Genetic analysis of immune suppression |
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Authors: | Barbara A. Araneo Judith A. Kapp |
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Affiliation: | (1) Department of Pathology and Laboratory Medicine, The Jewish Hospital of St. Louis, 63110 St. Louis, Missouri, USA;(2) Departments of Pathology and of Microbiology and Immunology, Washington University School of Medicine, 63110 St. Louis, Missouri |
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Abstract: | We have analyzed the genetic control of susceptibility to suppression by 1-J+, suppressor-T-cell derived factors (TsF) specific for the synthetic polymer L-glutamic acid50-L-tyrosine50 (GT). GT-TsF activity was measured as specific inhibition of proliferative responses to GT developed in cultures of lymph-node T cells from mice primed with GT complexed to methylated bovine serum albumin (GT-MBSA). These experiments demonstrated that there is no MHC-encoded genetic restriction between donors and recipients of GT-TsF in suppression of proliferative responses. We have also confirmed the observations that mice of the H-2b, H-2d, and H-2khaplotypes can produce GT-TsF, whereas H-2amice do not, and that H-2b, H-2d, and H-2kmice are sensitive to GT-TsF from all producer strains, whereas H-2bmice are not sensitive to GT-TsF from any strain. Analysis of the effect of GT-TsF on responses by mice bearing recombinant haplotypes suggests that at least two genes are required for susceptibility to GT-TsF and that these genes show coupled complementation.Abbreviations used in this paper GAT random linear terpolymer of L-glutamic acid60-L-alanine30-L-tyrosine10 - GAT-MBSA GAT complexed to methylated bovine serum albumin - GATTsF GAT-specific-T-cell derived suppressor factor - GT random linear copolymer of L-glutamic acid50-L-tyrosine50 - GT-MBSA GT complexed methylated bovine serum albumin - GT-TsF GT, specific, T-cell derived suppressor factor - 3H-TdR tritiated thymidine - Ir gene immune response gene - MBSA methylated bovine serum albumin - MEM minimal essential media - MHC major histocompatibility complex - PFC plaque-forming cell(s) - PPD purified protein derivative of M. tuberculosis H37Ra |
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