Induction of peripheral tolerance in dual TCR T cells: An evidence for non-dominant signaling by one TCR

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Abstract

Recently, the existence of T cells with dual T cell receptor (TCR) in the immune system is generally accepted, while it has been controversial whether signals through one TCR would affect the functions of the other. In this study T cells expressing two different TCR were obtained from cross-hybrids of LCMV and AND TCR transgenic mice specific for the gp33 and peptide fragment of PCC (fPCC), respectively. Peptide stimulation demonstrated that the dual TCR T cells functioned independently in an antigen-specific manner. To examine whether the tolerance targeted for the one TCR affects the responsiveness of the other, the cross-hybrids were treated with gp33. Although T cells from F1 mice were rendered anergenic to gp33, no functional changes to fPCC were observed in terms of cellular proliferation and IL-2 secretion, suggesting that the dual TCR T cells remained reactive to fPCC. We therefore propose that signaling through the TCR is receptor-specific and 'negative dominance' of one TCR by tolerance induction is not applicable in this dual TCR system.

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APA

Hah, C., Kim, M., & Kim, K. (2005). Induction of peripheral tolerance in dual TCR T cells: An evidence for non-dominant signaling by one TCR. Journal of Biochemistry and Molecular Biology, 38(3), 334–342. https://doi.org/10.5483/bmbrep.2005.38.3.334

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