Viruses (Jul 2024)

Immunogenicity of a Rotavirus VP8* Multivalent Subunit Vaccine in Mice

  • Roberto Cárcamo-Calvo,
  • Irene Boscá-Sánchez,
  • Sergi López-Navarro,
  • Noemi Navarro-Lleó,
  • Nazaret Peña-Gil,
  • Cristina Santiso-Bellón,
  • Javier Buesa,
  • Roberto Gozalbo-Rovira,
  • Jesús Rodríguez-Díaz

DOI
https://doi.org/10.3390/v16071135
Journal volume & issue
Vol. 16, no. 7
p. 1135

Abstract

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Rotavirus remains a significant public health threat, especially in low-income countries, where it is the leading cause of severe acute childhood gastroenteritis, contributing to over 128,500 deaths annually. Although the introduction of the Rotarix and RotaTeq vaccines in 2006 marked a milestone in reducing mortality rates, approximately 83,158 preventable deaths persisted, showing ongoing challenges in vaccine accessibility and effectiveness. To address these issues, a novel subcutaneous vaccine formulation targeting multiple rotavirus genotypes has been developed. This vaccine consists of nine VP8* proteins from nine distinct rotavirus genotypes and sub-genotypes (P[4], P[6], P[8]LI, P[8]LIII, P[8]LIV, P[9], P[11], P[14], and P[25]) expressed in E. coli. Two groups of mice were immunized either with a single immunogen, the VP8* from the rotavirus Wa strain (P[8]LI), or with the nonavalent formulation. Preliminary results from mouse immunization studies showed promising outcomes, eliciting antibody responses against six of the nine immunogens. Notably, significantly higher antibody titers against VP8* P[8]LI were observed in the group immunized with the nonavalent vaccine compared to mice specifically immunized against this genotype alone. Overall, the development of parenteral vaccines targeting multiple rotavirus genotypes represents a promising strategy in mitigating the global burden of rotavirus-related morbidity and mortality, offering new avenues for disease prevention and control.

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