Department of Neurochemistry, Stockholm University, SE-10691 Stockholm, Sweden.
J Neuroinflammation. 2011 Apr 14;8:34. doi: 10.1186/1742-2094-8-34.
The transcription factors CCAAT/enhancer binding proteins (C/EBP) α, β and δ have been shown to be expressed in brain and to be involved in regulation of inflammatory genes in concert with nuclear factor κB (NF-κB). In general, C/EBPα is down-regulated, whereas both C/EBPβ and δ are up-regulated in response to inflammatory stimuli. In Alzheimer's disease (AD) one of the hallmarks is chronic neuroinflammation mediated by astrocytes and microglial cells, most likely induced by the formation of amyloid-β (Aβ) deposits. The inflammatory response in AD has been ascribed both beneficial and detrimental roles. It is therefore important to delineate the inflammatory mediators and signaling pathways affected by Aβ deposits with the aim of defining new therapeutic targets.
Here we have investigated the effects of Aβ on expression of C/EBP family members with a focus on C/EBPδ in rat primary astro-microglial cultures and in a transgenic mouse model with high levels of fibrillar Aβ deposits (tg-ArcSwe) by western blot analysis. Effects on DNA binding activity were analyzed by electrophoretic mobility shift assay. Cross-talk between C/EBPδ and NF-κB was investigated by analyzing binding to a κB site using a biotin streptavidin-agarose pull-down assay.
We show that exposure to fibril-enriched, but not oligomer-enriched, preparations of Aβ inhibit up-regulation of C/EBPδ expression in interleukin-1β-activated glial cultures. Furthermore, we observed that, in aged transgenic mice, C/EBPα was significantly down-regulated and C/EBPβ was significantly up-regulated. C/EBPδ, on the other hand, was selectively down-regulated in the forebrain, a part of the brain showing high levels of fibrillar Aβ deposits. In contrast, no difference in expression levels of C/EBPδ between wild type and transgenic mice was detected in the relatively spared hindbrain. Finally, we show that interleukin-1β-induced C/EBPδ DNA binding activity to both C/EBP and κB sites is abolished after exposure to Aβ.
These data suggest that both expression and function of C/EBPδ are dysregulated in Alzheimer's disease. C/EBPδ seems to be differently regulated in response to different conformations of Aβ. We propose that Aβ induces an imbalance between NF-κB and C/EBP transcription factors that may result in abnormal responses to inflammatory stimuli.
转录因子 CCAAT/增强子结合蛋白(C/EBP)α、β 和 δ 已被证明在大脑中表达,并与核因子 κB(NF-κB)一起参与调节炎症基因。一般来说,C/EBPα 被下调,而 C/EBPβ 和 δ 则被上调以响应炎症刺激。在阿尔茨海默病(AD)中,一个标志是由星形胶质细胞和小胶质细胞介导的慢性神经炎症,很可能是由淀粉样β(Aβ)沉积的形成引起的。AD 中的炎症反应被归因于有益和有害的作用。因此,重要的是要描绘受 Aβ 沉积影响的炎症介质和信号通路,以确定新的治疗靶点。
在这里,我们通过 Western blot 分析研究了 Aβ 对大鼠原代星形胶质细胞-小胶质细胞培养物中 C/EBP 家族成员(特别是 C/EBPδ)表达的影响,以及在具有高纤维状 Aβ 沉积的转基因小鼠模型(tg-ArcSwe)中的影响。通过电泳迁移率变动分析分析 DNA 结合活性的影响。通过生物素链霉亲和素琼脂糖下拉测定分析 κB 位点的结合来研究 C/EBPδ 和 NF-κB 之间的串扰。
我们表明,暴露于富含纤维但不富含寡聚体的 Aβ 制剂可抑制白细胞介素-1β 激活的神经胶质细胞培养物中 C/EBPδ 表达的上调。此外,我们观察到,在老年转基因小鼠中,C/EBPα 明显下调,C/EBPβ 明显上调。另一方面,C/EBPδ 在大脑前脑选择性下调,前脑是显示高水平纤维状 Aβ 沉积的大脑部分。相反,在相对保留的后脑中,未检测到野生型和转基因小鼠之间 C/EBPδ 表达水平的差异。最后,我们表明,暴露于 Aβ 后,白细胞介素-1β 诱导的 C/EBPδ 对 C/EBP 和 κB 位点的 DNA 结合活性被消除。
这些数据表明,C/EBPδ 在阿尔茨海默病中的表达和功能均失调。C/EBPδ 似乎对不同构象的 Aβ 的反应不同。我们提出,Aβ 诱导 NF-κB 和 C/EBP 转录因子之间的不平衡,可能导致对炎症刺激的异常反应。
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