Augmentation of macrophage complement receptor function in vitro. V. Studies on the mechanisms of ligation of macrophage Fc receptors required to trigger macrophages to signal T lymphocytes to elaborate the lymphokine that activates macrophage C3 receptors for phagocytosis

We previously described a unique lymphokine that activates macrophage C3 receptors for phagocytosis. The lymphokine is generated when T lymphocytes receive a signal from macrophages that have ingested IgG-coated material. In the present work, we examined the mechanisms by which macrophage Fc recepto...

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Bibliographic Details
Published inThe Journal of immunology (1950) Vol. 135; no. 1; pp. 344 - 349
Main Authors Griffin, FM, Jr, Mullinax, PJ
Format Journal Article
LanguageEnglish
Published Bethesda, MD Am Assoc Immnol 01.07.1985
American Association of Immunologists
Subjects
Analysis of the immune response. Humoral and cellular immunity
Animals
Antigen-Antibody Complex - physiology
Biological and medical sciences
Cell interactions
Female
Fundamental and applied biological sciences. Psychology
Fundamental immunology
Immunobiology
Lymphokines - biosynthesis
Macrophage Activation
Macrophage-1 Antigen
Macrophages - immunology
Macrophages - metabolism
Mice
Phagocytosis
Receptors, Complement - classification
Receptors, Complement - physiology
Receptors, Fc - classification
Receptors, Fc - physiology
T-Lymphocytes - immunology
T-Lymphocytes - metabolism
Vertebrata
Membrane receptor
Mammalia
Cell-cell interaction
Mouse
Complement C3
Rodentia
T-Lymphocyte
Activation
Lymphokine
Phagocytosis
Macrophage
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Summary:We previously described a unique lymphokine that activates macrophage C3 receptors for phagocytosis. The lymphokine is generated when T lymphocytes receive a signal from macrophages that have ingested IgG-coated material. In the present work, we examined the mechanisms by which macrophage Fc receptors must be engaged for macrophages to signal lymphocytes to elaborate the lymphokine. We found that ingestion mediated by any of the three classes of murine macrophage Fc receptors was sufficient to trigger macrophages, and that engagement of macrophage Fc receptors by immobilized immune complexes was effective as well. We also found that ligation of Fc receptors by an anti-Fc receptor IgG antibody or by its F(ab')2 or Fab fragments also triggered macrophages. The ability of monovalent ligation of the receptor to elicit biologic activity suggests that this system may be of value in elucidating general mechanisms by which ligand binding of receptors is transduced into biologic effects.
Bibliography:ObjectType-Article-1
SourceType-Scholarly Journals-1
ObjectType-Feature-2
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ISSN:0022-1767
1550-6606
DOI:10.4049/jimmunol.135.1.344