A new function for LAT and CD8 during CD8-mediated apoptosis that is independent of TCR signal transduction.

The majority (>95%) of thymocytes undergo apoptosis during selection in the thymus. Several mechanisms have been proposed to explain how apoptosis of thymocytes that are not positively selected occurs, however it is unknown whether thymocytes die purely by “neglect” or whether signaling through a cell surface receptor initiates an apoptotic pathway. We have previously demonstrated that on double positive (DP) thymocytes the ligation of CD8 in the absence of TCR engagement results in apoptosis and have postulated this is a mechanism to remove thymocytes that have failed positive selection. On mature single positive (SP) T cells CD8 acts as a co-receptor to augment signaling through the T cell receptor (TCR) that is dependent on the phosphorylation of the adaptor protein, Linker for Activation of T cells (LAT). Here we show that during CD8-mediated apoptosis of DP thymocytes there is an increase in the association of CD8 with LAT and an increase in LAT tyrosine phosphorylation. Decreasing LAT expression and mutation of tyrosine residues of LAT reduced apoptosis upon crosslinking of CD8. Our results identify novel functions for both CD8 and LAT that are independent of TCR signal transduction and suggest a mechanism for signal transduction leading to apoptosis upon CD8 crosslinking.