辛伐他汀治疗原发性高胆固醇血症。新西兰多中心评估。

Treatment of primary hypercholesterolaemia with simvastatin. New Zealand multicentre evaluation.

作者信息

Lintott C J, Scott R S, Sharpe D N, Nye E R, Charleson H, French J K, White H D, Reuben S, Maling T J, Lewis G R

机构信息

Princess Margaret Hospital, Christchurch, New Zealand.

出版信息

Med J Aust. 1991 Oct 7;155(7):433-6.

PMID:1921811

Abstract

OBJECTIVE

To assess the efficacy of simvastatin in a large patient cohort.

DESIGN

In an open multicentre study, after a four week placebo phase, patients were treated with simvastatin for 24 weeks; a subgroup continued therapy for a further 24 weeks. Efficacy of simvastatin (a) with prolonged use over three years, and (b) in combination with bezafibrate was assessed in an open single site study.

SETTING

Lipid or cardiology specialist hospital outpatient clinics.

PATIENTS

For the open multicentre study, 228 patients with primary hypercholesterolaemia (total cholesterol level greater than 6.5 mmol/L) were recruited, of whom 224 met entry criteria and completed the study. Forty-seven of these patients continued therapy for one year. In the open single site study, 22 patients (with low density lipoprotein [LDL] cholesterol levels greater than 4.3 mmol/L) participated in studies of long term use (n = 9) or of combined therapy (n = 13).

INTERVENTION

Therapy in the open multicentre study began with 10 mg of simvastatin per day, doubling to 20 mg after six weeks and then 40 mg after 12 weeks of therapy if total cholesterol levels persisted above 5.2 mmol/L. In the study of long term use, simvastatin (40 mg daily) was taken continuously over three years. In the study of combination therapy, bezafibrate (600 mg daily) was taken in addition to simvastatin (40 mg daily) for 10 months.

MAIN OUTCOME MEASURES

Plasma lipid and lipoprotein concentrations.

RESULTS

In the multicentre study, total plasma cholesterol levels were reduced by 32.8% from 9.11 +/- 1.84 (in mmol/L, mean +/- SD) to 6.12 +/- 1.25 (P less than 0.001), and LDL cholesterol levels by 41.4% from 6.90 +/- 1.92 to 4.04 +/- 0.31 (P less than 0.001). The effect of therapy was sustained in those patients continuing therapy to 48 weeks. The study of long term use found no significant attenuation of effect over three years of monotherapy. Combined simvastatin/bezafibrate therapy reduced the LDL cholesterol concentration by a further 19.9% (P less than 0.001) from levels achieved on simvastatin alone.

CONCLUSIONS

Simvastatin is an effective, well tolerated lipid lowering drug, without significant attenuation of effect with prolonged use. Simvastatin plus bezafibrate appears to be a potentially useful drug combination.

摘要

目的

评估辛伐他汀在一大群患者中的疗效。

设计

在一项开放性多中心研究中，经过为期四周的安慰剂阶段后，患者接受辛伐他汀治疗24周；一个亚组继续治疗另外24周。在一项开放性单中心研究中评估了辛伐他汀（a）三年长期使用以及（b）与苯扎贝特联合使用的疗效。

地点

脂质或心脏病专科医院门诊。

患者

对于开放性多中心研究，招募了228例原发性高胆固醇血症患者（总胆固醇水平大于6.5 mmol/L），其中224例符合入选标准并完成了研究。这些患者中有47例继续治疗一年。在开放性单中心研究中，22例患者（低密度脂蛋白[LDL]胆固醇水平大于4.3 mmol/L）参与了长期使用研究（n = 9）或联合治疗研究（n = 13）。

干预

开放性多中心研究中的治疗开始时每天服用10 mg辛伐他汀，六周后加倍至20 mg，如果总胆固醇水平持续高于5.2 mmol/L，则在治疗12周后增至40 mg。在长期使用研究中，连续三年每天服用辛伐他汀（40 mg）。在联合治疗研究中，除每天服用辛伐他汀（40 mg）外，还服用苯扎贝特（600 mg）10个月。

主要观察指标

血浆脂质和脂蛋白浓度。

结果

在多中心研究中，血浆总胆固醇水平从9.11±1.84（mmol/L，均值±标准差）降至6.12±1.25，降低了32.8%（P<0.001），LDL胆固醇水平从6.90±1.92降至4.04±0.31，降低了41.4%（P<0.001）。在继续治疗至48周的患者中，治疗效果得以维持。长期使用研究发现，三年单一疗法的效果无显著减弱。辛伐他汀/苯扎贝特联合治疗使LDL胆固醇浓度在仅使用辛伐他汀所达到的水平基础上进一步降低了19.9%（P<0.001）。