Major histocompatibility complex class I- and II-deficient knock-out mice are resistant to primary but susceptible to secondary Eimeria papillata infections |
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Authors: | Marco L Schito Bill Chobotar John R Barta |
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Institution: | (1) Department of Pathobiology, Ontario Veterinary College, University of Guelph, Guelph, Ontario, Canada N1G 2W2 Tel.: +1-519-824-4120 ext. 4017; Fax: +1-519-824-5930; E-mail: jbarta@uoguelph.ca, CA;(2) Department of Biology, Andrews University, Berrien Springs, MI 49104, USA, US |
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Abstract: | Two distinct mechanisms seem to function in reducing oocyst output during Eimeria papillata infections in mice. For naive mice, immunity was afforded␣by␣a T-cell-independent gamma-interferon (IFN-γ) response mediated
by natural killer (NK) cells. On reinfection, resistance was associated with T-cells and, to a lesser extent, perforin. To
determine if antigen presentation with major histocompatibility complex␣(MHC) molecules was required to control oocyst production
by NK cells during primary infection or by T-cells during secondary infection, mutant mice that lacked H2-IAβb (Aβb−/−) or β2-microglobulin (β2m−/−) were used. Since MHC molecules are required for the maturation of αβ T-cells, Aβb−/− and β2m−/− mutant mice are also deficient in functional αβ+CD4+ or αβ+CD8+ T-cells, respectively. As compared with wild-type control mice, oocyst output by mutant mice was not significantly affected
during primary infection, suggesting that the ability of NK cells to control parasite replication is not dependent on the
expression of MHC molecules. On reinfection, differences were observed for mutant mice as compared with controls. Aβb−/− mice were found to be more susceptible than β2m−/− mice, suggesting that the αβ+CD4+ T-cell subset plays a greater role in resistance to reinfection than does the αβ+CD8+ T-cell subset. The mechanism of resistance depends on the immune status of the host and requires the coordinated interaction
of both αβ+ T-cell subsets for optimal parasite control during subsequent infections.
Received: 6 August 1997 / Accepted: 24 October 1997 |
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