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辛伐他汀与吉非贝齐治疗混合性高脂蛋白血症疗效的比较研究:基于基线血脂、载脂蛋白E基因型、脂蛋白(a)和胰岛素水平预测疗效

A comparative study of the efficacy of simvastatin and gemfibrozil in combined hyperlipoproteinemia: prediction of response by baseline lipids, apo E genotype, lipoprotein(a) and insulin.

作者信息

Nestel P, Simons L, Barter P, Clifton P, Colquhoun D, Hamilton-Craig I, Sikaris K, Sullivan D

机构信息

Baker Medical Research Institute, Prahran, Victoria, Australia.

出版信息

Atherosclerosis. 1997 Mar 21;129(2):231-9. doi: 10.1016/s0021-9150(96)06031-5.

Abstract

Combined hyperlipoproteinemia (CHL) can be difficult to treat because of the heterogeneous nature of the lipoprotein abnormalities. We compared the relative efficacies of simvastatin and gemfibrozil and sought predictors of responsiveness in terms of the baseline lipids and other potential metabolic determinants (plasma insulin, Lp(a) and apo E genotype). Sixty-six subjects entered a cross-over, randomized trial involving 12 weeks on each drug. Efficacy was assessed after 6 and 12 weeks on each treatment. Simvastatin lowered total cholesterol 24%, triglycerides 12%, LDL cholesterol 33%, raised HDL cholesterol 13% and substantially reduced the cholesterol:triglyceride ratio in VLDL and IDL. Gemfibrozil lowered total cholesterol 5%, triglycerides 44%, raised HDL 26% and reduced VLDL and IDL lipids more than simvastatin did. LDL size increased with both treatments and HDL size increased with simvastatin. Responsiveness (25% fall in cholesterol or 40% fall in triglycerides) was shown by 31/61 subjects when taking simvastatin (cholesterol-lowering) and by 44/60 taking gemfibrozil (triglyceride-lowering). Responsiveness was greatest in those with apo E2 genotype with both drugs (P < 0.05). Unexpectedly, responders to simvastatin tended to have lower baseline total cholesterol but higher triglyceride levels than those whose cholesterol or triglyceride was lowered by gemfibrozil. Nevertheless, more hypercholesterolemic subjects responded to simvastatin and more hypertriglyceridemic subjects to gemfibrozil. Lp(a) (P = 0.04) and plasma insulin concentrations (P = 0.03) were negative predictors of percentage triglyceride-lowering with gemfibrozil. The difference between the two drugs in triglyceride-lowering lessened with rising insulin and falling HDL cholesterol. Thus, the responsiveness to the two major classes of lipid lowering drugs can be partly predicted from baseline lipids and related metabolic parameters.

摘要

混合型高脂血症(CHL)由于脂蛋白异常具有异质性,可能难以治疗。我们比较了辛伐他汀和吉非贝齐的相对疗效,并根据基线血脂和其他潜在的代谢决定因素(血浆胰岛素、Lp(a)和载脂蛋白E基因型)寻找反应性的预测指标。66名受试者进入一项交叉随机试验,每种药物治疗12周。在每种治疗的6周和12周后评估疗效。辛伐他汀使总胆固醇降低24%,甘油三酯降低12%,低密度脂蛋白胆固醇降低33%,高密度脂蛋白胆固醇升高13%,并大幅降低了极低密度脂蛋白和中间密度脂蛋白中的胆固醇:甘油三酯比值。吉非贝齐使总胆固醇降低5%,甘油三酯降低44%,高密度脂蛋白升高26%,并且比辛伐他汀更能降低极低密度脂蛋白和中间密度脂蛋白的脂质。两种治疗均使低密度脂蛋白大小增加,辛伐他汀使高密度脂蛋白大小增加。服用辛伐他汀(降低胆固醇)时,61名受试者中有31名出现反应性(胆固醇降低25%或甘油三酯降低40%),服用吉非贝齐(降低甘油三酯)时,60名受试者中有44名出现反应性。两种药物对载脂蛋白E2基因型的患者反应性最大(P < 0.05)。出乎意料的是,与吉非贝齐降低胆固醇或甘油三酯的患者相比,辛伐他汀的反应者基线总胆固醇往往较低,但甘油三酯水平较高。然而,更多的高胆固醇血症患者对辛伐他汀有反应,更多的高甘油三酯血症患者对吉非贝齐有反应。Lp(a)(P = 0.04)和血浆胰岛素浓度(P = 0.03)是吉非贝齐降低甘油三酯百分比的负预测指标。随着胰岛素升高和高密度脂蛋白胆固醇降低,两种药物在降低甘油三酯方面的差异减小。因此,对两类主要降脂药物的反应性可以部分地从基线血脂和相关代谢参数中预测出来。

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