Pharmacology of the ACAT inhibitor avasimibe (CI-1011).

G. Llaverías, J. Laguna, M. Alegret
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引用次数: 70

Abstract

Avasimibe is a novel orally bioavailable ACAT inhibitor, currently under clinical development (phase III trials). It was safe when administered to rats, dogs, and humans. In vitro studies in human macrophages demonstrated that avasimibe reduces foam cell formation not only by enhancing free cholesterol efflux, but also by inhibiting the uptake of modified LDL. The concentration-dependent reduction in cellular cholesteryl ester content in these cells was not accompanied by an increase in intracellular free cholesterol, which is in agreement with a good safety profile for avasimibe. In the liver, avasimibe caused a significant reduction in the secretion of apo B and apo B-containing lipoproteins into plasma. Avasimibe induced cholesterol 7alpha-hydroxylase and increased bile acid synthesis in cultured rat hepatocytes, and its administration to rats did not produce an increase in lithogenicity index of the bile. The hypolipidemic efficacy of the compound was demonstrated in cholesterol-fed as well as in non-cholesterol-fed animals. In these models, plasma cholesterol levels were reduced, mainly due to the decrease in the non-HDL cholesterol fraction. Clinical data are scarce, but in a study performed in 130 men and women with combined hyperlipidemia and hypoalphalipoproteinemia, avasimibe, 50-500 mg/day, significantly reduced plasma total triglyceride and VLDL-cholesterol. Although total cholesterol, LDL-cholesterol, and HDL-cholesterol were unchanged, it must be stressed that animal data suggest that avasimibe may have direct antiatherosclerotic activity in addition to its cholesterol-lowering effect. Avasimibe treatment can also contribute to increase plaque stability, as it reduces the accumulation of lipids in the arterial wall, inhibits macrophage infiltration into the media and reduces matrix metalloproteinase expression and activity. Moreover, avasimibe and statins have been shown to have synergistic effects, and the combination therapy may not only inhibit atherosclerotic lesion progression but also induce lesion regression, independently of changes in plasma cholesterol.
ACAT抑制剂avasimibe (CI-1011)的药理学。
Avasimibe是一种新型口服ACAT抑制剂,目前正处于临床开发阶段(III期试验)。它在老鼠、狗和人类身上都是安全的。在人巨噬细胞中的体外研究表明,avasimibe不仅通过增强游离胆固醇外排,而且通过抑制修饰LDL的摄取来减少泡沫细胞的形成。在这些细胞中,细胞胆固醇酯含量的浓度依赖性降低没有伴随着细胞内游离胆固醇的增加,这与avasimibe良好的安全性一致。在肝脏中,阿瓦辛贝贝引起血浆中载脂蛋白B和含载脂蛋白B分泌的显著减少。阿瓦斯米贝诱导培养的大鼠肝细胞胆固醇7 - α -羟化酶和胆汁酸合成增加,给药大鼠未产生胆汁产石指数的增加。该化合物的降血脂功效在胆固醇喂养和非胆固醇喂养的动物中都得到了证明。在这些模型中,血浆胆固醇水平降低,主要是由于非高密度脂蛋白胆固醇含量降低。临床数据很少,但在一项对130名合并高脂血症和低脂蛋白血症的男性和女性进行的研究中,50-500 mg/天的阿瓦西米贝可显著降低血浆总甘油三酯和vldl -胆固醇。虽然总胆固醇、低密度脂蛋白胆固醇和高密度脂蛋白胆固醇没有变化,但必须强调的是,动物数据表明,阿瓦斯米贝除了具有降胆固醇作用外,还可能具有直接的抗动脉粥样硬化活性。Avasimibe治疗也有助于增加斑块的稳定性,因为它可以减少动脉壁脂质的积累,抑制巨噬细胞向介质的浸润,降低基质金属蛋白酶的表达和活性。此外,阿伐昔米贝和他汀类药物已被证明具有协同作用,联合治疗不仅可以抑制动脉粥样硬化病变进展,还可以诱导病变消退,而不依赖于血浆胆固醇的变化。
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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