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实验性高β脂蛋白血症及其新型降血脂药物的改善作用

Experimental hyper-beta-lipoproteinemia and its amelioration by a novel hypolipidemic agent.

作者信息

Kobayakawa T, Osuga K, Yasuda H

出版信息

Atherosclerosis. 1978 Jul;30(3):219-25. doi: 10.1016/0021-9150(78)90048-5.

Abstract

Experimental models for hyper-beta-lipoproteinemia were established in rats and the effects of certain hypolipidemic drugs were studied with these models. In the hyperlipemia induced in rats by feeding a high cholesterol diet, Y-9738 [ethyl 2(4-chlorophenyl)-5-ethoxy-4-oxazoleacetate] produced a dose-dependent reduction of serum cholesterol: such hypolipidemic activity was estimated to be about 7 times as great as that of clofibrate. On the other hand, clofibrate induced hepatomegaly at 100 mg/kg, whereas Y-9738 did not at this dosage, which is about 10 times the effective dose. Hyperlipemia induced by high cholesterol and thiouracil was characterized by increased beta-lipoprotein (heparin-calcium and disc electrophoresis). In this model, Y-9738 showed a dose-dependent lowering effect on beta-lipoprotein cholesterol with a marked decrease in the beta/alpha lipoprotein ratio. A tendency was noted for alpha-lipoprotein to be increased. In contrast, clofibrate exerted no effect on this hyper-beta-lipoproteinemia. These results suggest that the above models may be of value in exploring hyper-beta-lipoproteinemia and that Y-9738 may be more useful than clofibrate in the therapy of hyperlipemia.

摘要

在大鼠中建立了高β-脂蛋白血症的实验模型,并使用这些模型研究了某些降血脂药物的效果。在通过喂食高胆固醇饮食诱导大鼠产生的高脂血症中,Y-9738[2-(4-氯苯基)-5-乙氧基-4-恶唑乙酸乙酯]使血清胆固醇呈剂量依赖性降低:这种降血脂活性估计约为氯贝丁酯的7倍。另一方面,氯贝丁酯在100mg/kg时会诱导肝肿大,而Y-9738在此剂量下不会,该剂量约为有效剂量的10倍。高胆固醇和硫脲诱导的高脂血症的特征是β-脂蛋白增加(肝素-钙和圆盘电泳)。在该模型中,Y-9738对β-脂蛋白胆固醇显示出剂量依赖性降低作用,β/α脂蛋白比值显著降低。有α-脂蛋白增加的趋势。相比之下,氯贝丁酯对这种高β-脂蛋白血症没有作用。这些结果表明,上述模型在探索高β-脂蛋白血症方面可能有价值,并且Y-9738在高脂血症治疗中可能比氯贝丁酯更有用。

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