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Clinical and Experimental Immunology logoLink to Clinical and Experimental Immunology
. 1997 Dec;110(3):397–402. doi: 10.1046/j.1365-2249.1997.4251442.x

Phenotypic characterization and analysis of allogeneic T cell responses in ZAP-70 dominant negative transgenic mice

R P GLADUE *, M ALLEN *, A CUNNINGHAM *, J GARDNER *, A M LAQUERRE *, P A CONNELLY *, A S SHAW *, J MCNEISH *
PMCID: PMC1904829  PMID: 9409642

Abstract

Antigen stimulation of T cells results in a series of biochemical events including the interaction of both SH2 domains of ZAP-70 with phosphorylated ITAMS on the T cell receptor. In order to study the physiological relevance of decreasing native ZAP-70–SH2 interaction in vivo, we generated transgenic mice expressing a T cell-specific, dominant negative form of ZAP-70 consisting of only the tandem SH2 domains (ZAP-NC). Phenotypically, these animals had a comparable distribution of lymphocyte subsets in the thymus and spleen compared with the wild-type (WT) controls. However, examination of peripheral blood revealed a slow but progressive decrease in the number of lymphocytes, particularly CD4+ cells, with age (17% reduction by 3 months, 58% reduction by 6 months). Allogeneic responses were then evaluated in vitro as well as in vivo using a subcutaneous sponge matrix implant. Although spleen cells cultured for 4 days in vitro with alloantigen developed normal functional responses, allogeneic responses generated in vivo within a subcutaneous sponge matrix were impaired. This was characterized by a depression in cytotoxic T lymphocyte (CTL) activity, a 82% reduction in the frequency of helper T cells, and a 78% reduction in the capacity of sponge-infiltrating lymphocytes to produce IL-2 in response to secondary antigen stimulation. These results indicate that although overt lymphocyte development and in vitro function were unremarkable, expression of a truncated ZAP-70 affected the in vivo survival of peripheral lymphocytes and altered the in vivo generation of functional activity to alloantigen.

Keywords: ZAP-70, allogeneic responses, sponge matrix model

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