Relative efficacy of GLP-1 and GLP-1/GIP receptor agonists in the prevention of alcohol-use disorders using a target trial emulation approach.

IF 5.7 2区医学 Q1 ENDOCRINOLOGY & METABOLISM

Diabetes, Obesity & Metabolism Pub Date : 2025-10-07 DOI:10.1111/dom.70169

Alex E Henney, David R Riley, Megan Heague, Carl A Roberts, Theresa J Hydes, Matthew Anson, David M Hughes, Uazman Alam, Daniel J Cuthbertson

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引用次数: 0

Abstract

Aims: There is growing evidence that the GLP-1 system is implicated in alcohol and other substance use disorders, and that GLP-1-based therapies may have therapeutic relevance in alcohol use disorder (AUD). We aimed to determine the impact of GLP-1 based therapies on incident AUDs in a real-world setting in patients with T2D.

Material and methods: We conducted emulation target trials based on a real-world network of electronic health records (EHRs) from over 120 million patients in the United States of America. Four target trials were emulated among eligible patients with type 2 diabetes (T2D) who had no prior AUD diagnosis by comparing tirzepatide, semaglutide, liraglutide, and dulaglutide with DPP4 inhibitors (DPP4i). First-ever diagnosis of AUD occurred within an 18-month follow-up period and was examined using Kaplan-Meier survival analyses. Four target trial cohorts were generated and compared with a reference arm of patients treated with DPP4i: cohort (1) treatment with tirzepatide; cohort (2) treatment with semaglutide; cohort (3) treatment with liraglutide; and cohort (4) treatment with dulaglutide. Cohorts underwent propensity score matching 1:1 for confounders. We examined rates of incident AUD (ICD-10 code F10) and performed head-to-head analyses of the incretin-based therapies. We also performed sensitivity analyses relating to whether treatment was adjunctive therapy with metformin and by treatment adherence.

Results: After propensity-score matching, we identified four target trials of patients treated with tirzepatide (n = 7165), semaglutide (n = 20 198), liraglutide (n = 6565), and dulaglutide (n = 19 061); 1:1 with the reference (DPP4i) patients. Tirzepatide and semaglutide (but not liraglutide or dulaglutide) were associated with significant risk reduction of incident AUD compared to DPP4i (hazard ratio 0.47 [95% confidence interval 0.29, 0.75] and 0.68 [0.52, 0.89], respectively). Head-to-head comparison revealed tirzepatide had a significant risk reduction compared to liraglutide in incident AUD (0.47 [0.24, 0.92]).

Conclusion: In patients with T2D, tirzepatide and semaglutide treatment is associated with a lower incidence of AUD; robust randomised, controlled evidence for the use of these drugs for this novel indication is appropriate.

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GLP-1和GLP-1/GIP受体激动剂在预防酒精使用障碍中的相对功效

目的：越来越多的证据表明，GLP-1系统与酒精和其他物质使用障碍有关，基于GLP-1的治疗可能与酒精使用障碍（AUD）的治疗相关。我们的目的是确定基于GLP-1的治疗对现实世界中T2D患者发生aud的影响。材料和方法：我们基于来自美国超过1.2亿患者的电子健康记录（EHRs）的真实世界网络进行了模拟目标试验。通过比较替西帕肽、西马鲁肽、利拉鲁肽和杜拉鲁肽与DPP4抑制剂（DPP4i），在没有AUD诊断的符合条件的2型糖尿病（T2D）患者中模拟了四项目标试验。首次诊断AUD发生在18个月的随访期间，并使用Kaplan-Meier生存分析进行检查。生成了四个目标试验队列，并与接受DPP4i治疗的患者的参考组进行了比较：队列(1)接受替西肽治疗；队列(2)使用西马鲁肽治疗；队列(3)：利拉鲁肽治疗；用dulaglutide治疗的队列(4)。对混杂因素进行1:1匹配的倾向评分。我们检查了AUD的发生率（ICD-10代码F10），并对以肠促胰岛素为基础的治疗进行了正面分析。我们还对治疗是否为二甲双胍辅助治疗和治疗依从性进行了敏感性分析。结果：经过倾向评分匹配，我们确定了4个目标试验，患者接受了替西帕肽（n = 7165）、西马鲁肽（n = 20198）、利拉鲁肽（n = 6565）和杜拉鲁肽（n = 19061）治疗；与对照（DPP4i）患者的比例为1:1。与DPP4i相比，替西帕肽和西马鲁肽（但不包括利拉鲁肽或杜拉鲁肽）与发生AUD的风险显著降低相关（风险比分别为0.47[95%可信区间0.29,0.75]和0.68[0.52,0.89]）。头对头比较显示，与利拉鲁肽相比，替西帕肽在发生AUD方面的风险显著降低（0.47[0.24,0.92]）。结论：在T2D患者中，替西帕肽和西马鲁肽治疗与较低的AUD发生率相关；这些药物用于这种新适应症的可靠的随机对照证据是适当的。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Diabetes, Obesity & Metabolism 医学-内分泌学与代谢

CiteScore

10.90

自引率

6.90%

发文量

319

审稿时长

3-8 weeks

期刊介绍： Diabetes, Obesity and Metabolism is primarily a journal of clinical and experimental pharmacology and therapeutics covering the interrelated areas of diabetes, obesity and metabolism. The journal prioritises high-quality original research that reports on the effects of new or existing therapies, including dietary, exercise and lifestyle (non-pharmacological) interventions, in any aspect of metabolic and endocrine disease, either in humans or animal and cellular systems. ‘Metabolism’ may relate to lipids, bone and drug metabolism, or broader aspects of endocrine dysfunction. Preclinical pharmacology, pharmacokinetic studies, meta-analyses and those addressing drug safety and tolerability are also highly suitable for publication in this journal. Original research may be published as a main paper or as a research letter.