Smith Steve R, Aronne Louis J, Burns Colleen M, Kesty Nicole C, Halseth Amy E, Weyer Christian
Pennington Biomedical Research Center, Louisiana State University, Baton Rouge, Louisiana, USA.
Diabetes Care. 2008 Sep;31(9):1816-23. doi: 10.2337/dc08-0029. Epub 2008 Jun 20.
To assess long-term weight loss efficacy and safety of pramlintide used at different dosing regimens and in conjunction with lifestyle intervention (LSI).
In a 4-month, double-blind, placebo-controlled, dose-ranging study, 411 obese subjects were randomized to receive pramlintide (six arms: 120, 240, and 360 microg b.i.d. and t.i.d.) or placebo in conjunction with a structured LSI program geared toward weight loss. Of the 4-month evaluable subjects (n = 270), 77% opted to continue preexisting treatment during an 8-month single-blind extension (LSI geared toward weight maintenance).
At month 4, mean weight loss from baseline in the pramlintide arms ranged from 3.8 +/- 0.7 to 6.1 +/- 0.8 kg (2.8 +/- 0.8 kg with placebo). By month 12, initial 4-month weight loss was regained in the placebo group but was maintained in all but the 120-microg b.i.d. group. Placebo-corrected weight loss with 120 microg t.i.d. and 360 microg b.i.d. averaged 3.2 +/- 1.2 kg (3.1 +/- 1.1% body wt) and 3.3 +/- 1.1 kg (3.1 +/- 1.0% body wt), respectively, at month 4 (both P < 0.01; 4-month evaluable n = 270) and 6.1 +/- 2.1 kg (5.6 +/- 2.1% body wt) and 7.2 +/- 2.3 kg (6.8 +/- 2.3% body wt), respectively, at month 12 (both P < 0.01; 12-month evaluable n = 146). At month 12, 40 and 43% of subjects treated with 120 microg t.i.d. and 360 microg b.i.d., respectively, achieved >or=10% weight loss (vs. 12% for placebo). Nausea, the most common adverse event with pramlintide in the 4-month study (9-29% pramlintide vs. 2% placebo), was generally mild to moderate and occurred in <10% of subjects during the extension.
When used over 12 months as an adjunct to LSI, pramlintide treatment, with low-dose three-times-daily or higher-dose two-times-daily regimens, helped obese subjects achieve greater initial weight loss and enhanced long-term maintenance of weight loss.
评估不同给药方案的普兰林肽联合生活方式干预(LSI)的长期减肥疗效及安全性。
在一项为期4个月的双盲、安慰剂对照、剂量范围研究中,411名肥胖受试者被随机分配接受普兰林肽(六个组:每日两次,每次120、240和360微克;每日三次,每次120、240和360微克)或安慰剂,并结合旨在减肥的结构化LSI计划。在4个月可评估的受试者(n = 270)中,77%的人选择在为期8个月的单盲延长期(旨在维持体重的LSI)继续原有治疗。
在第4个月时,普兰林肽组从基线开始的平均体重减轻范围为3.8±0.7至6.1±0.8千克(安慰剂组为2.8±0.8千克)。到第12个月时,安慰剂组恢复了最初4个月的体重减轻,但除每日两次120微克组外,其他普兰林肽组均维持了体重减轻。在第4个月时,每日三次120微克和每日两次360微克的普兰林肽组校正安慰剂后的体重减轻平均分别为3.2±1.2千克(体重的3.1±1.1%)和3.3±1.1千克(体重的3.1±1.0%)(P均<0.01;4个月可评估n = 270);在第12个月时,分别为6.1±2.1千克(体重的5.6±2.1%)和7.2±2.3千克(体重的6.8±2.3%)(P均<0.01;12个月可评估n = 146)。在第12个月时,每日三次120微克和每日两次360微克治疗的受试者中分别有40%和43%实现了体重减轻≥10%(安慰剂组为12%)。恶心是4个月研究中普兰林肽最常见的不良事件(普兰林肽组为9 - 29%,安慰剂组为2%),一般为轻至中度,在延长期<10%的受试者中出现。
当作为LSI的辅助手段使用12个月时,普兰林肽治疗采用低剂量每日三次或高剂量每日两次方案,有助于肥胖受试者实现更大的初始体重减轻,并增强体重减轻的长期维持效果。
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