首页> 美国卫生研究院文献>Journal of the Royal Society of Medicine >Gemfibrozil: effect on serum lipids lipoproteins postheparin plasma lipase activities and glucose tolerance in primary hypertriglyceridaemia.
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Gemfibrozil: effect on serum lipids lipoproteins postheparin plasma lipase activities and glucose tolerance in primary hypertriglyceridaemia.

机译:吉非贝齐:对原发性高甘油三酯血症的血脂脂蛋白肝素后血浆脂肪酶活性和葡萄糖耐量的影响。

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摘要

The hypolipidaemic effect of a new drug, gemfibrozil (CI-719), was studied for 20 weeks in 20 patients with primary type IIb, III, IV or V hyperlipoproteinaemia. Baseline recordings of serum cholesterol (9.1 mmol/l), triglyceride (3.79 mmol/l) and ultra-centrifugally isolated lipoproteins were obtained during a six-week pretreatment period with stable diet and body weight. With 800 mg of gemfibrozil per day given in two divided doses, the mean serum triglyceride and cholesterol levels were decreased by 44.6% and 10.5% respectively, during 20 treatment weeks. Only 2 patients were completely resistant to the hypolipidaemic action of the drug. Serum triglyceride was brought down to normal levels in 9 subjects. After 12 weeks of treatment the mean VLDL-triglyceride, VLDL-cholesterol, and LDL-triglyceride were reduced by 48.5%, 57.6%, and 22.7% respectively, while the HDL-cholesterol rose by 16%. The LDL-cholesterol increased slightly but significantly during treatment in type IV patients and decreased in type IIb patients. The change of LDL-cholesterol showed an inverse correlation with the initial LDL-cholesterol level (r=-0.87). The postheparin plasma lipoprotein lipase and hepatic lipase activities, determined separately by an immunochemical method, increased during four weeks of gemfibrozil treatment (+18.1% and +20.6% respectively), but neither of these changes was significantly correlated with the changes in any of the serum lipid or lipoprotein levels. Oral glucose tolerance was not influenced by the treatment, but one-hour plasma insulin increased slightly during administration of the drug. One patient discontinued the drug after eight weeks because of generalized allergic eczema, but no other side effects were recorded. It is concluded that gemfibrozil is highly effective in reducing elevated serum VLDL levels. The simultaneous elevation of LDL in type IV patients needs more attention and study. The mechanism of the hypolipidaemic action of the drug is so far obscure, but it might partly be due to an increased efficiency in VLDL removal by an increased activity of lipoprotein lipase.
机译:在20例原发性IIb,III,IV或V型高脂蛋白血症患者中研究了一种新药吉非贝齐(CI-719)的降血脂作用20周。在为期六周的预处理过程中,以稳定的饮食和体重获得了血清胆固醇(9.1 mmol / l),甘油三酸酯(3.79 mmol / l)和超离心分离的脂蛋白的基线记录。每天800 mg吉非贝齐分两次服用,在20个治疗周内,平均血清甘油三酸酯和胆固醇水平分别降低了44.6%和10.5%。仅2例患者对该药的降血脂作用完全抵抗。 9名受试者的血清甘油三酸酯降至正常水平。治疗12周后,平均VLDL-甘油三酸酯,VLDL-胆固醇和LDL-甘油三酸酯分别降低了48.5%,57.6%和22.7%,而HDL-胆固醇则提高了16%。 IV型患者在治疗期间LDL胆固醇略有升高,但IIb型患者则降低。 LDL-胆固醇的变化与初始LDL-胆固醇水平呈负相关(r = -0.87)。肝素后血浆脂蛋白脂肪酶和肝脂肪酶活性(通过免疫化学方法分别确定)在吉非贝齐治疗的四个星期内增加(分别为+ 18.1%和+ 20.6%),但这些变化均与任何其他因素的变化均无显着相关性。血清脂质或脂蛋白水平。口服葡萄糖耐量不受治疗的影响,但是在给药期间一小时血浆胰岛素略有增加。一名患者由于全身性过敏性湿疹在八周后停药,但未记录到其他副作用。结论是吉非贝齐在降低升高的血清VLDL水平方面非常有效。 IV型患者中LDL的同时升高需要更多的关注和研究。迄今为止,该药物的降血脂作用的机理尚不清楚,但这可能部分归因于脂蛋白脂肪酶活性的提高,VLDL去除效率提高。

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