生的病变中回收的病毒进行分析,发现选择了非结构蛋白中具有两个氨基酸替换的变体,2C中的I(248)-->T和3A中的Q(44)-->R。在进一步传代过程中,在衣壳蛋白VP1的G-H环中的一个重要抗原位点选择了另一个突变L(147)-->P。3A中的氨基酸替换Q(44)-->R,单独或与2C中的替换I(248)-->T组合,足以赋予FMDV产生病变的能力。通过使用产生具有相关氨基酸替换的嵌合病毒的感染性转录本证明了这一点。人工嵌合体产生的临床症状与自然适应病毒产生的症状相似。用FMDV获得的这些结果表明,病毒非结构蛋白中的一个或极少数替换,应该在复制病毒准种的突变谱范围内,可能导致病毒适应新的动物宿主。
