Genetic basis of attenuation of the Sabin type 3 oral poliovirus vaccine
GD Westrop, KA Wareham, DM Evans, G Dunn… - Journal of …, 1989 - Am Soc Microbiol
GD Westrop, KA Wareham, DM Evans, G Dunn, PD Minor, DI Magrath, F Taffs, S Marsden…
Journal of virology, 1989•Am Soc MicrobiolThe poliovirus type 3 Sabin oral poliovirus vaccine strain P3/Leon/12a1b differs in
nucleotide sequence from its neurovirulent progenitor P3/Leon/37 by just 10 point mutations.
The contribution of each mutation to the attenuation phenotype of the vaccine strain was
determined by the construction of a series of recombinant viruses from infectious cDNA
clones. The neurovirulence testing of recombinant viruses indicated that the attenuation
phenotype is determined by just two point mutations: a C to U in the noncoding region at …
nucleotide sequence from its neurovirulent progenitor P3/Leon/37 by just 10 point mutations.
The contribution of each mutation to the attenuation phenotype of the vaccine strain was
determined by the construction of a series of recombinant viruses from infectious cDNA
clones. The neurovirulence testing of recombinant viruses indicated that the attenuation
phenotype is determined by just two point mutations: a C to U in the noncoding region at …
The poliovirus type 3 Sabin oral poliovirus vaccine strain P3/Leon/12a1b differs in nucleotide sequence from its neurovirulent progenitor P3/Leon/37 by just 10 point mutations. The contribution of each mutation to the attenuation phenotype of the vaccine strain was determined by the construction of a series of recombinant viruses from infectious cDNA clones. The neurovirulence testing of recombinant viruses indicated that the attenuation phenotype is determined by just two point mutations: a C to U in the noncoding region at position 472 and a C to U at nucleotide 2034 which results in a serine-to-phenylalanine amino acid substitution in the structural protein VP3.
American Society for Microbiology