Clinical Research Center, Nagasaki University Hospital, Nagasaki, Japan.
Department of Respiratory Medicine, Nagasaki University Hospital, Nagasaki, Japan.
Trials. 2021 Apr 28;22(1):309. doi: 10.1186/s13063-021-05282-w.
The aim of this trial is to evaluate the antiviral efficacy, clinical efficacy, and safety of nelfinavir in patients with asymptomatic and mild COVID-19.
The study is designed as a multicenter, open-label, blinded outcome assessment, parallel group, investigator-initiated, exploratory, randomized (1:1 ratio) controlled clinical trial.
Asymptomatic and mild COVID-19 patients will be enrolled in 10 university and teaching hospitals in Japan. The inclusion and exclusion criteria are as follows: Inclusion criteria: (1) Japanese male or female patients aged ≥ 20 years (2) SARS-CoV-2 detected from a respiratory tract specimen (e.g., nasopharyngeal swab or saliva) using PCR, LAMP, or an antigen test within 3 days before obtaining the informed consent (3) Provide informed consent Exclusion criteria: (1) Symptoms developed ≥ 8 days prior to enrolment (2) SpO < 96 % (room air) (3) Any of the following screening criteria: a) ALT or AST ≥ 5 × upper limit of the reference range b) Child-Pugh class B or C c) Serum creatinine ≥ 2 × upper limit of the reference range and creatinine clearance < 30 mL/min (4) Poorly controlled diabetes (random blood glucose ≥ 200 mg/dL or HbA1c ≥ 7.0%, despite treatment) (5) Unsuitable serious complications based on the assessment of either the principal investigator or the sub-investigator (6) Hemophiliac or patients with a marked hemorrhagic tendency (7) Severe diarrhea (8) Hypersensitivity to the investigational drug (9) Breastfeeding or pregnancy (10) With childbearing potential and rejecting contraceptive methods during the study period from the initial administration of the investigational drug (11) Receiving rifampicin within the previous 2 weeks (12) Participated in other clinical trials and received drugs within the previous 12 weeks (13) Undergoing treatment for HIV infection (14) History of SARS-CoV-2 vaccination or wishes to be vaccinated against SARS-CoV-2 (15) Deemed inappropriate (for miscellaneous reasons) based on the assessment of either the principal investigator or the sub-investigator INTERVENTION AND COMPARATOR: Patients who meet the inclusion criteria and do not meet any of the exclusion criteria will be randomized to either the nelfinavir group or the symptomatic treatment group. The nelfinavir group will be administered 750 mg of nelfinavir orally, three times daily for 14 days (treatment period). However, if a participant tests negative on two consecutive PCR tests of saliva samples, administration of the investigational drug for that participant can be discontinued at the discretion of the investigators. The symptomatic treatment group will not be administered the investigational drug, but all other study procedures and conditions will be the same for both groups for the duration of the treatment period. After the treatment period of 14 days, each group will be followed up for 14 days (observational period).
The primary endpoint is the time to negative conversion of SARS-CoV-2. During the study period from Day 1 to Day 28, two consecutive negative PCR results of saliva samples will be considered as the negative conversion of the virus. The secondary efficacy endpoints are as follows: For patients with both asymptomatic and mild disease: area under the curve of viral load, half decay period of viral load, body temperature at each time point, all-cause mortality, incidence rate of pneumonia, percentage of patients with newly developed pneumonia, rate of oxygen administration, and the percentage of patients who require oxygen administration. For asymptomatic patients: incidence of symptomatic COVID-19, incidence of fever (≥ 37.0 °C for two consecutive days), incidence of cough For patients with mild disease: incidence of defervescence (< 37.0 °C), incidence of recovery from clinical symptoms, incidence of improvement of each symptom The secondary safety endpoints are adverse events and clinical examinations.
Patients will be randomized to either the nelfinavir group or the symptomatic treatment group using the electric data capture system (1:1 ratio, dynamic allocation based on severity [asymptomatic], and age [< 60 years]).
BLINDING (MASKING): Only the assessors of the primary outcome will be blinded (blinded outcome assessment).
NUMBERS TO BE RANDOMIZED (SAMPLE SIZE): The sample size was determined based on our power analysis to reject the null hypothesis, S (t | z =1) = S (t | z = 0) where S is a survival function, t is time to negative conversion, and z denotes randomization group, by the log-rank test with a two-sided p value of 0.05. We estimated viral dynamic parameters by fitting a nonlinear mixed-effects model to reported viral load data, and simulated our primary endpoint from viral-load time-courses that were realized from sets of viral dynamics parameters sampled from the estimated probability distribution of the parameters (sample size: 2000; 1000 each for randomization group). From this estimation of the hazard ratio between the randomization groups for the event of negative conversion using this simulation dataset, the required number of events for rejecting our null hypothesis with a power of 0.80 felled 97.345 by plugging the estimated hazard ratio, 1.79, in Freedman's equation. Therefore, we decided the required number of randomizations to be 120 after consideration of the frequency of censoring and the anticipated rate of withdrawal caused by factors such as withdrawal of consent.
Protocol version 6.0 of February 12, 2021. Recruitment started on July 22, 2020 and is anticipated to be completed by March 31, 2022.
This trial was registered in Japan Registry of Clinical Trials (jRCT) ( jRCT2071200023 ) on 21 July 21, 2020.
The full protocol is attached as an additional file, accessible from the Trials website (Additional file 1). In the interest in expediting dissemination of this material, the familiar formatting has been eliminated; this Letter serves as a summary of the key elements of the full protocol. The study protocol has been reported in accordance with the Standard Protocol Items: Recommendations for Clinical Interventional Trials (SPIRIT) guidelines (Additional file 2).
本试验旨在评估奈非那韦在无症状和轻症 COVID-19 患者中的抗病毒疗效、临床疗效和安全性。
本研究设计为多中心、开放标签、盲终点评估、平行组、研究者发起、探索性、随机(1:1 比例)对照临床试验。
将在日本的 10 所大学和教学医院招募无症状和轻症 COVID-19 患者。纳入和排除标准如下:纳入标准:(1)年龄≥20 岁的日本男性或女性患者(2)在获得知情同意前 3 天内,通过 PCR、LAMP 或抗原检测从呼吸道标本(如鼻咽拭子或唾液)中检测到 SARS-CoV-2(3)提供知情同意。排除标准:(1)入组前症状出现≥8 天(2)SpO <96%(空气)(3)以下任何一项筛选标准:a)ALT 或 AST≥5×参考范围上限 b)Child-Pugh 分级 B 或 C c)血清肌酐≥2×参考范围上限且肌酐清除率<30 mL/min(4)控制不佳的糖尿病(随机血糖≥200 mg/dL 或 HbA1c≥7.0%,尽管治疗)(5)根据主要研究者或次要研究者的评估,不适合严重并发症(6)血友病或有明显出血倾向的患者(7)严重腹泻(8)对研究药物过敏(9)哺乳期或妊娠(10)具有生育能力并在研究期间(从最初给予研究药物开始)拒绝避孕方法(11)在过去 2 周内接受利福平治疗(12)在过去 12 周内参加过其他临床试验并接受过药物治疗(13)正在接受 HIV 感染治疗(14)SARS-CoV-2 疫苗接种史或希望接种 SARS-CoV-2 疫苗(15)根据主要研究者或次要研究者的评估,认为不适合(因其他原因)。
符合纳入标准且无任何排除标准的患者将被随机分配至奈非那韦组或对症治疗组。奈非那韦组将口服奈非那韦 750 mg,每日 3 次,共 14 天(治疗期)。然而,如果参与者的两份连续唾液样本 PCR 检测均为阴性,则可由研究者决定停止该参与者的研究药物治疗。对症治疗组将不给予研究药物,但在治疗期间,两组的所有其他研究程序和条件均相同。治疗期 14 天后,每组将再随访 14 天(观察期)。
主要终点是 SARS-CoV-2 阴性转换时间。在从第 1 天到第 28 天的研究期间,两次连续的唾液样本 PCR 检测结果均为阴性,被认为是病毒的阴性转换。次要疗效终点如下:对于无症状和轻症疾病患者:病毒载量的曲线下面积、病毒载量的半衰期、各时间点的体温、全因死亡率、肺炎发生率、新发肺炎患者的百分比、氧疗率和需要氧疗的患者的百分比。对于无症状患者:有症状 COVID-19 的发生率、发热(连续 2 天≥37.0°C)的发生率、咳嗽的发生率。对于轻症患者:退热(<37.0°C)的发生率、临床症状的恢复、每个症状的改善发生率。次要安全性终点为不良事件和临床检查。
使用电子数据采集系统(1:1 比例,基于严重程度[无症状]和年龄[<60 岁]的动态分配)将患者随机分配至奈非那韦组或对症治疗组。
盲法(盲终点评估):只有主要结局评估者将被设盲(盲终点评估)。
随机数量(样本量):根据我们的功效分析确定样本量,以拒绝无效假设 S(t|z=1)=S(t|z=0),其中 S 是生存函数,t 是阴性转换时间,z 表示随机分组,通过双侧 p 值为 0.05 的对数秩检验。我们通过拟合非线性混合效应模型来估计病毒动力学参数,并通过从估计的参数概率分布中抽样的病毒载量时间序列来模拟我们的主要终点(样本量:2000;随机分组各 1000)。从使用该模拟数据集对随机分组的阴性转换事件的风险比的估计中,在考虑了截止率和由于退出同意等因素导致的撤回率的情况下,拒绝我们的无效假设所需的事件数为 97.345。因此,我们决定在考虑到截止率和由于退出同意等因素导致的撤回率的情况下,需要随机分配 120 名患者,以达到 80%的功效。
2021 年 2 月 12 日的协议版本 6.0。招募工作于 2020 年 7 月 22 日开始,预计于 2022 年 3 月 31 日完成。
该试验于 2020 年 7 月 21 日在日本临床试验注册处(jRCT)注册(jRCT2071200023)。
完整方案作为附加文件附在试验网站上(附加文件 1)。为了加快传播材料的速度,已经消除了熟悉的格式;此信是完整方案的关键要素摘要。该研究方案已根据标准方案项目:临床试验推荐(SPIRIT)指南(附加文件 2)进行了报告。
