Microglial complement receptor 3 regulates brain Aβ levels through secreted proteolytic activity.
Eva CzirrNicholas A CastelloKira I MosherJoseph M CastellanoIzumi V HinksonKurt M LucinBernat Baeza-RajaJae Kyu RyuLulin LiSasha N FarinaNadia P BelichenkoFrank M LongoKaterina AkassoglouMarkus BritschgiJohn R CirritoTony Wyss-CorayPublished in: The Journal of experimental medicine (2017)
Recent genetic evidence supports a link between microglia and the complement system in Alzheimer's disease (AD). In this study, we uncovered a novel role for the microglial complement receptor 3 (CR3) in the regulation of soluble β-amyloid (Aβ) clearance independent of phagocytosis. Unexpectedly, ablation of CR3 in human amyloid precursor protein-transgenic mice results in decreased, rather than increased, Aβ accumulation. In line with these findings, cultured microglia lacking CR3 are more efficient than wild-type cells at degrading extracellular Aβ by secreting enzymatic factors, including tissue plasminogen activator. Furthermore, a small molecule modulator of CR3 reduces soluble Aβ levels and Aβ half-life in brain interstitial fluid (ISF), as measured by in vivo microdialysis. These results suggest that CR3 limits Aβ clearance from the ISF, illustrating a novel role for CR3 and microglia in brain Aβ metabolism and defining a potential new therapeutic target in AD.
Keyphrases
- inflammatory response
- small molecule
- neuropathic pain
- resting state
- white matter
- endothelial cells
- wild type
- functional connectivity
- lipopolysaccharide induced
- induced apoptosis
- multiple sclerosis
- binding protein
- protein protein
- hydrogen peroxide
- atrial fibrillation
- climate change
- subarachnoid hemorrhage
- mild cognitive impairment