Development of recombinant rotavirus carrying herpes simplex virus 2 glycoprotein D gene based on reverse genetics technology.
Yoshiki KawamuraSatoshi KomotoSaori FukudaMasanori KugitaShuang TangAmita PatelJulianna R PieknikShizuko NagaoKoki TaniguchiPhilip R KrauseTetsushi YoshikawaPublished in: Microbiology and immunology (2023)
Vaccine development for herpes simplex virus 2 (HSV-2) has been attempted, but no vaccines are yet available. A plasmid-based reverse genetics system for Rotavirus (RV), which can cause gastroenteritis, allows the generation of recombinant RV containing foreign genes. In this study, we sought to develop simian RV (SA11) as a vector to express HSV-2 glycoprotein D (gD2) and evaluated its immunogenicity in mice. We generated the recombinant SA11-gD2 virus (rSA11-gD2) and confirmed its ability to express gD2 in vitro. The virus was orally inoculated into suckling BALB/c mice and into 8-week-old mice. Serum IgG and IgA titers against RV and gD2 were measured by ELISA. In the 8-week-old mice inoculated with rSA11-gD2, significant increases in not only antibodies against RV but also IgG against gD2 were demonstrated. In the suckling mice, antibodies against RV were induced, but gD2 antibody was not detected. Diarrhea observed after the first inoculation of rSA11-gD2 in suckling mice was similar to that induced by the parent virus. A gD2 expressing simian RV recombinant, which was orally inoculated, induced IgG against gD2. This strategy holds possibility for genital herpes vaccine development.
Keyphrases
- mycobacterium tuberculosis
- herpes simplex virus
- high fat diet induced
- escherichia coli
- clinical trial
- wild type
- type diabetes
- gene expression
- randomized controlled trial
- diabetic rats
- cell free
- insulin resistance
- crispr cas
- metabolic syndrome
- genome wide
- skeletal muscle
- copy number
- adipose tissue
- drug induced
- stress induced
- study protocol
- clostridium difficile