Up‐regulation of the α‐secretase ADAM10 by retinoic acid receptors and acitretin

ADAM10型 维甲酸 阿维A 视黄醇X受体 维甲酸 内分泌学 化学 内科学 受体 视黄醇X受体α 贝沙罗汀 生物 药理学 生物化学 医学 免疫学 银屑病 核受体 基因 金属蛋白酶 去整合素 转录因子
作者
Frank Tippmann,Jana Hundt,Anja Schneider,Kristina Endres,Falk Fahrenholz
出处
期刊:The FASEB Journal [Wiley]
卷期号:23 (6): 1643-1654 被引量:209
标识
DOI:10.1096/fj.08-121392
摘要

Late-onset Alzheimer's disease is often connected with nutritional misbalance, such as enhanced cholesterol intake, deficiency in polyunsaturated fatty acids, or hypovitaminosis. The alpha-secretase ADAM10 has been found to be regulated by retinoic acid, the bioreactive metabolite of vitamin A. Here we show that retinoids induce gene expression of ADAM10 and alpha-secretase activity by nonpermissive retinoid acid receptor/retinoid X receptor (RAR/RXR) heterodimers, whereby alpha- and beta-isotypes of RAR play a major role. However, ligands of other RXR binding partners, such as the vitamin D receptor, do not stimulate alpha-secretase activity. On the basis of these findings, we examined the effect of synthetic retinoids and found a strong enhancement of nonamyloidogenic processing of the amyloid precursor protein by the vitamin A analog acitretin: it stimulated ADAM10 promoter activity with an EC(50) of 1.5 microM and led to an increase of mature ADAM10 protein that resulted in a two- to three-fold increase of the ratio between alpha- and beta-secretase activity in neuroblastoma cells. The alpha-secretase stimulation by acitretin was completely inhibited by the ADAM10-specific inhibitor GI254023X. Intracerebral injection of acitretin in APP/PS1-21 transgenic mice led to a reduction of Abeta(40) and Abeta(42). The results of this study may have clinical relevance because acitretin has been approved for the treatment of psoriasis since 1997 and found generally safe for long-term use in humans.
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