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E and prM proteins of genotype V Japanese encephalitis virus are required for its increased virulence in mice.


ABSTRACT: We previously showed that the Japanese encephalitis virus (JEV) genotype V (GV) strain Muar exhibits significantly higher virulence in mice than the genotype I (GI) JEV strain Mie/41/2002. In this study, we attempted to identify the region responsible for the increased virulence of GV JEV using recombinant intertypic and single mutant JEVs. Intertypic viruses containing the GV E region in the Mie/41/2002 backbone showed increased pathogenicity in mice. The amino acid at position 123 in the E protein (E123) of the Mie/41/2002 and GV JEVs was serine and histidine, respectively. A serine-to-histidine substitution at E123 of the Mie/41/2002 increased its virulence. However, histidine-to-serine changes at E123 in the intertypic mutants with the GV E region remained highly virulent. GV Muar prM-bearing mutants were also highly pathogenic in mice. Our results suggest that the E and prM proteins of GV JEV are responsible for the highly virulent characteristics of GV JEV.

SUBMITTER: Tajima S 

PROVIDER: S-EPMC6881638 | biostudies-literature | 2019 Nov

REPOSITORIES: biostudies-literature

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E and prM proteins of genotype V Japanese encephalitis virus are required for its increased virulence in mice.

Tajima Shigeru S   Shibasaki Ken-Ichi KI   Taniguchi Satoshi S   Nakayama Eri E   Maeki Takahiro T   Lim Chang-Kweng CK   Saijo Masayuki M  

Heliyon 20191123 11


We previously showed that the Japanese encephalitis virus (JEV) genotype V (GV) strain Muar exhibits significantly higher virulence in mice than the genotype I (GI) JEV strain Mie/41/2002. In this study, we attempted to identify the region responsible for the increased virulence of GV JEV using recombinant intertypic and single mutant JEVs. Intertypic viruses containing the GV E region in the Mie/41/2002 backbone showed increased pathogenicity in mice. The amino acid at position 123 in the E pro  ...[more]

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