Publication | Open Access
Antibodies to membrane structures that distinguish suppressor/cytotoxic and helper T lymphocyte subpopulations block the mixed leukocyte reaction in man.
303
Citations
22
References
1981
Year
Clinical ImmunologyAdaptive Immune SystemImmunologyImmune RegulationImmunophenotypingImmunologic MechanismAntigen ProcessingImmune SystemImmunotherapyLymphocyte BiologyMixed Leukocyte ReactionAllergyAutoimmune DiseaseAutoimmunityHumoral ImmunityIgg1 Monoclonal AntibodyAntibody BiologyHuman TMajor SubsetsMedicine
Two major subsets of human T lymphocytes that are functionally analogous to the mouse Lyt-2+ and Lyt-2- subsets have been defined by their expression of two thymus-dependent membrane antigens, Leu-2 and Leu-3. Leu-2+,3- cells have suppressor/cytotoxic functions and Leu-2-,3+ cells have helper functions. These studies were designed to determine the effects of adding IgG1 monoclonal anti-Leu-2 and anti-Leu-3 antibodies to the mixed leukocyte reaction (MLR). At high concentrations, each antibody partially inhibited the proliferative response of unseparated T cells and abolished the response of the isolated subset having the appropriate phenotype. An IgG1 monoclonal antibody to HLA-A2 and an IgG2a antibody to Leu-1, a pan-T antigen, failed to inhibited the MLR. These results suggest that the Leu-2 and Leu-3 antigens may have a direct role in the mechanism whereby T cells recognize and respond to alloantigen.
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