Journal
MOLECULAR IMMUNOLOGY
Volume 45, Issue 13, Pages 3649-3660Publisher
PERGAMON-ELSEVIER SCIENCE LTD
DOI: 10.1016/j.molimm.2008.04.025
Keywords
complement; dementia; apoptosis; C4BP
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Funding
- Foundations of Tore Nilsson
- Royal Physiographic Society in Lund
- wedish Foundation for Strategic Research (INGVAR)
- Foundations of Kock, Osterlund
- King Gustav V's
- US Immunodeficiency Network
- Cancerfonden
- University Hospital in Malmo
- Swedish Research Council
- lzheimer's Foundation
- Queen Victoria Foundations
- Stichting Dioraphte
- ISAO [03509]
- Wenner-Gren
- nna-Greta Crafoord
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the Alzheimer's disease (AD) brain, binding of C1q within the C1 complex, the initiating molecule of the classical complement pathway, to apoptotic cells, DNA and amyloid-beta (A beta), the major constituent of senile plaques, can initiate complement activation. However, the extent of activation is determined by the balance between activation and inhibition. Fluid-phase complement inhibitor C4b-binding protein (C4BP) was immunohistochemically detected in A beta plaques and on apoptotic cells in AD brain. In vitro, C4BP bound apoptotic and necrotic but not viable brain cells (astrocytes, neurons and oligodendrocytes) and limited complement activation on dead brain cells. C4BP also bound A beta(1-42) peptide directly, via the C4BP a-chain, and limited the extent of complement activation by A beta. C4BP levels in cerebrospinal fluid (CSF) of dementia patients and controls were low compared to levels in plasma and correlated with CSF levels of other inflammation-related factors. In conclusion, C4BP binds to dead brain cells and A beta peptide in vitro, is present in CSF and possibly protects against excessive complement activation in AD brains. (C) 2008 Elsevier Ltd. All rights reserved.
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