胰岛素抵抗会导致动脉中脂蛋白残粒的滞留增加，这是由于动脉中 biglycan 的增加以及富含胆固醇的动脉粥样硬化颗粒的产生所致，而在 JCR:LA-cp 大鼠中，依折麦布可以改善这种情况。

Arterial retention of remnant lipoproteins ex vivo is increased in insulin resistance because of increased arterial biglycan and production of cholesterol-rich atherogenic particles that can be improved by ezetimibe in the JCR:LA-cp rat.

机构信息

Metabolic and Cardiovascular Diseases Laboratory, University of Alberta, Edmonton, Alberta, Canada.

出版信息

J Am Heart Assoc. 2012 Oct;1(5):e003434. doi: 10.1161/JAHA.112.003434. Epub 2012 Oct 25.

BACKGROUND

Literature supports the "response-to-retention" hypothesis-that during insulin resistance, impaired metabolism of remnant lipoproteins can contribute to accelerated cardiovascular disease progression. We used the JCR:LA-cp rat model of metabolic syndrome (MetS) to determine the extent of arterial accumulation of intestinal-derived remnants ex vivo and potential mechanisms that contribute to exacerbated cholesterol deposition in insulin resistance.

METHODS AND RESULTS

Arteries from control and MetS (insulin-resistant) JCR:LA-cp rats were perfused ex vivo with Cy5-labeled remnant lipoproteins, and their arterial retention was quantified by confocal microscopy. Arterial proteoglycans were isolated from control and MetS rats at 6, 12, and 32 weeks of age. There was a significant increase in the arterial retention of remnants and in associated cholesterol accumulation in MetS rats as compared to control rats. Mechanistic studies reveal that increased cholesterol deposition is a result of greater arterial biglycan content; longer glycosaminoglycans and increased production of cholesterol-rich intestinal-derived remnants, as compared to controls. Additionally, perfusion of vessels treated with ezetimibe, alone or in combination with simvastatin, with remnants isolated from the respective treatment group reduced ex vivo arterial retention of remnant-derived cholesterol ex vivo as compared to untreated controls.

CONCLUSIONS

Increased progression of atherosclerotic cardiovascular disease in MetS and type 2 diabetes mellitus might be explained in part by an increase in the arterial retention of cholesterol-rich remnants. Furthermore, ezetimibe alone or in combination treatment with simvastatin could be beneficial in ameliorating atherosclerotic cardiovascular disease in insulin resistance and MetS.

背景

文献支持“应答-滞留”假说，即在胰岛素抵抗时，残脂蛋白代谢受损可能导致心血管疾病进展加速。我们使用 JCR:LA-cp 代谢综合征（MetS）大鼠模型，来确定残余脂蛋白在动脉中的积累程度以及促进胰岛素抵抗时胆固醇沉积加剧的潜在机制。

方法和结果

用 Cy5 标记的残余脂蛋白对来自对照和 MetS（胰岛素抵抗）JCR:LA-cp 大鼠的动脉进行离体灌注，并通过共聚焦显微镜定量其动脉滞留率。在 6、12 和 32 周龄时，从对照和 MetS 大鼠中分离动脉蛋白聚糖。与对照组相比，MetS 大鼠的残余物动脉滞留和相关胆固醇积累显著增加。机制研究表明，胆固醇沉积增加是由于动脉中大聚糖含量增加；与对照组相比，糖胺聚糖更长，富含胆固醇的肠源性残余物的产生增加。此外，与未处理的对照组相比，用依折麦布单独或与辛伐他汀联合处理的血管进行残余物灌注，可减少离体残余衍生胆固醇的动脉滞留。