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培养的ARPE-19细胞分泌载脂蛋白B100受胆固醇水平变化的调节。

Apolipoprotein B100 secretion by cultured ARPE-19 cells is modulated by alteration of cholesterol levels.

作者信息

Wu Tinghuai, Fujihara Masashi, Tian Jane, Jovanovic Miroslava, Grayson Celene, Cano Marisol, Gehlbach Peter, Margaron Philippe, Handa James T

机构信息

Wilmer Eye Institute, Johns Hopkins School of Medicine, Baltimore, Maryland, USA.

出版信息

J Neurochem. 2010 Sep;114(6):1734-44. doi: 10.1111/j.1471-4159.2010.06884.x. Epub 2010 Jul 27.

Abstract

Cholesteryl ester rich apolipoprotein B100 (apoB100) lipoproteins accumulate in Bruch's membrane before the development of age-related macular degeneration. It is not known if these lipoproteins come from the circulation or local ocular tissue. Emerging, but incomplete evidence suggests that the retinal pigmented epithelium (RPE) can secrete lipoproteins. The purpose of this investigation was to determine (i) whether human RPE cells synthesize and secrete apoB100, and (ii) whether this secretion is driven by cellular cholesterol, and if so, (iii) whether statins inhibit this response. The established, human derived ARPE-19 cells challenged with 0-0.8 mM oleic acid accumulated cellular cholesterol, but not triglycerides. Oleic acid increased the amount of apoB100 protein recovered from the medium by both western blot analysis and (35) S-radiolabeled immunoprecipitation while negative stain electron microscopy showed lipoprotein-like particles. Of nine statins evaluated, lipophilic statins induced HMG-CoA reductase mRNA expression the most. The lipophilic Cerivastatin (5 μM) reduced cellular cholesterol by 39% and abrogated apoB100 secretion by 3-fold. In contrast, the hydrophilic statin Pravastatin had minimal effect on apoB100 secretion. These data suggest that ARPE-19 cells synthesize and secrete apoB100 lipoproteins, that this secretion is driven by cellular cholesterol, and that statins can inhibit apoB100 secretion by reducing cellular cholesterol.

摘要

富含胆固醇酯的载脂蛋白B100(apoB100)脂蛋白在年龄相关性黄斑变性发生之前就积聚在布鲁赫膜中。目前尚不清楚这些脂蛋白是来自循环系统还是局部眼组织。新出现但尚不完整的证据表明,视网膜色素上皮(RPE)可以分泌脂蛋白。本研究的目的是确定:(i)人RPE细胞是否合成并分泌apoB100;(ii)这种分泌是否由细胞胆固醇驱动,如果是,(iii)他汀类药物是否抑制这种反应。用0 - 0.8 mM油酸刺激已建立的人源ARPE - 19细胞,细胞内胆固醇会积聚,但甘油三酯不会。通过蛋白质免疫印迹分析和(35)S - 放射性标记免疫沉淀法发现,油酸增加了从培养基中回收的apoB100蛋白的量,而负染电子显微镜显示有脂蛋白样颗粒。在所评估的9种他汀类药物中,亲脂性他汀类药物对HMG - CoA还原酶mRNA表达的诱导作用最强。亲脂性的西立伐他汀(5 μM)使细胞胆固醇降低了39%,并使apoB100分泌减少了3倍。相比之下,亲水性他汀类药物普伐他汀对apoB100分泌的影响最小。这些数据表明,ARPE - 19细胞合成并分泌apoB100脂蛋白,这种分泌由细胞胆固醇驱动,并且他汀类药物可以通过降低细胞胆固醇来抑制apoB100分泌。

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