Single Mutation in the Flavivirus Envelope Protein Hinge Region Increases Neurovirulence for Mice and Monkeys but Decreases Viscerotropism for Monkeys: Relevance to Development and Safety Testing of Live, Attenuated Vaccines

Monath, Thomas P.; Arroyo, Juan; Levenbook, Inessa S.; Zhang, Zhenxi; Catalan, John; Draper, Ken; Guirakhoo, Farshad

doi:10.1128/jvi.76.4.1932-1943.2002

Cited by 136 publications

(101 citation statements)

References 41 publications

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“…The growth rate of Muar was less than that of the (Tajima et al, 2010). Other reports have also highlighted the importance of the E protein as a determinant of pathogenicity (Monath et al, 2002;Sumiyoshi et al, 1995;Zhao et al, 2005). In contrast, our group determined that an amino acid substitution in the JEV NS4A protein alters virulence in mice (Yamaguchi et al, 2011).…”

Section: Discussioncontrasting

confidence: 41%

In vitro growth, pathogenicity and serological characteristics of the Japanese encephalitis virus genotype V Muar strain

Tajima

Yagasaki

Kotaki

et al. 2015

Journal of General Virology

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The characteristics of genotype V Japanese encephalitis virus (GV JEV) remain poorly understood as only two strains have been isolated to date. In this study, we examined the effects of the GV JEV Muar strain on in vitro growth and pathogenicity in mice; we also evaluated the efficacy of inactivated JEV vaccines against the Muar strain. Although growth of the Muar strain in mouse neuroblastoma N18 cells was clearly worse than that of the GIII Beijing-1 and GI Mie/41/2002 strains, neuroinvasiveness of the Muar strain was similar to that of the Beijing-1 strain and significantly higher than that of the Mie/41/2002 strain. The results of a plaque reduction neutralization test suggested that the neutralization ability of the JEV vaccines against the Muar strain was reduced compared with the GI and GIII strains. However, the protection potency of the JEV vaccine against the Muar strain was similar to that for the Beijing-1 strain in mice. Our data indicate that GV JEV has unique growth, virulence and antigenicity features.

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Section: Discussioncontrasting

confidence: 41%

In vitro growth, pathogenicity and serological characteristics of the Japanese encephalitis virus genotype V Muar strain

Tajima

Yagasaki

Kotaki

et al. 2015

Journal of General Virology

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“…Residues E136 and E138 lie in close proximity and are located within the so-called "hinge" region at the domain I-II interface of the E protein, which is responsible for a pH-dependent conformational change during virus penetration from the endosome into the cytoplasm of an infected cell (24). Other studies have provided data indicating that mutations within this region modulate virulence phenotypes in mice, and this modulation is believed to occur through effects of such mutations on the low-pH-induced dimer-to-trimer structural transition of the E protein associated with virus entry (3,9,12,19,20,28).…”

Section: Discussionmentioning

confidence: 99%

“…The study of chimeras has afforded new insights into the molecular basis of virulence and new prospects for vaccine development (19). Detailed investigation of virus adaptation to different hosts and tissues remains to be conducted.…”

mentioning

confidence: 99%

Molecular Basis for Adaptation of a Chimeric Dengue Type‐4/Japanese Encephalitis Virus to Vero Cells

Tang

Eshita

Tadano

et al. 2005

Microbiology and Immunology

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The premembrane and envelope (E) genes of a full‐length cDNA clone of the dengue type‐4 (DEN4) virus 814669 strain were replaced with those of the Japanese encephalitis (JE) virus JaOH0566 strain. The in vitro‐synthesized RNA transcripts prepared from chimeric cDNA were used to transfect mosquito C6/36 cells. A viable chimeric virus (designated DEN4/JE) was recovered. Unexpectedly, DEN4/JE exhibited restricted growth in Vero cells. After a serial passage in Vero cells, the Vero‐adapted chimeras were obtained (two clones, designated Strain I and Strain II, respectively). The entire genomes of DEN4/JE, Strain I, and Strain II were sequenced and compared. There were multiple mutations, but amino acid substitutions occurred only in E and nonstructural (NS) protein NS4B. Our findings in this study indicate that the 5′ nontranslated region, E, and NS4B may be involved in Vero cell adaptation in this chimeric system.

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“…DIII is also believed to contain the receptor-binding sites to the host cell (Erb et al, 2010;Mukhopadhyay et al, 2005) and has been implicated in determining host range, tropism and virulence (Lindenbach et al, 2007). A hinge region formed by the four strands that span between the different DI and DII coding segments provides the flexibility for E conformational changes during virus maturation (Butrapet et al, 2011;Monath et al, 2002), while a linker of 11 aa connects DI to DIII and is fundamental for proper E folding (de Wispelaere & Yang, 2012). …”

Section: Introductionmentioning

confidence: 99%

Secretion of dengue virus envelope protein ectodomain from mammalian cells is dependent on domain II serotype and affects the immune response upon DNA vaccination

Slon-Campos

Poggianella

Marchese

et al. 2015

Journal of General Virology

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Dengue virus (DENV) is currently among the most important human pathogens and affects millions of people throughout the tropical and subtropical regions of the world. Although it has been a World Health Organization priority for several years, there is still no efficient vaccine available to prevent infection. The envelope glycoprotein (E), exposed on the surface on infective viral particles, is the main target of neutralizing antibodies. For this reason it has been used as the antigen of choice for vaccine development efforts. Here we show a detailed analysis of factors involved in the expression, secretion and folding of E ectodomain from all four DENV serotypes in mammalian cells, and how this affects their ability to induce neutralizing antibody responses in DNA-vaccinated mice. Proper folding of E domain II (DII) is essential for efficient E ectodomain secretion, with DIII playing a significant role in stabilizing soluble dimers. We also show that the level of protein secreted from transfected cells determines the strength and efficiency of antibody responses in the context of DNA vaccination and should be considered a pivotal feature for the development of E-based DNA vaccines against DENV.

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Single Mutation in the Flavivirus Envelope Protein Hinge Region Increases Neurovirulence for Mice and Monkeys but Decreases Viscerotropism for Monkeys: Relevance to Development and Safety Testing of Live, Attenuated Vaccines

Cited by 136 publications

References 41 publications

In vitro growth, pathogenicity and serological characteristics of the Japanese encephalitis virus genotype V Muar strain

In vitro growth, pathogenicity and serological characteristics of the Japanese encephalitis virus genotype V Muar strain

Molecular Basis for Adaptation of a Chimeric Dengue Type‐4/Japanese Encephalitis Virus to Vero Cells

Secretion of dengue virus envelope protein ectodomain from mammalian cells is dependent on domain II serotype and affects the immune response upon DNA vaccination

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