Antibody responses to human rotavirus (HRV) in gnotobiotic pigs following a new prime/boost vaccine strategy using oral attenuated HRV priming and intranasal VP2/6 rotavirus‐like particle (VLP) boosting with ISCOM

SUMMARY Safer and more effective human rotavirus (HRV) vaccines are needed. We evaluated oral priming with attenuated WaHRV (AttHRV) followed by boosting with two intranasal (IN) doses of VP2/6 virus‐like particles (2/6 VLP) with immunostimulating complexes (ISCOM) to determine if this regimen induc...

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Published in:Clinical and experimental immunology 2004-03, Vol.135 (3), p.361-372
Main Authors: GONZÁLEZ, A. M., NGUYEN, T. V., AZEVEDO, M. S. P., JEONG, K., AGARIB, F., IOSEF, C., CHANG, K., LOVGREN‐BENGTSSON, K., MOREIN, B., SAIF, L. J.
Format: Article
Language:English
Subjects:
6 rotavirus‐like particles
Adjuvants, Immunologic
Animal Studies
Animals
Antibodies, Viral - biosynthesis
Biological and medical sciences
Diarrhea - immunology
Diarrhea - prevention & control
Diarrhea - veterinary
Dose-Response Relationship, Immunologic
Fundamental and applied biological sciences. Psychology
Fundamental immunology
Germ-Free Life
gnotobiotic pig model
Humans
Immunoglobulin A - biosynthesis
Immunoglobulin G - biosynthesis
Immunoglobulin M - biosynthesis
Immunopathology
intestinal immunity
Intestines - immunology
ISCOMs - immunology
Medical sciences
Rotavirus
Rotavirus - immunology
rotavirus antibody responses
Rotavirus Infections - immunology
Rotavirus Infections - prevention & control
Rotavirus Infections - veterinary
rotavirus intranasal vaccine
Rotavirus Vaccines - immunology
Swine
Swine Diseases - immunology
Swine Diseases - prevention & control
Vaccines, Attenuated - immunology
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Summary:SUMMARY Safer and more effective human rotavirus (HRV) vaccines are needed. We evaluated oral priming with attenuated WaHRV (AttHRV) followed by boosting with two intranasal (IN) doses of VP2/6 virus‐like particles (2/6 VLP) with immunostimulating complexes (ISCOM) to determine if this regimen induces protection against diarrhoea and viral shedding in the gnotobiotic pig model. IgM, IgA and IgG antibody titres in serum and intestinal contents were quantified by enzyme‐linked immunosorbent assay (ELISA) and serum neutralizing antibody titres were measured by a virus neutralization (VN) test. Seven groups of neonatal gnotobiotic pigs were vaccinated at post‐inoculation days (PID) 0, 10 and 21 and challenged with virulent WaHRV at PID 28. The vaccine groups included: (1, 2) oral priming with AttHRV and boosting with two IN immunizations with 2/6 VLP–ISCOM (Att + 2/6 VLP–ISCOM) at VLP concentrations of 250 µg or 25 µg; (3, 4) three IN immunizations with 2/6 VLP–ISCOM at VLP concentrations of 250 µg or 25 µg (2/6 VLP–ISCOM); (5) three oral immunizations with AttHRV (3×AttHRV); (6) one oral immunization with AttHRV (1×AttHRV); (7) controls (ISCOM matrix and/or diluent). The pigs that received 3×AttHRV or Att + 2/6 VLP250–ISCOM had the highest protection rates against diarrhoea upon challenge at PID 28 with virulent WaHRV. The IgA antibody titres to HRV in intestinal contents were significantly higher in the Att + 2/6 VLP250–ISCOM group than in all other groups prechallenge (PID 28). Serum VN antibody titres were statistically similar after the first inoculation among the groups given AttHRV, but at PID 28 VN antibody titres were significantly higher for the 3×AttHRV and Att + 2/6 VLP250–ISCOM groups than for the 1×AttHRV group suggesting that boosting with 2/6 VLP also boosted VN antibody responses. In humans, intestinal IgA antibodies have been correlated with protection against symptomatic reinfection. Thus the vaccine regimen of one oral dose of AttHRV and two IN immunizations with 2/6 VLP250–ISCOM may be an alternative to multiple‐dose live oral vaccines in humans.
ISSN:0009-9104
1365-2249
DOI:10.1111/j.1365-2249.2004.02395.x