McMaster University, Hamilton, Canada.
McMaster Children's Hospital, Hamilton, Canada.
Pediatr Obes. 2024 Nov;19(11):e13169. doi: 10.1111/ijpo.13169. Epub 2024 Sep 6.
To summarize the literature on pharmacotherapy for managing paediatric obesity.
A systematic review and meta-analysis were conducted of randomized controlled trials (RCTs) with <18-year-olds of pharmacotherapeutic agents published up to November 2022. Estimates of effect for outcomes were presented relative to minimal important differences and GRADE certainty of evidence. We examined data on patient/proxy-reported outcome measures (PROMs), cardiometabolic risk factors, anthropometry and adverse events (AEs).
Overall, 35 RCTs were included. Trials examined metformin (n = 26), glucagon-like peptide-1 receptor agonists (GLP1RAs) (n = 7) and a lipase inhibitor (orlistat; n = 2). Intervention duration varied (3-24 months). Metformin had little to no benefit on PROMs (e.g., health-related quality of life [HRQoL]; 6 RCTs), moderate reductions in triglycerides, a moderate decline in insulin resistance, a small to moderate decline in BMI z-score (BMIz) and a moderate increase in mild to moderate gastrointestinal AEs. Response to GLP1RAs was heterogeneous and results of subgroup analysis demonstrated variability of impact. Liraglutide (2 RCTs) resulted in a small reduction in HOMA-IR and BMIz, but little to no benefit on other outcomes. Exenatide (4 RCTs) had a moderate reduction on blood pressure and a small decrease in BMIz with little to no benefit on other outcomes. Semaglutide (1 RCT) had a small benefit on HRQoL, a small reduction on SBP, a moderate reduction on total cholesterol and LDL-cholesterol, a large reduction on triglyceride, and a very large decline in BMIz accompanied by a small increase in mild to moderate gastrointestinal AEs. Orlistat had a moderate reduction in DBP and little to no benefit in other outcomes measured, but had a very large increased risk of mild to moderate gastrointestinal AEs. Serious AEs were rare and for interventions with sufficent AE reporting, were considered not likely attributable to the interventions.
Few studies examined the impact of pharmacotherapy on PROMs. There is evidence that metformin and GLP1RAs lead to important improvements in cardiometabolic and anthropometric outcomes while accompanied by mild to moderate AEs. Long-term effectiveness and safety of GLP1RAs remain to be evaluated.
总结治疗儿科肥胖症的药物治疗文献。
对截至 2022 年 11 月发表的关于 18 岁以下儿童药物治疗的随机对照试验(RCT)进行系统评价和荟萃分析。根据最小重要差异和 GRADE 证据确定性,报告了结局的效应估计值。我们检查了患者/代理报告的结局测量(PROMs)、心血管代谢风险因素、人体测量和不良事件(AE)的数据。
共有 35 项 RCT 纳入。试验研究了二甲双胍(n=26)、胰高血糖素样肽-1 受体激动剂(GLP1RAs)(n=7)和脂肪酶抑制剂(奥利司他;n=2)。干预持续时间不同(3-24 个月)。二甲双胍对 PROMs(如健康相关生活质量 [HRQoL];6 项 RCT)几乎没有益处,适度降低甘油三酯,适度降低胰岛素抵抗,适度降低 BMIz,适度增加轻度至中度胃肠道 AE。GLP1RA 的反应具有异质性,亚组分析结果表明影响的可变性。利拉鲁肽(2 项 RCT)导致 HOMA-IR 和 BMIz 略有降低,但对其他结局几乎没有益处。艾塞那肽(4 项 RCT)适度降低血压,BMIz 略有下降,其他结局几乎没有益处。司美格鲁肽(1 项 RCT)对 HRQoL 有较小的益处,SBP 有较小的降低,总胆固醇和 LDL 胆固醇有适度的降低,甘油三酯有较大的降低,BMIz 有很大的降低,轻度至中度胃肠道 AE 有小的增加。奥利司他适度降低舒张压,对其他测量的结局几乎没有益处,但轻度至中度胃肠道 AE 的风险显著增加。严重不良事件很少见,对于具有足够 AE 报告的干预措施,认为不太可能归因于干预措施。
很少有研究考察药物治疗对 PROMs 的影响。有证据表明,二甲双胍和 GLP1RA 可导致心血管代谢和人体测量结局的重要改善,同时伴有轻度至中度 AE。GLP1RA 的长期有效性和安全性仍有待评估。
