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Selective immunotargeting of diabetogenic CD4 T cells by genetically redirected T cells.

Immunology.. 2014-06; 
Perez S, Fishman S, Bordowitz A, Margalit A, Susan Wong F, Gross G. Laboratory of Immunology, MIGAL Galilee Research Institute, Kiryat Shmona, Israel.
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摘要

The key role played by islet-reactive CD8 and CD4 T cells in type 1 diabetes calls for new immunotherapies which target pathogenic T cells in a selective manner. We previously demonstrated that genetically linking the signaling portion of CD3-ζ onto the C-terminus of β2 -microglobulin and an autoantigenic peptide to its N-terminus converts MHC-I complexes into functional T cell receptor-specific receptors. CD8 T cells expressing such receptors specifically killed diabetogenic CD8 T cells, blocked T cell-induced diabetes in immunodeficient NOD.SCID mice and suppressed disease in wild-type NOD mice. Here we describe the immunotargeting of CD4 T cells by chimeric MHC-II receptors. To this end we chose th... More

关键词

T cell activation; adoptive T cell immunotherapy; chimeric receptors; mRNA transfection; type 1 diabetes