Association of immunomodulatory therapies with COVID-19 mortality in rheumatoid arthritis: An analysis of the FDA adverse event reporting system

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Abstract

Background

The COVID-19 pandemic significantly affects patients with RA and other rheumatic diseases. Our study aims to explore the factors associated with COVID-19-related fatality among Rheumatoid Arthritis (RA) patients, especially immunomodulatory therapies, using the international Food and Drug Administration (FDA) Adverse Event Reporting System (FAERS).

Methods

Reportes from FAERS were extracted from February 2020 to September 2022, and uesd for this cross-sectional analysis. The investigative outcome was COVID-19-related death. Age, sex, region, event date, and immunomodulatory medications classies were included as co-variates in multivariable logistic regression. In view of the different targeting and affinity of individual JAKi, Tofacitinib, Upadacitinib and Baricitinib was respectively analyzed.

Results

In all, 3808 cases (mean age 58.85 years, 82.8% female), 267 (7.0%) died. JAKi therapies (41.2%), followed by TNFi (37.7%), IL-1i (12.2%), IL-6i (4.1%) and Anti-CD20 (3%) were reported. Risk factors associated with COVID-19-related death in RA patients were age (odds ratio [OR]: 1.06; 95% confidence interval [CI]: 1.05–1.08; p ​< ​0.01), male sex (1.71, 1.26–2.33; p ​= ​0.01) and anti-CD20 therapies (5.05; 1.40–18.19; p ​= ​0.013). With TNFi conference, anti-CD20 was still a risk predictor (4.29; 2.39–7.70; p ​< ​0.01). Other DMARDs except for anti-CD20, did not confer a significant association with mortality, compared with csDMARDs or TNFi. Individual JAKi showed no obvious difference in the risk of death, compared with csDMARDs or TNFis.

Conclusions

Conclusions Using FAERS open access data for risk prediction of death, anti-CD20 therapies were recognized as a risk factor for COVID-19-related fatalities among RA patients, other immunomodulatory therapies were not associated with mortality, compared with csDMARDs or TNFis.

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类风湿关节炎患者的免疫调节疗法与 COVID-19 死亡率之间的关系:对 FDA 不良事件报告系统的分析
背景COVID-19大流行严重影响了类风湿关节炎和其他风湿性疾病患者。我们的研究旨在利用国际食品药品管理局(FDA)的不良事件报告系统(FAERS),探讨类风湿关节炎(RA)患者中与 COVID-19 相关死亡的相关因素,尤其是免疫调节疗法。研究结果为与 COVID-19 相关的死亡。在多变量逻辑回归中,年龄、性别、地区、事件发生日期和免疫调节药物分类被列为共变因素。结果 在所有 3808 例病例(平均年龄 58.85 岁,82.8% 为女性)中,有 267 例(7.0%)死亡。据报道,JAKi疗法占41.2%,其次是TNFi疗法(37.7%)、IL-1i疗法(12.2%)、IL-6i疗法(4.1%)和抗CD20疗法(3%)。与COVID-19相关的RA患者死亡的风险因素是年龄(几率比[OR]:1.06;95% 置信区间 [CI]:1.05-1.08; p < 0.01)、男性(1.71, 1.26-2.33; p = 0.01)和抗CD20疗法(5.05; 1.40-18.19; p = 0.013)。在 TNFi 会议上,抗 CD20 仍是一个风险预测因子(4.29;2.39-7.70;p <;0.01)。与csDMARDs或TNFi相比,除抗CD20外,其他DMARDs与死亡率无显著相关性。结论 使用FAERS开放数据进行死亡风险预测,抗CD20疗法被认为是RA患者COVID-19相关死亡的风险因素,与csDMARDs或TNFis相比,其他免疫调节疗法与死亡率无关。
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