Hyperglycaemic disorders associated with PCSK9 inhibitors: a real-world, pharmacovigilance study

医学 Evolocumab公司 不良事件报告系统 优势比 内科学 药物警戒 不利影响 胆固醇 载脂蛋白B 载脂蛋白A1
作者
Adam Goldman,Emanuel Raschi,Tali Cukierman‐Yaffe,Rachel Dankner,Roni Shouval,Michael Shechter,Ilan Ben‐Zvi,Hertzel C. Gerstein,Elad Maor
出处
期刊:European Journal of Preventive Cardiology [Oxford University Press]
卷期号:29 (9): 1334-1342 被引量:31
标识
DOI:10.1093/eurjpc/zwab209
摘要

Abstract Aims While genetic and biological studies indicated a potential association between proprotein-convertase subtilisin/kexin type 9 inhibitors (PCSK9i) and hyperglycaemia, real-world data are limited. Therefore, we sought to investigate this association using the FDA adverse event reporting system (FAERS). Methods and results The FAERS database (2015–2020) was retrospectively queried to characterize reporting of hyperglycaemic adverse events (AEs) with PCSK9i. Disproportionality analyses were performed using the adjusted reporting odds ratio (adj.ROR), and the lower bound of the information component (IC) 95% credibility interval (IC025 > 0 is deemed significant). Among 7 295 624 eligible patients, 71 748 reports of evolocumab and 15 976 of alirocumab were identified. Compared to the full database, PCSK9i treatment was associated with increased reporting of hyperglycaemic AEs [n = 1841, adj.ROR = 1.14 (1.07–1.22), IC025 = 0.13]. Hyperglycaemic AEs were primarily mild hyperglycaemia [n = 1469, adj. ROR = 1.48 (1.36–1.62), IC025 = 0.51] rather than diabetes [n = 372, adj. ROR = 0.67 (0.60–0.74), IC025 = −0.90]. Among PCSK9i agents, evolocumab, but not alirocumab, was associated with hyperglycaemic AEs [n = 1587, adj. ROR = 1.24 (1.15–1.32), IC025 = 0.20; n = 254, adj. ROR = 0.73 (0.60–0.88), IC025 = −0.38, respectively]. Hyperglycaemic AEs were reported more often with PCSK9i compared to ezetimibe [adj.ROR = 1.99 (1.35–2.94)], and less often compared to statins [adj.ROR = 0.26 (0.25–0.28)]. Notably, hyperglycaemic AEs were reported more frequently by diabetic than by non-diabetic patients (P < 0.001), mostly occurred within 6 months of treatment and were reversible upon drug discontinuation. Conclusion In a real-world setting, PCSK9i treatment was associated with increased reporting of mild hyperglycaemia, but not diabetes. While initial monitoring is warranted, the favourable glycaemic safety profile compared to statins supports their essential role in the management of lipid disorders.
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