Myelin ingestion alters macrophage antigen-presenting function in vitro and in vivo.
Publication year
2011Source
Journal of Leukocyte Biology, 90, 1, (2011), pp. 123-32ISSN
Annotation
01 juli 2011
Publication type
Article / Letter to editor
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Organization
Laboratory of Clinical Chemistry
Journal title
Journal of Leukocyte Biology
Volume
vol. 90
Issue
iss. 1
Page start
p. 123
Page end
p. 32
Subject
IGMD 6: Hormonal regulation; N4i 4: Auto-immunity, transplantation and immunotherapy; Laboratory Medicine - Radboud University Medical CenterAbstract
During MS, phagocytosing myelin-containing macrophages arise and lie in close proximity to T cells. To date, it has not been addressed whether these myelin-laden macrophages have the capacity to present antigens to T cells and whether this contributes to inflammation in disease. We demonstrate that in vitro-generated human and mouse myelin-laden macrophages expressed MHC class I and II and costimulatory molecules and are thus well equipped for antigen presentation. Human myelin-laden macrophages exhibited normal endocytosis of particulate and soluble antigens. In addition, human myelin-laden macrophages elicited active T cell proliferation of naive as well as memory T cells. Furthermore, mouse myelin-laden macrophages induced primary antigen-specific CD4(+) T cell proliferation in vivo but transiently diminished IFN-gamma release. Functionally, MOG peptide-loaded myelin-laden mouse macrophages modestly but significantly reduced the severity of MOG peptide-induced EAE. These data show that myelin uptake results in the induction of a population of macrophages that retains antigen-presenting capacity and limits autoimmune-mediated disease.
This item appears in the following Collection(s)
- Academic publications [246625]
- Faculty of Medical Sciences [93367]
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