Acute renal failure and cardiac arrhythmias associated with remdesivir use in patients with COVID-19 infections: Analysis using the US FDA adverse event reporting system.

Pub Date : 2023-01-01 DOI:10.3233/JRS-220009
Lisajo Orogun, Te-Yuan Chyou, Prasad S Nishtala
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Abstract

Background: Recently, antivirals, including remdesivir, have been repurposed to treat COVID-19 infections. Initial concerns have been raised about the adverse renal and cardiac events associated with remdesivir.

Objective: This study aimed to analyse the adverse renal and cardiac events associated with remdesivir in patients with COVID-19 infections using the US FDA adverse event reporting system.

Method: A case/non-case method was used to determine adverse drug events associated with remdesivir as the primary suspect drug between January 1, 2020, and November 11, 2021, for patients with COVID-19 infections. Cases were reports for remdesivir with ≥1 ADEs as preferred terms included in the Medical Dictionary of Regulatory Activities (MedDRA) system organ classes 'Renal and urinary disorders' or 'cardiac' disorders. To measure disproportionality in reporting of ADEs, frequentist approaches, including the proportional reporting ratio (PRR) and reporting odds ratio (ROR), were used. The empirical Bayesian Geometric Mean (EBGM) score and information component (IC) value were calculated using a Bayesian approach. A signal was defined as the lower limit of 95% confidence intervals of ROR ≥ 2, PRR ≥ 2, IC > 0, and EBGM > 1 for ADEs with ≥4 reports. Sensitivity analyses were undertaken by excluding reports for non-Covid indications and medications strongly associated with AKI and cardiac arrhythmias.

Results: In the main analysis for remdesivir use in patients with COVID-19 infections, we identified 315 adverse cardiac events comprising 31 different MeDRA PTs and 844 adverse renal events comprising 13 different MeDRA PTs. Regarding adverse renal events, disproportionality signals were noted for "renal failure" (ROR = 2.8 (2.03-3.86); EBGM = 1.92 (1.58-2.31), "acute kidney injury" (ROR = 16.11 (12.52-20.73); EBGM = 2.81 (2.57-3.07), "renal impairment" (ROR = 3.45 (2.68-4.45); EBGM = 2.02 (1.74-2.33). Regarding adverse cardiac events, strong disproportionality signals were noted for "electrocardiogram QT prolonged" (ROR = 6.45 (2.54-16.36); EBGM = 2.04 (1.65-2.51), "pulseless electrical activity" (ROR = 43.57 (13.64-139.20); EBGM = 2.44 (1.74-3.33), "sinus bradycardia" (ROR = 35.86 (11.16-115.26); EBGM = 2.82 (2.23-3.53), "ventricular tachycardia" (ROR = 8.73 (3.55-21.45); EBGM = 2.52 (1.89-3.31). The risk of AKI and cardiac arrythmias were confirmed by sensitivity analyses.

Conclusion: This hypothesis-generating study identified AKI and cardiac arrhythmias associated with remdesivir use in patients with COVID-19 infections. The relationship between AKI and cardiac arrhythmias should be further investigated using registries or large clinical data to assess the impact of age, genetics, comorbidity, and the severity of Covid infections as potential confounders.

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COVID-19感染患者使用瑞德西韦相关的急性肾功能衰竭和心律失常:使用美国FDA不良事件报告系统进行分析
背景:最近,包括瑞德西韦在内的抗病毒药物已被重新用于治疗COVID-19感染。最初的担忧是与瑞德西韦相关的肾脏和心脏不良事件。目的:本研究旨在利用美国FDA不良事件报告系统分析COVID-19感染患者与瑞德西韦相关的肾脏和心脏不良事件。方法:采用病例/非病例法,对2020年1月1日至2021年11月11日期间COVID-19感染患者以瑞德西韦作为主要可疑药物相关的药物不良事件进行分析。报告的病例中,瑞德西韦的不良反应≥1次,首选术语包括在《调节活动医学词典》(MedDRA)系统器官类别“肾脏和泌尿系统疾病”或“心脏”疾病。为了测量不良事件报告的不相称性,使用了频率分析方法,包括比例报告比(PRR)和报告优势比(ROR)。利用贝叶斯方法计算经验贝叶斯几何平均(EBGM)得分和信息分量(IC)值。≥4例ade报告的95%置信区间ROR≥2、PRR≥2、IC > 0、EBGM > 1定义为信号。通过排除非covid适应症和与AKI和心律失常密切相关的药物的报告,进行敏感性分析。结果:在对COVID-19感染患者使用瑞德西韦的主要分析中,我们确定了315例不良心脏事件,包括31种不同的MeDRA PTs, 844例不良肾脏事件,包括13种不同的MeDRA PTs。对于肾脏不良事件,“肾功能衰竭”的歧化信号被注意到(ROR = 2.8 (2.03-3.86);EBGM = 1.92(1.58 ~ 2.31),“急性肾损伤”(ROR = 16.11 (12.52 ~ 20.73);EBGM = 2.81(2.57 ~ 3.07),“肾功能损害”(ROR = 3.45 (2.68 ~ 4.45);Ebgm = 2.02(1.74-2.33)。对于心脏不良事件,“心电图QT间期延长”存在强烈的歧化信号(ROR = 6.45 (2.54-16.36);EBGM = 2.04(1.65-2.51),“无脉电活动”(ROR = 43.57 (13.64-139.20);EBGM = 2.44(1.74 ~ 3.33),“窦性心动过缓”(ROR = 35.86 (11.16 ~ 115.26);EBGM = 2.82(2.23-3.53),“室性心动过速”(ROR = 8.73 (3.55-21.45);Ebgm = 2.52(1.89-3.31)。敏感性分析证实了AKI和心律失常的风险。结论:这项产生假设的研究确定了COVID-19感染患者使用瑞德西韦相关的AKI和心律失常。AKI与心律失常之间的关系应通过注册表或大量临床数据进一步研究,以评估年龄、遗传、合并症和Covid感染严重程度作为潜在混杂因素的影响。
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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