A single amino acid substitution in envelope protein E of tick-borne encephalitis virus leads to attenuation in the mouse model

Abstract

We have determined the virulence characteristics of seven monoclonal antibody escape mutants of tick-borne ecephalitis virus to the mouse model. One of the mutants with an amino acid substitution from tyrosine to histidine at residue 384 revealed strongly reduced pathogenicity after peripheral inoculation of adult mice but retained its capacity to replicate in the mice and to induce a high-titered antibody response. Infection with the attenuated mutant resulted in resistance to challenge with virulent virus. Assessment of nonconservative amino acid substitutions in other attenuated flaviviruses suggest that a structural element including residue 384 may represent an important determinant of flavivirus virulence in general.