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PURPOSE

Glucagon-like peptide-1 receptor agonists (GLP-1 RAs) are important therapeutic options for type 2 diabetes and obesity; however, concerns about ophthalmic safety persist. This study examined associations between GLP-1 RAs and ocular adverse events (AEs).

DESIGN

Global observational pharmacovigilance study.

METHODS

We searched the US FAERS database (via OpenVigil 2.1) and WHO's VigiBase (via VigiAccess) for optic nerve and retinal AEs associated with semaglutide and tirzepatide, covering the period from their respective approval dates-December 2017 for semaglutide and May 2022 for tirzepatide-through September 2024. In FAERS, all other drugs were compared, while in VigiBase, metformin, empagliflozin, dulaglutide, and insulin served as controls. Disproportionality metrics included reporting odds ratios (RORs) with 95% confidence intervals.

RESULTS

Semaglutide and tirzepatide accounted for 76 444 cases (0.59%) in FAERS (n = 12 936 341) and 118 639 cases (0.34%) in VigiBase (n > 35 000 000). Semaglutide showed significantly higher odds of ischemic optic neuropathy (ION) (FAERS: ROR = 11.12, 95% CI = 8.15-15.16; VigiBase: ROR = 68.58, 95% CI = 16.75-280.67), diabetic retinopathy (DR) (FAERS: ROR = 17.28, 95% CI = 13.62-21.91; VigiBase: ROR = 7.81, 95% CI = 5.60-10.90), as well as retinal/vitreous detachment, retinal/vitreous hemorrhage, and retinal tear (FAERS: ROR = 2.44-5.89, 95% CI = 1.70-8.97, all P < .001, IC = 0.49, compared to all other drugs. VigiBase: ROR = 5.49-20.91, 95% CI = 2.71-90.11, all P ≤ .0001, IC ≥ 0.53, compared to metformin). Unique to VigiBase were macular edema (ROR = 3.87, 95% CI = 1.89-7.92), macular hole (ROR = 20.90, 95% CI = 2.65-165.01), and papilledema (ROR = 6.97, 95% CI = 2.53-19.17) (all P ≤ .004, IC ≥ 0.27, compared to metformin). Sensitivity analyses using empagliflozin and dulaglutide revealed significant associations with ION and DR, while vitreous detachment and hemorrhage were significant when compared to dulaglutide. Additionally, when insulin was used as a comparator, semaglutide showed a higher ROR for ION (ROR = 9.84, 95% CI = 4.25-22.81, P < .0001, IC = 0.42). However, tirzepatide was only significantly associated with DR in FAERS.

CONCLUSIONS

Given the widespread use of semaglutide, its association with ocular AEs highlight the need for global pharmacovigilance and post-marketing surveillance.

目的

胰高血糖素样肽-1受体激动剂（GLP-1 RAs）是2型糖尿病和肥胖症的重要治疗选择；然而，对其眼部安全性的担忧依然存在。本研究探讨了GLP-1 RAs与眼部不良事件（AE）之间的关联。

设计

全球观察性药物警戒研究。

方法

我们通过OpenVigil 2.1搜索美国食品药品不良事件报告系统（FAERS）数据库，并通过VigiAccess搜索世界卫生组织的VigiBase数据库，以查找与司美格鲁肽和替尔泊肽相关的视神经和视网膜AE，涵盖从它们各自的批准日期（司美格鲁肽为2017年12月，替尔泊肽为2022年5月）至2024年9月的时间段。在FAERS中，将所有其他药物作为对照；在VigiBase中，将二甲双胍、恩格列净、度拉糖肽和胰岛素作为对照。不成比例性指标包括报告比值比（ROR）及其95%置信区间。

结果

在FAERS（n = 12 936 341）中，司美格鲁肽和替尔泊肽占76444例（0.59%）；在VigiBase（n > 35 000 000）中占118639例（0.34%）。司美格鲁肽发生缺血性视神经病变（ION）的几率显著更高（FAERS：ROR = 11.12，95% CI = 8.15 - 15.16；VigiBase：ROR = 68.58，95% CI = 16.75 - 280.67）、糖尿病视网膜病变（DR）（FAERS：ROR = 17.28，95% CI = 13.62 - 21.91；VigiBase：ROR = 7.81，95% CI = 5.60 - 10.90），以及视网膜/玻璃体脱离、视网膜/玻璃体出血和视网膜裂孔（FAERS：ROR = 2.44 - 5.89，95% CI = 1.70 - 8.97，所有P <.001，IC = 0.49，与所有其他药物相比。VigiBase：ROR = 5.49 - 20.91，95% CI = 2.71 - 90.11，所有P ≤.0001，IC ≥ 0.53，与二甲双胍相比）。VigiBase中特有的是黄斑水肿（ROR = 3.87，95% CI = 1.89 - 7.92）、黄斑裂孔（ROR = 20.90，95% CI = 2.65 - 165.01）和视乳头水肿（ROR = 6.97，95% CI = 2.53 - 19.17）（所有P ≤.004，IC ≥ 0.27，与二甲双胍相比）。使用恩格列净和度拉糖肽进行的敏感性分析显示与ION和DR存在显著关联，而与度拉糖肽相比，玻璃体脱离和出血具有显著性。此外，当使用胰岛素作为对照时，司美格鲁肽在ION方面显示出更高的ROR（ROR = 9.84，95% CI = 4.25 - 22.81，P <.0001，IC = 0.42）。然而，替尔泊肽仅在FAERS中与DR显著相关。

结论

鉴于司美格鲁肽的广泛使用，其与眼部AE的关联凸显了全球药物警戒和上市后监测的必要性。

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