Abstract
The identification of endogenously produced antigenic peptides presented by MHC class I molecules has opened the way to peptide‐based strategies for CTL induction in vivo. Here we demonstrate that the induction in vivo of CTL directed against naturally processed antigens can be triggered by injection of syngeneic cells expressing covalent major histocompatibility complex class I‐peptide complexes. In the model system used, the induction of HLA‐Cw3 specific cytotoxic T lymphocytes (CTL) in mice by cell surface‐associated, covalent H‐2K^d^ (K^d^)‐Cw3 peptide complexes was investigated. The K^d^‐restricted Cw3 peptide 170–179 (RYLKNGKETL), which mimics the major natural epitope recognized by Cw3‐specific CTL in H‐2^d^ mice, was converted to a photoreactive derivative by replacing Arg‐170 with N‐β‐(4‐azidosalicyloyl)‐L‐2,3‐diaminopropionic acid. This peptide derivative was equivalent to the parental Cw3 peptide in terms of binding to K^d^ molecules and recognition by Cw3‐specific CTL clones and could be cross‐linked efficiently and selectively to K^d^ molecules on the surface of Con A‐stimulated spleen cells from H‐2^d^ mice. Photocross‐linking prevented the rapid dissociation of K^d^‐peptide derivative complexes that takes place under physiological conditions. Cultures of spleen cells or peritoneal exudate cells from mice inoculated i.p. with peptide‐pulsed and photocross‐linked cells developed a strong CTL response following antigenic stimulation in vitro. The cultured cells efficiently lysed not only target cells sensitized with the Cw3 170–179 peptide but also target cells transfected with the Cw3 gene. Moreover, their TCR preferentially expressed Vβ10 and JαpHDS58 segments as well as conserved junctional sequences, as has been observed previously in Cw3‐specific CTL responses. In contrast, no Cw3‐specific CTL response could be obtained in cultures derived from mice injected with Con A‐stimulated spleen cells pulsed with the peptide derivative without photocross‐linking.