Autologous dendritic cells or cells expressing both B7-1 and MUC1 can rescue tumor-specific cytotoxic T lymphocytes from MUC1-mediated apoptotic cell death

Keiichi Kontani^*^,, Osamu Taguchi^*, Tatsuhiko Narita^*, Nozomu Hiraiwa^*, Satoru Sawai, Jun Hanaoka, Masutaro Ichinose, Noriaki Tezuka, Shuhei Inoue, Shozo Fujino and Reiji Kannagi^*

^* Laboratory of Experimental Pathology, Aichi Cancer Center Research Institute, Nagoya; and
Second Department of Surgery, Shiga University of Medical Science, Otsu, Japan

We attempted to induce MUC1-specific cytotoxic T lymphocytes(CTLs) by mixed-lymphocyte tumor cell culture (MLTC) using twoallogeneic MUC1-positive cancer cell lines, T-47D and MCF7.The induced CTLs exhibited MUC1-specific cytotoxicity 16 daysafter the initial stimulation. However, these CTLs underwentapoptotic death within 16 days. To examine whether the B7-1molecule is required for the expansion of the responder cells,a B7-1(+)/MUC1(-) cell line was transfected with MUC1 cDNA,and the resulting transfectant was employed as a stimulatorin an autologous MLTC. The CTLs exhibited MUC1 specificity butalso continued to propagate. In parallel, autologous dendriticcells (DCs) were added to an MLTC containing peripheral blood lymphocytes(PBLs) and the allogeneic MUC1-positive stimulators. The CTLsdemonstrated MUC1 specificity and their number increased. This suggeststhat the B7-1 molecule is required for rescuing CTLs from MUC1-mediatedapoptotic death, but not for the induction of MUC1-specificresponsiveness. This strategy to obtain the CTLs efficientlymay be useful for adoptive immunotherapy against cancer.

Key Words: apoptosis • dendritic cell • CTL