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Trichuris muris: CD4+ T cell-mediated protection in reconstituted SCID mice

Published online by Cambridge University Press:  27 April 2001

C. J. BETTS
Affiliation:
3.239 Stopford Building, School of Biological Sciences, University of Manchester, Oxford Road, Manchester M13 9PT, UK Present address: AstraZeneca, H1.11 CTL, Alderley Park, Macclesfield, Cheshire, SK10 4TJ. E-mail: [email protected]
M. L. deSCHOOLMEESTER
Affiliation:
3.239 Stopford Building, School of Biological Sciences, University of Manchester, Oxford Road, Manchester M13 9PT, UK
K. J. ELSE
Affiliation:
3.239 Stopford Building, School of Biological Sciences, University of Manchester, Oxford Road, Manchester M13 9PT, UK

Abstract

Resistance to the murine intestinal nematode Trichuris muris requires the development of a strong Th2 response. In a reconstituted SCID mouse model, CD4+ Th2 cells can mediate resistance to infection in the absence of antibody (Else & Grencis, 1996). The data presented here address the issue of how CD4+ T cells mediate this protective immunity within the SCID host. These studies demonstrate that timing and cell dose are critical if transfer is to result in resistance, with a minimum of 5 × 106 immune donor cells required to confer immunity. Furthermore, this CD4-mediated protective immunity only operates against the larval stages of the parasite. When the molecules necessary for activated CD4+ T cell migration to the GALT are inhibited with a cocktail of anti-integrin/addressin antibodies (anti-β7, anti-MAdCAM-1 and anti-αE), the resistance conferred by immune donor cells is completely abrogated. This implies that the effector mechanism acts locally at the level of the gut. CD4+ mediated cytotoxicity, directed against the epithelial cells inhabited by the parasite, could represent a novel, locally acting effector mechanism. However, Fas and Fas ligand-deficient mice, which are unable to mount CD4-mediated cytotoxic responses, readily expel T. muris indicating that the mechanism by which CD4+ T cells mediate protective immunity is unlikely to involve killing of infected gut epithelial cells.

Type
Research Article
Copyright
2000 Cambridge University Press

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