Macrophage‐T cell interaction in experimental visceral leishmaniasis: failure to express costimulatory molecules on Leishmania‐infected macrophages and its implication in the suppression of cell‐mediated immunity
- 1 September 1995
- journal article
- research article
- Published by Wiley in European Journal of Immunology
- Vol. 25 (9), 2492-2498
- https://doi.org/10.1002/eji.1830250913
Abstract
The most important immunopathological consequence of infection with Leishmania seen in murine and human hosts is the suppression of T cell-mediated immune responses to both mitogens and leishmanial antigens. It has been suggested that this suppression is mediated by macrophages, either by defective antigen processing and presentation or by the elaboration of suppressive mediators like prostaglandins. Optimum activation of T helper cells requires not only T cell receptor occupancy by the antigen-Ia complex, but also costimulatory signals provided by the antigen-presenting cells. We investigated the status of several costimulatory molecules on infected macrophages from both genetically susceptible BALB/c and resistant C57BL/6 mice. Our results demonstrate that upon parasitization, the macrophages become unable to deliver costimulatory signals to T helper cells, and that this effects is mediated by prostaglandins, as the inhibition of its synthesis by indomethacin recovered the defect. Upon infection with L. donovani, B7-1 expression was decreased, while ICAM-1 was marginally increased in BALB/c macrophages and there was no significant change in the expression of B7-1 and ICAM-1 in Leishmania-infected C57BL/6 macrophages. Expression of VCAM-1 did not change during infection. This selective alteration in the expression of costimulatory molecules on L. donovani-infected BALB/c macrophages was caused by the living parasite, as shown by the fact that killing of the parasites by stibogluconate led to no alteration in the levels of costimulatory molecules. We found that the change in B7-1 expression on the surface of infected macrophages resulted in the inhibition of delayed-type hypersensitivity-mediating functions of T helper cells from BALB/c mice. The results described in this study not only throw light on the possible mechanism of leishmanial pathogenesis, but also open up the possibility of immunotherapy of leishmaniasis by selective manipulation of costimulatory molecules.Keywords
This publication has 40 references indexed in Scilit:
- Deficient expression of co‐stimulatory molecules on Leishmania‐infected macrophagesEuropean Journal of Immunology, 1994
- Effect of macrophage infection by Leishmania on the proliferation of an antigen‐specific T‐cell line, TPB1, to a non‐parasite antigenParasite Immunology, 1993
- Immunobiological Studies on Experimental Visceral Leishmaniasis. III. Cytokine‐Mediated Regulation of Parasite ReplicationScandinavian Journal of Immunology, 1993
- Immunobiological studies on experimental visceral leishmaniasis. II. Adherent cell‐mediated down‐regulation of delayed‐type hypersensitivity response and up‐regulation of B cell activationEuropean Journal of Immunology, 1992
- Effect of sodium stibogluconate and pentamidine on in vitro multiplication of Leishmania donovani in peritoneal macrophages from infected and drug‐treated BALB/c miceImmunology & Cell Biology, 1992
- Immunobiological studies on experimental visceral leishmaniasis I. Changes in lymphoid organs and their possible role in pathogenesisEuropean Journal of Immunology, 1991
- Clonal Expansion Versus Functional Clonal Inactivation: A Costimulatory Signalling Pathway Determines the Outcome of T Cell Antigen Receptor OccupancyAnnual Review of Immunology, 1989
- Reciprocal expression of interferon gamma or interleukin 4 during the resolution or progression of murine leishmaniasis. Evidence for expansion of distinct helper T cell subsets.The Journal of Experimental Medicine, 1989
- Influence of H–2 complex on acquired resistance to Leishmania donovani infection in miceNature, 1980
- Suppression of human T-cell mitogenesis by prostaglandin. Existence of a prostaglandin-producing suppressor cell.The Journal of Experimental Medicine, 1977