T-cell subsets in delayed-type hypersensitivity, protection, and granuloma formation in primary and secondary Listeria infection in mice: superior role of Lyt-2+ cells in acquired immunity.

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Infect Immun. 1988 August; 56(8): 1920-1925

T-cell subsets in delayed-type hypersensitivity, protection, and granuloma formation in primary and secondary Listeria infection in mice: superior role of Lyt-2+ cells in acquired immunity.

M E Mielke, S Ehlers and H Hahn

Institut für Medizinische Mikrobiologie und Infektionsimmunologie, Berlin, Federal Republic of Germany.

ABSTRACT

Immunity to Listeria monocytogenes was studied in mice treatedwith rat monoclonal antibodies (MAbs) specific for the Thy-1.2,L3T4, and Lyt-2 T-cell markers. Three characteristic T-cell-mediatedphenomena were investigated. Delayed-type hypersensitivity (DTH)to listerial antigen was totally abolished in mice treated withanti-Thy-1.2 or anti-L3T4 MAbs, whereas anti-Lyt-2 MAb treatmenthad no effect, regardless of whether the MAb was given duringthe induction or the expression of DTH. On the other hand, theelimination of bacteria from the spleens of infected animalswas inhibited only by the application of either anti-Thy-1.2MAb or anti-Lyt-2 MAb. This could be shown most impressivelyduring the secondary infection of immune mice with a normallylethal dose of listeriae. In this situation, treatment withanti-Lyt-2 MAb sufficed to completely abolish immunologic memory,whereas anti-L3T4 MAb had only a marginal effect on antibacterialprotection. However, the accelerated development of mononuclearcell foci in the livers of immune mice was inhibited by theapplication of both anti-L3T4 MAb and anti-Lyt-2 MAb. It isconcluded that in murine listeriosis, DTH and acquired immunityto reinfection are dissociable phenomena. Although DTH is afunction of L3T4+ T lymphocytes, Lyt-2+ T cells are necessaryand sufficient for the expression of acquired resistance toL. monocytogenes. The roles of the different T-cell subsetsin granuloma formation warrant further investigation.

Infect Immun. 1988 August; 56(8): 1920-1925

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