Abstract |
There is compelling evidence that a unique innate immune response in the CNS plays a critical role in host defense and clearance of toxic cell debris. Although complement has been implicated in neuronal impairment, axonal loss, and demyelination, some preliminary evidence suggests that the initial insult consequently activates surrounding cells to signal neuroprotective activities. Using two different models of experimental autoimmune encephalomyelitis, we herein demonstrate selective C1q complement activation on neuron cell bodies and axons. Interestingly, in brains with chronic but not acute experimental autoimmune encephalomyelitis, C3b opsonization of neuronal cell bodies and axons was consistently associated with robust neuronal expression of one of the most effective complement regulators, decay-accelerating factor (CD55). In contrast, levels of other complement inhibitors, complement receptor 1 (CD35), membrane cofactor protein (CD46), and CD59 were largely unaffected on neurons and reactive glial cells in both conditions. In vitro, we found that proinflammatory stimuli ( cytokines and sublytic doses of complement) failed to up-regulate CD55 expression on cultured IMR32 neuronal cells. Interestingly, overexpression of GPI-anchored CD55 on IMR32 was capable of modulating raft-associated protein kinase activities without affecting MAPK activities and neuronal apoptosis. Critically, ectopic expression of decay-accelerating factor conferred strong protection of neurons against complement attack (opsonization and lysis). We conclude that increased CD55 expression by neurons may represent a key protective signaling mechanism mobilized by brain cells to withstand complement activation and to survive within an inflammatory site.
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Authors | Johan van Beek, Marjan van Meurs, Bert A 't Hart, Herbert P M Brok, Jim W Neal, Alexandra Chatagner, Claire L Harris, Nader Omidvar, B Paul Morgan, Jon D Laman, Philippe Gasque |
Journal | Journal of immunology (Baltimore, Md. : 1950)
(J Immunol)
Vol. 174
Issue 4
Pg. 2353-65
(Feb 15 2005)
ISSN: 0022-1767 [Print] United States |
PMID | 15699172
(Publication Type: Comparative Study, Journal Article, Research Support, Non-U.S. Gov't)
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Chemical References |
- Antigens, CD
- CD46 protein, human
- CD55 Antigens
- CD59 Antigens
- Glycosylphosphatidylinositols
- Membrane Cofactor Protein
- Membrane Glycoproteins
- Opsonin Proteins
- Receptors, Complement 3b
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Topics |
- Acute Disease
- Animals
- Antigens, CD
(biosynthesis)
- Apoptosis
(immunology)
- Axons
(immunology, metabolism, pathology)
- Brain
(immunology, metabolism, pathology)
- CD55 Antigens
(biosynthesis, physiology)
- CD59 Antigens
(biosynthesis)
- Callithrix
- Cell Line
- Cell Line, Tumor
- Cell Movement
(immunology)
- Chronic Disease
- Complement Hemolytic Activity Assay
- Complement Pathway, Classical
(immunology)
- Encephalomyelitis, Autoimmune, Experimental
(immunology, pathology)
- Glycosylphosphatidylinositols
(physiology)
- Humans
- K562 Cells
- Macaca fascicularis
- Membrane Cofactor Protein
- Membrane Glycoproteins
(biosynthesis)
- Membrane Microdomains
(immunology, metabolism)
- Neurons
(immunology, metabolism, pathology)
- Opsonin Proteins
(metabolism)
- Receptors, Complement 3b
(biosynthesis)
- Signal Transduction
(immunology)
- U937 Cells
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