CD4 T Cells Are the Only Lymphocytes Needed To Protect Mice against Rotavirus Shedding after Intranasal Immunization with a Chimeric VP6 Protein and the Adjuvant LT(R192G)

McNeal, Monica; VanCott, John L.; Choi, Anthony H.-C.; Basu, M. N.; Flint, Jason; Stone, Susan; Clements, John D.; Ward, Richard L.

doi:10.1128/jvi.76.2.560-568.2002

Cited by 102 publications

(89 citation statements)

References 35 publications

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“…Our study demonstrated a direct correlation between the existence of extralymphoid IFN-γ producing T cells and protection at the site of virus entry (intestine). In studies of mice, intestinal IFN-γ producing CD4+ T cells were suggested to be the only lymphocytes required for protection against rotavirus infection after the mice were immunized with a chimeric VP6 vaccine using attenuated E. coli labile toxin as an adjuvant [15,28,46,47]. Their data and ours collectively emphasize the role of intestinal IFN-γ producing CD4+ T cells as correlates of rotavirus protective immunity, possibly more important than CD8+ T cells.…”

Section: Discussionmentioning

confidence: 55%

“…Also in studies of adult mice, CD4+ T cells were shown to be the only lymphocytes needed to protect mice against rotavirus infection after the mice were vaccinated with VP6 peptide vaccines [15,16]. Despite a large number of studies on the role of T cells in mediating protection against rotavirus infection in adult mice with various gene knockouts (protection against disease cannot be assessed in the adult mice model) [14][15][16][17][18], limited data is available on T cell immune responses to rotavirus in humans [19,20] or other out-bred native hosts, i.e. calves and pigs [21][22][23].…”

Section: Introductionmentioning

confidence: 99%

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Virus-specific intestinal IFN-γ producing T cell responses induced by human rotavirus infection and vaccines are correlated with protection against rotavirus diarrhea in gnotobiotic pigs

Yuan

Wen

Azevedo

et al. 2008

Vaccine

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We examined rotavirus-specific IFN-γ producing CD4+, CD8+ and CD4+CD8+ T cell responses in gnotobiotic pigs infected with a virulent human rotavirus (VirHRV) or vaccinated with an attenuated (Att) HRV vaccine (AttHRV3x or AttHRV2x) or an AttHRV oral priming and 2/6-virus-like particle (VLP) intranasal boosting (AttHRV-2/6VLP) regimen. In VirHRV infected pigs, HRV-specific IFN-γ producing T cells reside primarily in ileum. AttHRV-2/6VLP induced similar frequencies of intestinal IFN-γ producing T cells as the VirHRV, whereas AttHRV3x or 2x vaccines were less effective. Protection rates against rotavirus diarrhea upon VirHRV challenge significantly correlated (r = 0.97-1.0, p < 0.005) with frequencies of intestinal IFN-γ producing T cells, suggesting their role in protective immunity.

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Section: Discussionmentioning

confidence: 55%

Section: Introductionmentioning

confidence: 99%

Virus-specific intestinal IFN-γ producing T cell responses induced by human rotavirus infection and vaccines are correlated with protection against rotavirus diarrhea in gnotobiotic pigs

Yuan

Wen

Azevedo

et al. 2008

Vaccine

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show abstract

“…Thus, the secondary fecal Ab response observed in this model may be the consequence of a higher secondary systemic response. In this case, since anti-VP2 and anti-VP6 Ab are non-neutralizing, their role in protection should be limited, and other effectors, such as CD4 T cells, may be important for protection as shown recently by McNeal et al [29] after i.n. immunization of BALB/c mice with a chimeric protein VP6, a model which has some similarities with our model.…”

Section: Igdmentioning

confidence: 99%

Distribution and phenotype of murine rotavirus-specific B cells induced by intranasal immunization with 2/6 virus-like particles

et al. 2005

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Virus-like particles containing the rotavirus (RV) internal proteins VP2 and VP6 (2/6-VLP) have been shown to induce serum and fecal antibodies as well as protection in mice after intranasal administration with a mutant of E. coli toxin, LT-R192G. To better understand the origin of fecal IgA induced by this protocol, we studied the RV-specific B cell response in systemic and mucosal lymphoid tissues using a flow cytometry assay that allows quantification and phenotypic characterization of RV-specific B lymphocytes. We also assessed the RV-specific antibody-secreting cells in the spleen and intestinal lamina propria (ILP). A remarkably high frequency of RV-specific B cells was found in the respiratory lymphoid tissues and spleen, of which only a minority expressed the a4b7 integrin (intestinal homing receptor). In contrast, but in accordance with a4b7 expression at the induction site, a very low response was observed in intestinal lymphoid tissues (mesenteric lymph nodes and ILP), which did not increase after a second immunization. Thus, intranasal immunization with a nonreplicating antigen does not induce an important number of RV-specific B cells with an intestinal homing profile.

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“…The mechanisms by which VP6/LT(R192G) elicits protection appear to differ from those for live virus immunization in this model. That is, protection is reduced after live virus immunization of B-cell-deficient mice (27,42) but is fully retained for extended times after mucosal immunization with VP6/LT(R192G) (48).…”

mentioning

confidence: 99%

Mice Develop Effective but Delayed Protective Immune Responses When Immunized as Neonates either Intranasally with Nonliving VP6/LT(R192G) or Orally with Live Rhesus Rotavirus Vaccine Candidates

VanCott

Prada

McNeal

et al. 2006

J Virol

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Rotavirus vaccines are delivered early in life, when the immune system is immature. To determine the effects of immaturity on responses to candidate vaccines, neonatal (7 days old) and adult mice were immunized with single doses of either Escherichia coli-expressed rotavirus VP6 protein and the adjuvant LT(R192G) or live rhesus rotavirus (RRV), and protection against fecal rotavirus shedding following challenge with the murine rotavirus strain EDIM was determined. Neonatal mice immunized intranasally with VP6/LT(R192G) were unprotected at 10 days postimmunization (dpi) and had no detectable rotavirus B-cell (antibody) or CD4

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CD4 T Cells Are the Only Lymphocytes Needed To Protect Mice against Rotavirus Shedding after Intranasal Immunization with a Chimeric VP6 Protein and the Adjuvant LT(R192G)

Cited by 102 publications

References 35 publications

Virus-specific intestinal IFN-γ producing T cell responses induced by human rotavirus infection and vaccines are correlated with protection against rotavirus diarrhea in gnotobiotic pigs

Virus-specific intestinal IFN-γ producing T cell responses induced by human rotavirus infection and vaccines are correlated with protection against rotavirus diarrhea in gnotobiotic pigs

Distribution and phenotype of murine rotavirus-specific B cells induced by intranasal immunization with 2/6 virus-like particles

Mice Develop Effective but Delayed Protective Immune Responses When Immunized as Neonates either Intranasally with Nonliving VP6/LT(R192G) or Orally with Live Rhesus Rotavirus Vaccine Candidates

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