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质子泵抑制剂兰索拉唑是核肝脏 X 受体激动剂。

Proton pump inhibitor lansoprazole is a nuclear liver X receptor agonist.

机构信息

Department of Environmental and Occupational Health, University of Pittsburgh, Pittsburgh, PA 15219, USA.

出版信息

Biochem Pharmacol. 2010 May 1;79(9):1310-6. doi: 10.1016/j.bcp.2009.12.018. Epub 2010 Jan 8.

Abstract

The liver X receptors (LXRalpha and LXRbeta) are transcription factors that control the expression of genes primarily involved in cholesterol metabolism. In the brain, in addition to normal neuronal function, cholesterol metabolism is important for APP proteolytic cleavage, secretase activities, Abeta aggregation and clearance. Particularly significant in this respect is LXR mediated transcriptional control of APOE, which is the only proven risk factor for late onset Alzheimer's disease. Using a transactivation reporter assay for screening pharmacologically active compounds and off patent drugs we identified the proton pump inhibitor Lansoprazole as an LXR agonist. In secondary screens and counter-screening assays, it was confirmed that Lansoprazole directly activates LXR, increases the expression of LXR target genes in brain-derived human cell lines, and increases Abca1 and Apo-E protein levels in primary astrocytes derived from wild type but not LXRalpha/beta double knockout mice. Other PPIs activate LXR as well, but the efficiency of activation depends on their structural similarities to Lansoprazole. The identification of a widely used drug with LXR agonist-like activity opens the possibility for systematic preclinical testing in at least two diseases--Alzheimer's disease and atherosclerosis.

摘要

肝 X 受体(LXRα 和 LXRβ)是转录因子,主要控制参与胆固醇代谢的基因的表达。在大脑中,除了正常的神经元功能外,胆固醇代谢对于 APP 的蛋白水解、分泌酶活性、Abeta 的聚集和清除也很重要。在这方面特别重要的是 LXR 介导的 APOE 的转录控制,APOE 是唯一被证实的晚发性阿尔茨海默病的风险因素。我们使用一种用于筛选具有药理活性的化合物和非专利药物的转激活报告基因检测法,鉴定出质子泵抑制剂兰索拉唑是一种 LXR 激动剂。在次级筛选和反向筛选实验中,确认兰索拉唑直接激活 LXR,增加脑源性人细胞系中 LXR 靶基因的表达,并增加源自野生型而非 LXRα/β 双敲除小鼠的原代星形胶质细胞中的 Abca1 和 Apo-E 蛋白水平。其他的质子泵抑制剂也能激活 LXR,但激活的效率取决于它们与兰索拉唑的结构相似性。具有 LXR 激动剂样活性的广泛使用药物的鉴定为至少两种疾病——阿尔茨海默病和动脉粥样硬化——的系统临床前测试提供了可能性。

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