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KMID : 0370220050490020147
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Yakhak Hoeji
2005 Volume.49 No. 2 p.147 ~ p.150
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Enhancement of Type A Macrophage Scavenger Receptor Expression by Ginsenoside Rg3 in Rat Microglia
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À̼øÇö/Lee SH
ÀÌÁÖÈñ/ÇÑ¿ë¹®/Lee JH/Han YM
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Abstract
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Macrophage scavenger receptors (MSRs) induce microglial interaction with ¥â-amyloid fibrils (fA¥â) that are associated with Alzheimer¡¯s disease (AD). Although microglia are known to have a dual effect on formation of plaque and clearance of fA¥â in the AD brain, receptor-mediated phagocytosis is a very important tool for preventing amyloid plaque via activated microglia in the early stage of AD. In the study, we examined whether ginsonoside Rg3 enhances the microglial Phagocytosis of A¥â1-42 through Phagocytosis assay, gene expression (RT-PCR) and protein assay (western blots) for the cell responsiveness presented between Rg3-treated and non-treated groups. Fluro-labeled Ac-LDL and E.coli particles were used as control proteins for phagocytosis. In previous studies, this was a particularly interesting property of Rg3 in the stimulation and phagocytosis of macrophages in the periphery. We report here that ginsenoside Rg3 increased the expression of type-A MSR (MSR-A) in microglia and thus accelerated the phagocytosis with an effective degradation of engulfed fA¥â. This result suggests that Rg3 may play an important role in removing fA¥â by enhancing the receptor-mediated phagocytosis. In addition, Rg3 could be a potential candidate for balancing the rate of production of fA¥â in AD brain.
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