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由纤维状β-淀粉样蛋白和免疫球蛋白诱导的小胶质细胞吞噬作用受到促炎细胞因子的差异调节。

Microglial phagocytosis induced by fibrillar beta-amyloid and IgGs are differentially regulated by proinflammatory cytokines.

作者信息

Koenigsknecht-Talboo Jessica, Landreth Gary E

机构信息

Department of Neurosciences, Case Western Reserve University School of Medicine, Cleveland, Ohio 44106, USA.

出版信息

J Neurosci. 2005 Sep 7;25(36):8240-9. doi: 10.1523/JNEUROSCI.1808-05.2005.

DOI:10.1523/JNEUROSCI.1808-05.2005
PMID:16148231
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6725530/
Abstract

Microglia undergo a phenotypic activation in response to fibrillar beta-amyloid (fAbeta) deposition in the brains of Alzheimer's disease (AD) patients, resulting in their elaboration of inflammatory molecules. Despite the presence of abundant plaque-associated microglia in the brains of AD patients and in animal models of the disease, microglia fail to efficiently clear fAbeta deposits. However, they can be induced to do so during Abeta vaccination therapy attributable to anti-Abeta antibody stimulation of IgG receptor (FcR)-mediated phagocytic clearance of Abeta plaques. We report that proinflammatory cytokines attenuate microglial phagocytosis stimulated by fAbeta or complement receptor 3 and argue that this may, in part, underlie the accumulation of fAbeta-containing plaques within the AD brain. The proinflammatory suppression of fAbeta-elicited phagocytosis is dependent on nuclear factor kappaB activation. Significantly, the proinflammatory cytokines do not inhibit phagocytosis elicited by antibody-mediated activation of FcR, which may contribute to the efficiency of Abeta vaccination-based therapy. Importantly, the proinflammatory suppression of fAbeta phagocytosis can be relieved by the coincubation with anti-inflammatory cytokines, cyclooxygenase inhibitors, ibuprofen, or an E prostanoid receptor antagonist, suggesting that proinflammatory cytokines induce the production of prostaglandins, leading to an E prostanoid receptor-dependent inhibition of phagocytosis. These findings support anti-inflammatory therapies for the treatment of AD.

摘要

在阿尔茨海默病(AD)患者大脑中,小胶质细胞会因纤维状β-淀粉样蛋白(fAbeta)沉积而发生表型激活,进而产生炎症分子。尽管在AD患者大脑以及该疾病的动物模型中存在大量与斑块相关的小胶质细胞,但小胶质细胞无法有效清除fAbeta沉积物。然而,在β-淀粉样蛋白疫苗接种治疗期间,由于抗β-淀粉样蛋白抗体刺激IgG受体(FcR)介导的β-淀粉样蛋白斑块吞噬清除作用,可诱导小胶质细胞清除fAbeta沉积物。我们报告称,促炎细胞因子会减弱由fAbeta或补体受体3刺激的小胶质细胞吞噬作用,并认为这可能部分是AD大脑中含fAbeta斑块积累的原因。fAbeta引发的吞噬作用的促炎抑制依赖于核因子κB的激活。值得注意的是,促炎细胞因子不会抑制由抗体介导的FcR激活所引发的吞噬作用,这可能有助于基于β-淀粉样蛋白疫苗接种的治疗效果。重要的是,与抗炎细胞因子、环氧化酶抑制剂布洛芬或前列环素受体拮抗剂共同孵育可缓解fAbeta吞噬作用的促炎抑制,这表明促炎细胞因子会诱导前列腺素的产生,导致前列环素受体依赖性吞噬作用抑制。这些发现支持抗炎疗法用于治疗AD。

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