依折替贝和辛伐他汀可以降低高胆固醇饲料喂养的斑马鱼幼虫的胆固醇水平。

Cholesterol Pub Date : 2012-01-01 DOI:10.1155/2012/564705
Ji Sun Baek, Longhou Fang, Andrew C Li, Yury I Miller
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引用次数: 39

摘要

胆固醇喂养的斑马鱼是一种新兴的动物模型,用于研究与人类动脉粥样硬化发病相关的代谢、氧化和炎症血管过程。饲喂高胆固醇饲料(HCD)的斑马鱼会出现高胆固醇血症,其特征是脂蛋白氧化和血管脂质积累。利用光学半透明的斑马鱼幼虫具有监测血管病理和评估活体候选药物疗效的优点。因此,我们研究了用于治疗人类高胆固醇血症的主要药物辛伐他汀和依zetimibe是否也会降低hcd喂养的斑马鱼幼虫的胆固醇水平。我们发现依zetimibe对斑马鱼有良好的耐受性,并有效降低了hcd喂养的幼虫的胆固醇水平。相比之下,将辛伐他汀添加到水中对斑马鱼幼虫的耐受性很差,当添加到食物中时,对hcd喂养的幼虫的胆固醇水平几乎没有影响。低剂量依折麦比和辛伐他汀联合使用对降低斑马鱼体内的胆固醇水平有叠加效应。这些结果表明依折替贝在斑马鱼中发挥的治疗作用与在人类中相似,高胆固醇斑马鱼可以作为一种低成本和信息丰富的模型,用于测试新的候选药物和研究针对血脂异常的现有药物的作用机制。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Ezetimibe and simvastatin reduce cholesterol levels in zebrafish larvae fed a high-cholesterol diet.

Cholesterol-fed zebrafish is an emerging animal model to study metabolic, oxidative, and inflammatory vascular processes relevant to pathogenesis of human atherosclerosis. Zebrafish fed a high-cholesterol diet (HCD) develop hypercholesterolemia and are characterized by profound lipoprotein oxidation and vascular lipid accumulation. Using optically translucent zebrafish larvae has the advantage of monitoring vascular pathology and assessing the efficacy of drug candidates in live animals. Thus, we investigated whether simvastatin and ezetimibe, the principal drugs used in management of hypercholesterolemia in humans, would also reduce cholesterol levels in HCD-fed zebrafish larvae. We found that ezetimibe was well tolerated by zebrafish and effectively reduced cholesterol levels in HCD-fed larvae. In contrast, simvastatin added to water was poorly tolerated by zebrafish larvae and, when added to food, had little effect on cholesterol levels in HCD-fed larvae. Combination of low doses of ezetimibe and simvastatin had an additive effect in reducing cholesterol levels in zebrafish. These results suggest that ezetimibe exerts in zebrafish a therapeutic effect similar to that in humans and that the hypercholesterolemic zebrafish can be used as a low-cost and informative model for testing new drug candidates and for investigating mechanisms of action for existing drugs targeting dyslipidemia.

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