Department of Hematology, Clinical Immunology and Infectious Disease, Ehime University Graduate School of Medicine, Toon, Japan.
Department of Virology I, National Institute of Infectious Diseases, Shinjuku, Japan.
PLoS Negl Trop Dis. 2021 Feb 22;15(2):e0009103. doi: 10.1371/journal.pntd.0009103. eCollection 2021 Feb.
Severe fever with thrombocytopenia syndrome (SFTS) is a bunyavirus infection with high mortality. Favipiravir has shown effectiveness in preventing and treating SFTS virus (SFTSV) infection in animal models. A multicenter non-randomized, uncontrolled single arm trial was conducted to collect data on the safety and the effectiveness of favipiravir in treatment of SFTS patients. All participants received favipiravir orally (first-day loading dose of 1800 mg twice a day followed by 800 mg twice a day for 7-14 days in total). SFTSV RT-PCR and biochemistry tests were performed at designated time points. Outcomes were 28-day mortality, clinical improvement, viral load evolution, and adverse events (AEs). Twenty-six patients were enrolled, of whom 23 were analyzed. Four of these 23 patients died of multi-organ failure within one week (28-day mortality rate: 17.3%). Oral favipiravir was well tolerated in the surviving patients. AEs (abnormal hepatic function and insomnia) occurred in about 20% of the patients. Clinical symptoms improved in all patients who survived from a median of day 2 to day10. SFTSV RNA levels in the patients who died were significantly higher than those in the survivors (p = 0.0029). No viral genomes were detectable in the surviving patients a median of 8 days after favipiravir administration. The 28-day mortality rate in this study was lower than those of the previous studies in Japan. The high frequency of hepatic dysfunction as an AE was observed. However, it was unclear whether this was merely a side effect of favipiravir, because liver disorders are commonly seen in SFTS patients. The results of this trial support the effectiveness of favipiravir for patients with SFTS.
严重发热伴血小板减少综合征(SFTS)是一种布尼亚病毒感染,死亡率很高。在动物模型中,法匹拉韦已被证明对预防和治疗 SFTS 病毒(SFTSV)感染有效。进行了一项多中心、非随机、非对照、单臂试验,以收集法匹拉韦治疗 SFTS 患者的安全性和有效性数据。所有参与者均口服法匹拉韦(第 1 天负荷剂量为 1800mg,每日两次,随后 7-14 天每日两次,共 800mg)。在指定时间点进行 SFTSV RT-PCR 和生化检测。结果为 28 天死亡率、临床改善、病毒载量演变和不良事件(AE)。共纳入 26 例患者,其中 23 例进行了分析。这 23 例患者中有 4 例在一周内死于多器官衰竭(28 天死亡率:17.3%)。存活患者口服法匹拉韦耐受性良好。约 20%的患者出现 AE(肝功能异常和失眠)。所有存活患者的临床症状均在中位数第 2 天至第 10 天改善。死亡患者的 SFTSV RNA 水平明显高于存活患者(p = 0.0029)。在法匹拉韦给药后中位数 8 天,存活患者中均无法检测到病毒基因组。本研究的 28 天死亡率低于日本以前的研究。观察到 AE 中肝功能障碍的发生率较高。然而,尚不清楚这是否仅仅是法匹拉韦的副作用,因为肝功能障碍在 SFTS 患者中很常见。该试验结果支持法匹拉韦对 SFTS 患者的有效性。
