Brigham and Women's Hospital, Boston, Massachusetts.
Rotherham Institute for Obesity, Clifton Medical Centre, Rotherham, UK.
Diabetes Obes Metab. 2020 Mar;22(3):303-314. doi: 10.1111/dom.13896. Epub 2019 Nov 14.
To evaluate the impact of relevant patient-level characteristics on the efficacy and safety of subcutaneous, once-weekly semaglutide in subjects with type 2 diabetes.
Exploratory post hoc analyses of pooled SUSTAIN 1-5 (phase 3a) randomized, controlled trials examined the change from baseline in HbA1c and body weight (BW), and the proportions of subjects achieving the composite endpoint (HbA1c < 7.0% [53 mmol/mol]), without weight gain or severe/blood glucose-confirmed symptomatic hypoglycaemia at week 30 with semaglutide (0.5/1.0 mg) across clinically relevant patient subgroups: baseline HbA1c (≤7.5%, >7.5%-8.0%, >8.0%-8.5%, >8.5%-9.0% and > 9.0%), background medications, diabetes duration and pancreatic beta-cell function.
Mean HbA1c (% point) reductions increased from lowest to highest HbA1c subgroups (-0.9%, -1.2%,-1.5%, -1.7% and -2.3% [effect of subgroup within treatment: P = 0.247] for semaglutide 0.5 mg, and -1.1%, -1.4%, -1.9%, -2.1% and -2.7% [P = 0.045] for semaglutide 1.0 mg), with mean HbA1c ranges at week 30 of 6.3%-7.3% and 6.1%-6.9%, respectively. The corresponding BW reductions generally decreased with increasing baseline HbA1c (-4.4, -3.9, -3.9, -3.3 and -2.9 kg [P = 0.004], and -6.4, -5.9, -5.2, -4.5 and -4.8 kg [P < 0.001], respectively). HbA1c and BW reductions were consistently greater for semaglutide 1.0 mg versus 0.5 mg across background medication, diabetes duration and pancreatic beta-cell function subgroups. Adverse events with semaglutide were consistent with the glucagon-like peptide-1 receptor agonist class, with gastrointestinal events the most common.
Semaglutide was consistently efficacious across the continuum of diabetes care in a broad spectrum of patient subgroups with a range of clinical characteristics.
评估相关患者特征对 2 型糖尿病患者皮下每周一次司美格鲁肽疗效和安全性的影响。
对 SUSTAIN 1-5(3a 期)随机对照试验的探索性事后分析,考察了基线时 HbA1c 和体重(BW)的变化,以及在第 30 周时司美格鲁肽(0.5/1.0mg)治疗下达到复合终点(HbA1c<7.0%[53mmol/mol]、无体重增加或严重/血糖确认的症状性低血糖)的患者比例,这些患者按临床相关患者亚组进行分层:基线 HbA1c(≤7.5%、>7.5%-8.0%、>8.0%-8.5%、>8.5%-9.0%和>9.0%)、背景药物、糖尿病病程和胰岛β细胞功能。
HbA1c 降幅(%点)从最低到最高 HbA1c 亚组逐渐增加(司美格鲁肽 0.5mg 组分别为-0.9%、-1.2%、-1.5%、-1.7%和-2.3%[治疗内亚组的影响:P=0.247],司美格鲁肽 1.0mg 组分别为-1.1%、-1.4%、-1.9%、-2.1%和-2.7%[P=0.045]),第 30 周的平均 HbA1c 范围分别为 6.3%-7.3%和 6.1%-6.9%。相应的 BW 降低通常随基线 HbA1c 升高而降低(司美格鲁肽 0.5mg 组分别为-4.4、-3.9、-3.9、-3.3 和-2.9kg[P=0.004],司美格鲁肽 1.0mg 组分别为-6.4、-5.9、-5.2、-4.5 和-4.8kg[P<0.001])。与司美格鲁肽 0.5mg 相比,司美格鲁肽 1.0mg 在背景药物、糖尿病病程和胰岛β细胞功能亚组中均显示出更大的 HbA1c 和 BW 降低。司美格鲁肽的不良反应与胰高血糖素样肽-1 受体激动剂类一致,以胃肠道事件最常见。
在广泛的患者亚组中,司美格鲁肽在整个糖尿病治疗连续体中均具有一致的疗效,这些患者具有一系列临床特征。
