Phenotype of the accessory cell necessary for mitogen-stimulated T and B cell responses in human peripheral blood: delineation by its sensitivity to the lysosomotropic agent, L-leucine methyl ester.
Open Access
- 1 November 1983
- journal article
- research article
- Published by The American Association of Immunologists in The Journal of Immunology
- Vol. 131 (5), 2282-2290
- https://doi.org/10.4049/jimmunol.131.5.2282
Abstract
The lysosomotropic compound L-leucine methyl ester (Leu-OMe) was utilized to delineate the phenotype of the accessory cells involved in human B and T cell activation in vitro. Leu-OMe was shown to cause lysosomal disruption and selective death of human monocytes (M phi). After 30-45 minute incubations with this agent, human peripheral blood mononuclear cells (PBM) were nearly completely depleted of M phi. Associated with this M phi depletion, PBM were rendered unresponsive to a variety of T and B cell mitogens including the plant lectins phytohemagglutinin, concanavalin A, and pokeweed mitogen as well as the oxidative mitogens sodium periodate and neuraminidase plus galactose oxidase. Leu-OMe mediated loss of responsiveness was the result of a selective loss of an accessory cell necessary for each of these responses since reconstitution was accomplished by the addition of a M phi-enriched adherent cell population. While intact adherent cells could reconstitute responsiveness, crude M phi supernatants or highly purified human IL 1 alone were ineffective. Further identification of the Leu-OMe sensitive accessory cell indicated that it was entirely contained within the fraction of the adherent population identified by the monoclonal anti-M phi antibody, 63D3. The mechanism by which Leu-OMe Killed M phi was dependent on the lysosomal content of these cells, since agents that altered lysosomal enzyme activity such as chloroquine or NH4Cl protected M phi from Leu-OMe. Thus, the selective killing of M phi by Leu-OMe appeared to relate to the characteristically rich endowment of lysosomes within these cells. These results support the conclusion that a lysosome-rich, leucine methyl ester-sensitive, intact M phi identified by the monoclonal anti-M phi antibody 63D3 is the circulating accessory cell required for mitogen-triggered human B and T cell activation.This publication has 21 references indexed in Scilit:
- Cross-reaction of a rat-anti-mouse phagocyte-specific monoclonal antibody (anti-Mac-1) with human monocytes and natural killer cells.The Journal of Immunology, 1981
- Initial characterization of monoclonal antibodies against human monocytes.Proceedings of the National Academy of Sciences, 1980
- Dendritic cells are accessory cells for the development of anti-trinitrophenyl cytotoxic T lymphocytes.The Journal of Experimental Medicine, 1980
- Gold‐induced changes in the morphology and functional capabilities of human monocytesArthritis & Rheumatism, 1979
- Accumulation of amino acids by lysosomes incubated with amino acid methyl esters.Journal of Biological Chemistry, 1979
- Monocyte Dependence of Pokeweed Mitogen-Induced Differentiation of Immunoglobulin-Secreting Cells from Human Peripheral Blood Mononuclear CellsThe Journal of Immunology, 1979
- Fluorescence probe measurement of the intralysosomal pH in living cells and the perturbation of pH by various agents.Proceedings of the National Academy of Sciences, 1978
- Circulating and Mitogen-Induced Immunoglobulin-Secreting Cells in Human Peripheral Blood: Evaluation by a Modified Reverse Hemolytic Plaque AssayThe Journal of Immunology, 1977
- Natural Cytotoxic Reactivity of Human Lymphocytes Against a Myeloid Cell Line: Characterization of Effector CellsThe Journal of Immunology, 1977
- Temporary Inhibition of Antibody-Dependent, Cell-Mediated Cytotoxicity by Pretreatment of Human Attacking Cells with Ammonium ChlorideThe Journal of Immunology, 1976