Pilkington Victoria, Pepperrell Toby, Hill Andrew
Faculty of Medicine, Imperial College London, London, UK.
MetaVirology LTD, London, UK.
J Virus Erad. 2020 Apr 30;6(2):45-51. doi: 10.1016/S2055-6640(20)30016-9.
Repurposing broad-spectrum antivirals is an immediate treatment opportunity for 2019 coronavirus disease (COVID-19). Favipiravir is an antiviral previously indicated for influenza and Ebola, which has shown some promise in early trials for treatment of COVID-19. We aim to review existing favipiravir safety evidence, which is vital to informing the potential future use of favipiravir in COVID-19.
A search was conducted across EMBASE and MEDLINE databases, supplemented by relevant grey-literature and ClinicalTrials.gov. All studies assessing the use of favipiravir in humans by 27 March 2020 were considered for inclusion. Further analysis of available safety data from phase 2 and 3 studies was undertaken. Data extracted were adverse events (AEs) grade 1-4, serious AEs and discontinuation for AEs. Specific AEs of interest highlighted in early-phase studies, including gastrointestinal AEs and hyperuricaemia, were also examined.
Twenty-nine studies were identified as potential sources of evidence of the clinical safety of favipiravir. Six were phase 2 and 3 studies reporting relevant safety data for statistical comparison, representing a total of 4299 participants, an estimated 175 person-years-of-follow-up (PYFU). Comparator drugs were oseltamivir, umifenovir, lopinavir/ritonavir or placebo. Study follow-up was between 5 and 21 days. The proportions of grade 1-4 AEs on favipiravir was 28.2% 28.4% ( = n.s.) in the comparison arms. The proportion of discontinuations due to AEs on favipiravir was 1.1% 1.2% ( = n.s.) in the comparison arms. For serious AEs the proportion was 0.4% in both arms ( = n.s.). There were significantly fewer gastrointestinal AEs occurring on favipiravir comparators [8.7% 11.5%; = 0.003]. Favipiravir showed significantly more uric acid elevations than comparators [5.8% 1.3%; <0.0001].
Favipiravir demonstrates a favourable safety profile regarding total and serious AEs. However, safety concerns remain: hyperuricaemia, teratogenicity and QTc prolongation have not yet been adequately studied. Favipiravir may be safe and tolerable in short-term use, but more evidence is needed to assess the longer-term effects of treatment. Given the limitations of the evidence and unresolved safety concerns, caution is warranted in the widespread use of favipiravir against pandemic COVID-19.
重新利用广谱抗病毒药物是治疗2019冠状病毒病(COVID-19)的一个即时治疗机会。法匹拉韦是一种先前被用于治疗流感和埃博拉的抗病毒药物,在治疗COVID-19的早期试验中显示出了一些前景。我们旨在回顾现有的法匹拉韦安全性证据,这对于指导法匹拉韦未来在COVID-19中的潜在应用至关重要。
在EMBASE和MEDLINE数据库中进行了检索,并辅以相关的灰色文献和ClinicalTrials.gov。纳入所有在2020年3月27日前评估法匹拉韦在人类中使用情况的研究。对来自2期和3期研究的可用安全性数据进行了进一步分析。提取的数据包括1-4级不良事件(AE)、严重AE以及因AE而停药的情况。还检查了早期研究中突出的特定感兴趣的AE,包括胃肠道AE和高尿酸血症。
确定了29项研究作为法匹拉韦临床安全性证据的潜在来源。其中6项是2期和3期研究,报告了相关安全性数据用于统计比较,共有4299名参与者,估计随访175人年(PYFU)。对照药物为奥司他韦、乌米芬诺尔、洛匹那韦/利托那韦或安慰剂。研究随访时间为5至21天。在比较组中,法匹拉韦组1-4级AE的比例为28.2%对28.4%(P=无显著差异)。在比较组中,法匹拉韦组因AE停药的比例为1.1%对1.2%(P=无显著差异)。对于严重AE,两组的比例均为0.4%(P=无显著差异)。法匹拉韦组发生的胃肠道AE明显少于对照组[8.7%对11.5%;P=0.003]。法匹拉韦组尿酸升高的情况明显多于对照组[5.8%对1.3%;P<0.0001]。
法匹拉韦在总体和严重AE方面显示出良好的安全性。然而,仍存在安全问题:高尿酸血症、致畸性和QTc延长尚未得到充分研究。法匹拉韦在短期使用中可能是安全且可耐受的,但需要更多证据来评估治疗的长期效果。鉴于证据的局限性和未解决的安全问题,在广泛使用法匹拉韦治疗大流行的COVID-19时应谨慎。
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