Exploring the association between weight loss-inducing medications and multiple sclerosis: insights from the FDA adverse event reporting system database.

IF 5.4 3区 材料科学 Q2 CHEMISTRY, PHYSICAL ACS Applied Energy Materials Pub Date : 2024-04-01 eCollection Date: 2024-01-01 DOI:10.1177/17562864241241383
Afsaneh Shirani, Anne H Cross, Olaf Stuve
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Abstract

Background: Several studies have demonstrated that early childhood and adolescent obesity are risk factors for multiple sclerosis (MS) susceptibility. Obesity is thought to share inflammatory components with MS through overproduction of pro-inflammatory adipokines (e.g., leptin) and reduction of anti-inflammatory adipokines (e.g, adiponectin). Recently, drug repurposing (i.e. identifying new indications for existing drugs) has garnered significant attention. The US Food and Drug Administration Adverse Event Reporting System (FAERS) database serves not only as a resource for mining adverse drug reactions and safety signals but also for identifying inverse associations and potential medication repurposing opportunities.

Objective: We aimed to explore the association between weight-loss-inducing drugs and MS using real-world reports from the FAERS database.

Design: Secondary analysis of existing data from the FAERS database.

Methods: We conducted a disproportionality analysis using the FAERS database between the fourth quarter of 2003 and the second quarter of 2023 to explore associations between MS and weight loss-inducing drugs. Disproportionality was quantified using the reporting odds ratio (ROR). An inverse association was defined when the upper limit of the 95% confidence interval for ROR was <1.

Results: We found an inverse association between MS and anti-diabetic weight loss-inducing drugs including semaglutide (ROR: 0.238; 95% CI: 0.132-0.429), dulaglutide (ROR: 0.165; 95% CI: 0.109-0.248), liraglutide (ROR: 0.161; 95% CI: 0.091-0.284), empagliflozin (ROR: 0.234; 95% CI: 0.146-0.377), and metformin (ROR: 0.387; 95% CI: 0.340-0.440). No inverse associations were found for other weight loss-inducing drugs such as phentermine, bupropion, topiramate, zonisamide, and amphetamine. An exception was naltrexone (ROR: 0.556; 95% CI: 0.384-0.806).

Conclusion: Our findings suggest a potential consideration for repurposing anti-diabetic weight loss-inducing drugs including semaglutide, dulaglutide, and liraglutide (glucagon-like peptide-1 receptor agonists), empagliflozin (sodium-glucose cotransporter-2 inhibitor), and metformin (biguanide), for MS. This warrants validation through rigorous methodologies and prospective studies.

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探索减肥药物与多发性硬化症之间的关联:从美国食品及药物管理局不良事件报告系统数据库中获得的启示。
背景:多项研究表明,儿童早期和青少年肥胖是多发性硬化症(MS)易感性的危险因素。肥胖症被认为与多发性硬化症具有相同的炎症成分,即促炎性脂肪因子(如瘦素)分泌过多,而抗炎性脂肪因子(如脂肪连通素)分泌减少。最近,药物再利用(即为现有药物确定新的适应症)引起了广泛关注。美国食品和药物管理局不良事件报告系统(FAERS)数据库不仅是挖掘药物不良反应和安全信号的资源,也是识别反向关联和潜在药物再利用机会的资源:我们旨在利用 FAERS 数据库中的真实报告,探讨减肥药与多发性硬化症之间的关联:设计:对 FAERS 数据库中的现有数据进行二次分析:我们利用 FAERS 数据库中 2003 年第四季度至 2023 年第二季度的数据进行了比例失调分析,以探讨多发性硬化症与减肥药之间的关联。比例失调采用报告几率比(ROR)进行量化。当 ROR 的 95% 置信区间的上限为 "结果 "时,则定义为反向关联:我们发现 MS 与抗糖尿病减重诱导药物之间存在反比关系,这些药物包括塞马鲁肽(ROR:0.238;95% CI:0.132-0.429)、度拉鲁肽(ROR:0.165;95% CI:0.109-0.248)、利拉鲁肽(ROR:0.161;95% CI:0.091-0.284)、恩格列净(ROR:0.234;95% CI:0.146-0.377)和二甲双胍(ROR:0.387;95% CI:0.340-0.440)。芬特明、安非他明、托吡酯、唑尼沙胺和安非他明等其他减肥药物没有发现反向关联。纳曲酮(ROR:0.556;95% CI:0.384-0.806)是一个例外:我们的研究结果表明,有可能考虑将抗糖尿病减肥诱导药物(包括semaglutide、dulaglutide和liraglutide(胰高血糖素样肽-1受体激动剂)、empagliflozin(钠-葡萄糖共转运体-2抑制剂)和二甲双胍(双胍类))重新用于多发性硬化症。这需要通过严格的方法和前瞻性研究进行验证。
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来源期刊
ACS Applied Energy Materials
ACS Applied Energy Materials Materials Science-Materials Chemistry
CiteScore
10.30
自引率
6.20%
发文量
1368
期刊介绍: ACS Applied Energy Materials is an interdisciplinary journal publishing original research covering all aspects of materials, engineering, chemistry, physics and biology relevant to energy conversion and storage. The journal is devoted to reports of new and original experimental and theoretical research of an applied nature that integrate knowledge in the areas of materials, engineering, physics, bioscience, and chemistry into important energy applications.
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