Combined Live Oral Priming and Intramuscular Boosting Regimen with Rotarix(®) and a Nanoparticle-Based Trivalent Rotavirus Vaccine Evaluated in Gnotobiotic Pig Models of G4P[6] and G1P[8] Human Rotavirus Infection

Human rotavirus (HRV) is the causative agent of severe dehydrating diarrhea in children under the age of five, resulting in up to 215,000 deaths each year. These deaths almost exclusively occur in low- and middle-income countries where vaccine efficacy is the lowest due to chronic malnutrition, gut...

Descripción completa

Detalles Bibliográficos
Autores principales: Hensley, Casey, Nyblade, Charlotte, Zhou, Peng, Parreño, Viviana, Ramesh, Ashwin, Frazier, Annie, Frazier, Maggie, Garrison, Sarah, Fantasia-Davis, Ariana, Cai, Ruiqing, Huang, Peng-Wei, Xia, Ming, Tan, Ming, Yuan, Lijuan
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2023
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10223133/
https://www.ncbi.nlm.nih.gov/pubmed/37243031
http://dx.doi.org/10.3390/vaccines11050927
_version_ 1785049868359696384
author Hensley, Casey
Nyblade, Charlotte
Zhou, Peng
Parreño, Viviana
Ramesh, Ashwin
Frazier, Annie
Frazier, Maggie
Garrison, Sarah
Fantasia-Davis, Ariana
Cai, Ruiqing
Huang, Peng-Wei
Xia, Ming
Tan, Ming
Yuan, Lijuan
author_facet Hensley, Casey
Nyblade, Charlotte
Zhou, Peng
Parreño, Viviana
Ramesh, Ashwin
Frazier, Annie
Frazier, Maggie
Garrison, Sarah
Fantasia-Davis, Ariana
Cai, Ruiqing
Huang, Peng-Wei
Xia, Ming
Tan, Ming
Yuan, Lijuan
author_sort Hensley, Casey
collection PubMed
description Human rotavirus (HRV) is the causative agent of severe dehydrating diarrhea in children under the age of five, resulting in up to 215,000 deaths each year. These deaths almost exclusively occur in low- and middle-income countries where vaccine efficacy is the lowest due to chronic malnutrition, gut dysbiosis, and concurrent enteric viral infection. Parenteral vaccines for HRV are particularly attractive as they avoid many of the concerns associated with currently used live oral vaccines. In this study, a two-dose intramuscular (IM) regimen of the trivalent, nanoparticle-based, nonreplicating HRV vaccine (trivalent S(60)-VP8*), utilizing the shell (S) domain of the capsid of norovirus as an HRV VP8* antigen display platform, was evaluated for immunogenicity and protective efficacy against P[6] and P[8] HRV using gnotobiotic pig models. A prime–boost strategy using one dose of the oral Rotarix(®) vaccine, followed by one dose of the IM trivalent nanoparticle vaccine was also evaluated. Both regimens were highly immunogenic in inducing serum virus neutralizing, IgG, and IgA antibodies. The two vaccine regimens failed to confer significant protection against diarrhea; however, the prime–boost regimen significantly shortened the duration of virus shedding in pigs challenged orally with the virulent Wa (G1P[8]) HRV and significantly shortened the mean duration of virus shedding, mean peak titer, and area under the curve of virus shedding after challenge with Arg (G4P[6]) HRV. Prime–boost-vaccinated pigs challenged with P[8] HRV had significantly higher P[8]-specific IgG antibody-secreting cells (ASCs) in the spleen post-challenge. Prime–boost-vaccinated pigs challenged with P[6] HRV had significantly higher numbers of P[6]- and P[8]-specific IgG ASCs in the ileum, as well as significantly higher numbers of P[8]-specific IgA ASCs in the spleen post-challenge. These results suggest the promise of and warrant further investigation into the oral priming and parenteral boosting strategy for future HRV vaccines.
format Online
Article
Text
id pubmed-10223133
institution National Center for Biotechnology Information
language English
publishDate 2023
publisher MDPI
record_format MEDLINE/PubMed
spelling pubmed-102231332023-05-28 Combined Live Oral Priming and Intramuscular Boosting Regimen with Rotarix(®) and a Nanoparticle-Based Trivalent Rotavirus Vaccine Evaluated in Gnotobiotic Pig Models of G4P[6] and G1P[8] Human Rotavirus Infection Hensley, Casey Nyblade, Charlotte Zhou, Peng Parreño, Viviana Ramesh, Ashwin Frazier, Annie Frazier, Maggie Garrison, Sarah Fantasia-Davis, Ariana Cai, Ruiqing Huang, Peng-Wei Xia, Ming Tan, Ming Yuan, Lijuan Vaccines (Basel) Article Human rotavirus (HRV) is the causative agent of severe dehydrating diarrhea in children under the age of five, resulting in up to 215,000 deaths each year. These deaths almost exclusively occur in low- and middle-income countries where vaccine efficacy is the lowest due to chronic malnutrition, gut dysbiosis, and concurrent enteric viral infection. Parenteral vaccines for HRV are particularly attractive as they avoid many of the concerns associated with currently used live oral vaccines. In this study, a two-dose intramuscular (IM) regimen of the trivalent, nanoparticle-based, nonreplicating HRV vaccine (trivalent S(60)-VP8*), utilizing the shell (S) domain of the capsid of norovirus as an HRV VP8* antigen display platform, was evaluated for immunogenicity and protective efficacy against P[6] and P[8] HRV using gnotobiotic pig models. A prime–boost strategy using one dose of the oral Rotarix(®) vaccine, followed by one dose of the IM trivalent nanoparticle vaccine was also evaluated. Both regimens were highly immunogenic in inducing serum virus neutralizing, IgG, and IgA antibodies. The two vaccine regimens failed to confer significant protection against diarrhea; however, the prime–boost regimen significantly shortened the duration of virus shedding in pigs challenged orally with the virulent Wa (G1P[8]) HRV and significantly shortened the mean duration of virus shedding, mean peak titer, and area under the curve of virus shedding after challenge with Arg (G4P[6]) HRV. Prime–boost-vaccinated pigs challenged with P[8] HRV had significantly higher P[8]-specific IgG antibody-secreting cells (ASCs) in the spleen post-challenge. Prime–boost-vaccinated pigs challenged with P[6] HRV had significantly higher numbers of P[6]- and P[8]-specific IgG ASCs in the ileum, as well as significantly higher numbers of P[8]-specific IgA ASCs in the spleen post-challenge. These results suggest the promise of and warrant further investigation into the oral priming and parenteral boosting strategy for future HRV vaccines. MDPI 2023-05-02 /pmc/articles/PMC10223133/ /pubmed/37243031 http://dx.doi.org/10.3390/vaccines11050927 Text en © 2023 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Hensley, Casey
Nyblade, Charlotte
Zhou, Peng
Parreño, Viviana
Ramesh, Ashwin
Frazier, Annie
Frazier, Maggie
Garrison, Sarah
Fantasia-Davis, Ariana
Cai, Ruiqing
Huang, Peng-Wei
Xia, Ming
Tan, Ming
Yuan, Lijuan
Combined Live Oral Priming and Intramuscular Boosting Regimen with Rotarix(®) and a Nanoparticle-Based Trivalent Rotavirus Vaccine Evaluated in Gnotobiotic Pig Models of G4P[6] and G1P[8] Human Rotavirus Infection
title Combined Live Oral Priming and Intramuscular Boosting Regimen with Rotarix(®) and a Nanoparticle-Based Trivalent Rotavirus Vaccine Evaluated in Gnotobiotic Pig Models of G4P[6] and G1P[8] Human Rotavirus Infection
title_full Combined Live Oral Priming and Intramuscular Boosting Regimen with Rotarix(®) and a Nanoparticle-Based Trivalent Rotavirus Vaccine Evaluated in Gnotobiotic Pig Models of G4P[6] and G1P[8] Human Rotavirus Infection
title_fullStr Combined Live Oral Priming and Intramuscular Boosting Regimen with Rotarix(®) and a Nanoparticle-Based Trivalent Rotavirus Vaccine Evaluated in Gnotobiotic Pig Models of G4P[6] and G1P[8] Human Rotavirus Infection
title_full_unstemmed Combined Live Oral Priming and Intramuscular Boosting Regimen with Rotarix(®) and a Nanoparticle-Based Trivalent Rotavirus Vaccine Evaluated in Gnotobiotic Pig Models of G4P[6] and G1P[8] Human Rotavirus Infection
title_short Combined Live Oral Priming and Intramuscular Boosting Regimen with Rotarix(®) and a Nanoparticle-Based Trivalent Rotavirus Vaccine Evaluated in Gnotobiotic Pig Models of G4P[6] and G1P[8] Human Rotavirus Infection
title_sort combined live oral priming and intramuscular boosting regimen with rotarix(®) and a nanoparticle-based trivalent rotavirus vaccine evaluated in gnotobiotic pig models of g4p[6] and g1p[8] human rotavirus infection
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10223133/
https://www.ncbi.nlm.nih.gov/pubmed/37243031
http://dx.doi.org/10.3390/vaccines11050927
work_keys_str_mv AT hensleycasey combinedliveoralprimingandintramuscularboostingregimenwithrotarixandananoparticlebasedtrivalentrotavirusvaccineevaluatedingnotobioticpigmodelsofg4p6andg1p8humanrotavirusinfection
AT nybladecharlotte combinedliveoralprimingandintramuscularboostingregimenwithrotarixandananoparticlebasedtrivalentrotavirusvaccineevaluatedingnotobioticpigmodelsofg4p6andg1p8humanrotavirusinfection
AT zhoupeng combinedliveoralprimingandintramuscularboostingregimenwithrotarixandananoparticlebasedtrivalentrotavirusvaccineevaluatedingnotobioticpigmodelsofg4p6andg1p8humanrotavirusinfection
AT parrenoviviana combinedliveoralprimingandintramuscularboostingregimenwithrotarixandananoparticlebasedtrivalentrotavirusvaccineevaluatedingnotobioticpigmodelsofg4p6andg1p8humanrotavirusinfection
AT rameshashwin combinedliveoralprimingandintramuscularboostingregimenwithrotarixandananoparticlebasedtrivalentrotavirusvaccineevaluatedingnotobioticpigmodelsofg4p6andg1p8humanrotavirusinfection
AT frazierannie combinedliveoralprimingandintramuscularboostingregimenwithrotarixandananoparticlebasedtrivalentrotavirusvaccineevaluatedingnotobioticpigmodelsofg4p6andg1p8humanrotavirusinfection
AT fraziermaggie combinedliveoralprimingandintramuscularboostingregimenwithrotarixandananoparticlebasedtrivalentrotavirusvaccineevaluatedingnotobioticpigmodelsofg4p6andg1p8humanrotavirusinfection
AT garrisonsarah combinedliveoralprimingandintramuscularboostingregimenwithrotarixandananoparticlebasedtrivalentrotavirusvaccineevaluatedingnotobioticpigmodelsofg4p6andg1p8humanrotavirusinfection
AT fantasiadavisariana combinedliveoralprimingandintramuscularboostingregimenwithrotarixandananoparticlebasedtrivalentrotavirusvaccineevaluatedingnotobioticpigmodelsofg4p6andg1p8humanrotavirusinfection
AT cairuiqing combinedliveoralprimingandintramuscularboostingregimenwithrotarixandananoparticlebasedtrivalentrotavirusvaccineevaluatedingnotobioticpigmodelsofg4p6andg1p8humanrotavirusinfection
AT huangpengwei combinedliveoralprimingandintramuscularboostingregimenwithrotarixandananoparticlebasedtrivalentrotavirusvaccineevaluatedingnotobioticpigmodelsofg4p6andg1p8humanrotavirusinfection
AT xiaming combinedliveoralprimingandintramuscularboostingregimenwithrotarixandananoparticlebasedtrivalentrotavirusvaccineevaluatedingnotobioticpigmodelsofg4p6andg1p8humanrotavirusinfection
AT tanming combinedliveoralprimingandintramuscularboostingregimenwithrotarixandananoparticlebasedtrivalentrotavirusvaccineevaluatedingnotobioticpigmodelsofg4p6andg1p8humanrotavirusinfection
AT yuanlijuan combinedliveoralprimingandintramuscularboostingregimenwithrotarixandananoparticlebasedtrivalentrotavirusvaccineevaluatedingnotobioticpigmodelsofg4p6andg1p8humanrotavirusinfection

Ejemplares similares