Abstract EN:

We have identified a tumor antigen (AG) recognized on a human lung carcinoma by an autologous cytotoxic T cell clone. It is encoded by "calca" gene (calcitonin/calcitonin-gene-related peptide) which is overexpresses in a large range of lung cancers and medullary thyroïd carcinomas (MTC) but not in normal tissues. The epiptode derives from the signal peptide of the preprocalcitonin. Its processing is proteasome-and TAP-independent but involves the signal peptidase (SP) and the signal peptide peptidase (SPP). This antigenic peptide corresponds to a promising candidate for MTC and lung cancer immunotherapy. We have also studied the spontaneous T cell response generated against a tumor AG encoded by mutated A-actinin-4-gene. Our results indicated that T cell clones derivated from lymphocytes infiltrating the tumor lyse more efficiently the autologous tumor cells than those isolated from patient peripheral blood lymphocytes. The TCR inhibitory protein CD5 plays a critical role in modulating anti-tumor T cell response and in protecting peripheral blood T lymphocytes from activated induced cell death (AICD).