Co-receptor-independent signal transduction in a mismatched CD8+ major histocompatibility complex class II-specific allogeneic cytotoxic T lymphocyte

Abstract

The contribution of co‐receptors in signal transduction upon T cell receptor (TCR)‐mediated recognition of major histocompatibility complex (MHC) class II antigen by mature T lymphocytes expressing TCR derived from the apparently co‐receptor‐independent, I‐A^k‐specific allogeneic CD8⁺ CTL clone QM11 has been examined. Mature double‐negative, CD8⁺ and CD4⁺ bulk T cell lines and clones expressing TCRQM11 were developed from TCRQM11 transgenic mice. All these T cells, irrespective of co‐receptor expression, showed specific lytic activity on cells expressing I‐A^k. Furthermore, co‐receptorless mutants were obtained from a CD4⁺ and CD8⁺ clone. The responses of these co‐receptorless mutants upon specific recognition of the alloantigen, as judged by cytolytic activity, granule exocytosis, lymphokine production, proliferation, and tyrosine phos‐phorylation of the ξ chain, were comparable to those of the original clones. Thus, the results proved the co‐receptor independence of the recognition of I‐A^k by TCRQM11 and further indicated there is no indispensable unique signal transduced by co‐receptors. However, when the amount of the available antigen was limited by anti‐I‐A^k antibody, the CD4⁺ T cell clone showed a remarkable resistance to the inhibition whereas the mismatched CD8⁺ clone was readily inhibitable. The anti‐I‐A^k‐resistant component of the CD4⁺ clone showed dependency on the CD4 molecule. Taken collectively, the results indicate that the role played by a co‐receptor molecule in mature T cells is purely quantitative amplification of the signal through the formation of a TCR/MHC/co‐receptor ternary complex, and also indicate that the role of co‐receptor molecules as TCR‐independent adhesion molecules is at best minimal.