Several combinations of F1 hybrid mice were injected intravenously with parental spleen cells to determine the minimal H-2 differences between F1 and parent that are necessary to induce graft-vs.-host-associated immune suppression (GVH-associated suppression). 7-14 d after injection, the spleens of the F1 mice were tested for cytotoxic T lymphocyte potential by in vitro sensitization against trinitrophenyl-self and H-2 alloantigens. The results indicate that parental T lymphocytes must recognize I-A allogeneic determinants of the F1 recipient in order to induce suppression. Recognition of K or D alone or D with I region products other than I-A did not induce suppression. The recognition of I region without K and/or D and even the I-A difference between C57BL/6 and the B6.Cbm12 mutation resulted in immune suppression that was as potent as that resulting from the recognition of K, D, and I together. The possible significance of this function for I-A antigens is discussed with respect to three clinical examples of immune suppression for which this phenomenon may be relevant.
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1 March 1983
Article|
March 01 1983
Graft-vs.-host-associated immune suppression is activated by recognition of allogeneic murine I-A antigens.
G M Shearer
R B Levy
Online ISSN: 1540-9538
Print ISSN: 0022-1007
J Exp Med (1983) 157 (3): 936–946.
Citation
G M Shearer, R B Levy; Graft-vs.-host-associated immune suppression is activated by recognition of allogeneic murine I-A antigens.. J Exp Med 1 March 1983; 157 (3): 936–946. doi: https://doi.org/10.1084/jem.157.3.936
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