Muls E, Kolanowski J, Scheen A, Van Gaal L
Department of Endocrinology, Metabolism and Nutrition, University Hospital, Gasthuisberg, Leuven, Belgium.
Int J Obes Relat Metab Disord. 2001 Nov;25(11):1713-21. doi: 10.1038/sj.ijo.0801814.
Assessment of the effects of orlistat 120 mg three times daily vs placebo on weight loss and serum lipids in obese hypercholesterolemic patients.
A 24 week multicentre, double-blind, randomized, placebo-controlled trial. After a 2-week single-blind run-in period (placebo+diet (-600 kcal/day; < or =30% of calories as fat)), 294 patients were submitted to the hypocaloric diet and randomly assigned to either orlistat 120 mg or placebo three times daily. Patients who completed the double-blind study (n=255) were eligible for participation in a subsequent 24 week open-label orlistat extension phase.
Patients with body mass index (BMI) 27-40 kg/m2 and hypercholesterolemia (low-density-lipoprotein cholesterol, LDL-C, 4.1-6.7 mmol/l).
Efficacy assessments included weight loss, lipid levels, other cardiovascular risk factors and anthropometric parameters. Safety assessments.
Weight loss during run-in was similar in both groups. After randomization, orlistat-treated patients lost significantly more weight than placebo recipients: mean percentage weight loss from start of run-in to week 24 was-6.8% in the orlistat group and -3.8% in the placebo group (P<0.001). Moreover, more patients in the orlistat group than in the placebo group achieved clinically meaningful weight loss of > or =5% (64 vs 39%) or > or =10% (23 vs 13%) at week 24. Treatment with orlistat was associated with significantly greater changes in total cholesterol (-11.9% vs -4.0%; P<0.001) and LDL-C (-17.6 vs -7.6%; P<0.001). For any category of weight loss during the double-blind treatment period, change in LDL-C was more pronounced in orlistat-treated patients than in placebo recipients, indicating that orlistat had a direct cholesterol-lowering effect that was independent of weight reduction (P<0.001). Adjunction of orlistat during the extension phase in patients who initially received placebo induced a further decrease in weight, total cholesterol and LDL-C. Orlistat was generally well tolerated with a safety profile comparable to placebo, with the exception of a higher incidence of gastrointestinal events (> or =1 event in 64 vs 38% of patients).
Orlistat as an adjunct to dietary intervention promotes weight loss and reduces LDL-C beyond the effect of weight loss in overweight or obese patients with concomitant hypercholesterolemia.
评估每日三次服用120毫克奥利司他与安慰剂相比,对肥胖高胆固醇血症患者体重减轻及血脂的影响。
一项为期24周的多中心、双盲、随机、安慰剂对照试验。在为期2周的单盲导入期(安慰剂+节食(-600千卡/天;脂肪供能占卡路里的比例≤30%))后,294例患者接受低热量饮食,并随机分配至每日三次服用120毫克奥利司他组或安慰剂组。完成双盲研究的患者(n=255)有资格参加随后为期24周的开放标签奥利司他延长期试验。
体重指数(BMI)为27-40千克/平方米且患有高胆固醇血症(低密度脂蛋白胆固醇,LDL-C,4.1-6.7毫摩尔/升)的患者。
疗效评估包括体重减轻、血脂水平、其他心血管危险因素及人体测量参数。安全性评估。
导入期两组体重减轻情况相似。随机分组后,奥利司他治疗组患者体重减轻明显多于安慰剂组:从导入期开始至第24周,奥利司他组平均体重减轻百分比为-6.8%,安慰剂组为-3.8%(P<0.001)。此外,在第24周时,奥利司他组实现临床上有意义的体重减轻≥5%(64%对39%)或≥10%(23%对)的患者多于安慰剂组。服用奥利司他治疗与总胆固醇(-11.9%对-4.0%;P<0.001)和LDL-C(-17.6%对-7.6%;P<0.001)的显著更大变化相关。在双盲治疗期间,对于任何体重减轻类别,奥利司他治疗组患者的LDL-C变化比安慰剂组更明显,表明奥利司他具有独立于体重减轻的直接降胆固醇作用(P<0.001)。在最初接受安慰剂治疗的患者延长期加入奥利司他可进一步降低体重、总胆固醇和LDL-C。奥利司他总体耐受性良好,安全性与安慰剂相当,只是胃肠道事件发生率较高(≥1次事件的患者比例为64%对38%)。
对于伴有高胆固醇血症的超重或肥胖患者,奥利司他作为饮食干预的辅助手段可促进体重减轻并降低LDL-C,其作用超出体重减轻的效果。
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