Ferreira-da-Silva Renato, Silva Lurdes, Costa-Santos Cristina, Morato Manuela, Polónia Jorge Junqueira, Ribeiro-Vaz Inês, Pinto Manuela, Pereira Marta, Figueira Inês Marques, Baptista Sofia, Farinha Helena, Falcão Fátima, Mirco Ana, Calixto Liliana, Melo Madalena
Porto Pharmacovigilance Centre, Faculty of Medicine of the University of Porto, Porto, Portugal.
Department of Community Medicine, Information and Health Decision Sciences (MEDCIDS), Faculty of Medicine of the University of Porto, Porto, Portugal.
Pharmacol Rep. 2025 Apr 25. doi: 10.1007/s43440-025-00729-2.
Molnupiravir, approved for treating mild to moderate COVID-19 in adults, aims to reduce hospitalisation and mortality rates. Although it was withdrawn from the market after the present study was conducted, understanding its long-term effects remains pertinent. We aimed to assess the real-world effectiveness and safety of molnupiravir in high-risk COVID-19 outpatients.
This prospective, multicenter, noninterventional, postmarketing cohort study enrolled high-risk COVID-19 outpatients with mild to moderate COVID-19, eligible under national prescribing criteria, who initiated molnupiravir within five days of symptom onset and were ineligible for first-line antiviral therapy. Patients were consecutively enrolled from eight Portuguese study sites and monitored for three months. Effectiveness was assessed by all-cause mortality and hospitalisation through day 29. Safety was evaluated by the incidence, severity, and causality of adverse events (AE), coded using MedDRA terminology and assessed via the WHO-UMC system. Data were collected through structured patient questionnaires and electronic health records. Statistical analysis was descriptive; proportions were reported with 95% confidence intervals (CI), and comparisons between groups were performed using appropriate statistical tests.
By day 29 post-treatment initiation, no deaths were reported (n = 0; 0%; 95%CI = [0,26]), and all patients were either at home or institutionalised, with favourable outcomes. Out of the 12 patients enrolled, eight (67%; 95%CI = [35,90]) reported at least one AE, with the median time to the first AE being five days (range 5-7 days). Half of the patients (n = 6; 95%CI = [21,79]) reported AE deemed possibly or probably related to molnupiravir, involving nausea (25%), dizziness (17%), bitter taste (17%), and headache (17%). These AE were more commonly observed in older individuals and those overweight, indicating a potential influence of these factors on AE occurrence.
Molnupiravir appears to show good safety and effectiveness, offering an alternative for high-risk COVID-19 outpatients ineligible for first-line therapy. Despite its market withdrawal, ongoing research into its long-term effects is crucial to potentially repurpose it for other viral infections.
莫努匹拉韦已被批准用于治疗成人轻至中度新冠肺炎,旨在降低住院率和死亡率。尽管在本研究开展后它已退出市场,但了解其长期影响仍具有相关性。我们旨在评估莫努匹拉韦在高危新冠肺炎门诊患者中的真实世界有效性和安全性。
这项前瞻性、多中心、非干预性的上市后队列研究纳入了符合国家处方标准的轻至中度新冠肺炎高危门诊患者,这些患者在症状出现后五天内开始使用莫努匹拉韦,且不符合一线抗病毒治疗条件。患者从葡萄牙的八个研究地点连续入组,并接受为期三个月的监测。通过第29天的全因死亡率和住院率评估有效性。通过不良事件(AE)的发生率、严重程度和因果关系评估安全性,使用MedDRA术语进行编码,并通过WHO-UMC系统进行评估。数据通过结构化患者问卷和电子健康记录收集。统计分析为描述性分析;报告比例时给出95%置信区间(CI),组间比较使用适当的统计检验。
在开始治疗后的第29天,未报告死亡病例(n = 0;0%;95%CI = [0,26]),所有患者均在家中或住院,预后良好。在纳入的12名患者中,8名(67%;95%CI = [35,90])报告了至少一次AE,首次AE的中位时间为5天(范围5 - 7天)。一半的患者(n = 6;95%CI = [21,79])报告了被认为可能或很可能与莫努匹拉韦相关的AE,包括恶心(25%)、头晕(17%)、口苦(17%)和头痛(17%)。这些AE在老年人和超重者中更常见,表明这些因素可能对AE的发生有影响。
莫努匹拉韦似乎显示出良好的安全性和有效性,为不符合一线治疗条件的高危新冠肺炎门诊患者提供了一种选择。尽管它已退出市场,但对其长期影响的持续研究对于将其重新用于其他病毒感染可能至关重要。
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