TY - JOUR
T1 - Different repertoires of mouse T cells for bovine insulin presented by syngeneic and allogeneic cells
AU - Ishii, Norishisa
AU - Klein, Jan
AU - Nagy, Zoltan A.
PY - 1983
Y1 - 1983
N2 - Splenic T cells were primed, after removal of alloreactive cells, to beef insulin on allogeneic antigen‐presenting cells (APC). The fine specificity of in vitro secondary response was tested in combinations H‐2b (responder) T cell‐H‐2k (nonresponder) APC, and vice versa, using separated chains of beef and pork insulin. The response in both combinations exhibited identical specificity patterns demonstrating that both responder and nonresponder APC could present the same array of insulin epitopes to allogeneic T cells. The determinants presented to allogeneic T cells include the A‐chain loop epitope and the B‐chain determinant(s) that were found to be immunogenic for H‐2b and H‐2d T cells, respectively, in the context of syngeneic major histocompatibility complex (HC) molecules. In addition, minor determinants were detected in the A chain outside the loop that are not immunogenic in syngeneic T cell‐APC combinations. Inhibition of T cell proliferation with monoclonal antibodies has shown that class II MHC molecules of the nonresponder (AαkAβk, EαkEβk) as well as those of the responder APC (AαbAβb) are equally capable of presenting virtually all insulin epitopes recognizable by T cells. The data, therefore, demonstrate that the selective recognition of different insulin epitopes observed in syngeneic or semisyngeneic T cell‐APC combinations does not result from determinant selection at the level of APC.
AB - Splenic T cells were primed, after removal of alloreactive cells, to beef insulin on allogeneic antigen‐presenting cells (APC). The fine specificity of in vitro secondary response was tested in combinations H‐2b (responder) T cell‐H‐2k (nonresponder) APC, and vice versa, using separated chains of beef and pork insulin. The response in both combinations exhibited identical specificity patterns demonstrating that both responder and nonresponder APC could present the same array of insulin epitopes to allogeneic T cells. The determinants presented to allogeneic T cells include the A‐chain loop epitope and the B‐chain determinant(s) that were found to be immunogenic for H‐2b and H‐2d T cells, respectively, in the context of syngeneic major histocompatibility complex (HC) molecules. In addition, minor determinants were detected in the A chain outside the loop that are not immunogenic in syngeneic T cell‐APC combinations. Inhibition of T cell proliferation with monoclonal antibodies has shown that class II MHC molecules of the nonresponder (AαkAβk, EαkEβk) as well as those of the responder APC (AαbAβb) are equally capable of presenting virtually all insulin epitopes recognizable by T cells. The data, therefore, demonstrate that the selective recognition of different insulin epitopes observed in syngeneic or semisyngeneic T cell‐APC combinations does not result from determinant selection at the level of APC.
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U2 - 10.1002/eji.1830130810
DO - 10.1002/eji.1830130810
M3 - Article
C2 - 6193000
AN - SCOPUS:0020636587
SN - 0014-2980
VL - 13
SP - 658
EP - 662
JO - European Journal of Immunology
JF - European Journal of Immunology
IS - 8
ER -