TrippBio, Inc., Jacksonville, FL 32256, USA.
PCMC's PGI Yashwantrao Chavan Memorial Hospital, Pune 411018, India.
Viruses. 2023 Jul 6;15(7):1508. doi: 10.3390/v15071508.
Probenecid is an orally bioavailable, uricosuric agent that was first approved in 1951 for the treatment of gout, but was later found to have potent, broad-spectrum antiviral activity against several respiratory viruses including SARS-CoV-2. We conducted a phase 2 randomized, placebo-controlled, single-blind, dose-range finding study in non-hospitalized patients with symptomatic, mild-to-moderate COVID-19. Patients were randomly assigned in a 1:1:1 ratio to receive either 500 mg of probenecid, 1000 mg of probenecid, or a matching placebo every 12 h for five days. The patients' COVID-19 viral load hospitalization, or death from any cause through day 28, as well as safety, were evaluated. COVID-19-related symptoms were assessed at baseline, and on days 3, 5, 10, 15, and 28. The primary endpoints of the study were time to first negative SARS-CoV-2 viral test (or viral clearance) and the proportion of patients that were symptom-free at day 5. A total of 75 patients were randomized, with 25 patients in each group. All of the patients completed the study as planned with no hospitalizations or deaths being reported. The median time to viral clearance was significantly shorter for the probenecid 1000 mg group than for placebo (7 days vs. 11 days, respectively; < 0.0001), and for the probenecid 500 mg group versus placebo (9 days vs. 11 days, respectively; < 0.0001). In addition, the median time to viral clearance was significantly shorter for the probenecid 1000 mg group than for the probenecid 500 mg group (7 days vs. 9 days, respectively; < 0.0001). All patients reported at least one COVID-19-related symptom on days 3 and 5; however, on day 10, a significantly greater proportion of patients receiving probenecid 1000 mg reported the complete resolution of symptoms versus placebo (68% vs. 20%, respectively; = 0.0006), as well as for those receiving probenecid 500 mg versus placebo (56% vs. 20%, respectively, = 0.0087). The incidence of adverse events during treatment was similar across all groups for any adverse event, and was 12%. All events were mild with no serious adverse events reported and no discontinuations due to an adverse event. The treatment of patients with symptomatic, mild-to-moderate COVID-19 with probenecid resulted in a significant, dose-dependent decrease in the time to viral clearance and a significantly higher proportion of patients reporting complete symptom resolution by day 10. (Supported by TrippBio; ClinicalTrials.gov number, NCT05442983 and Clinical Trials Registry India number CTRI/2022/07/043726).
丙磺舒是一种口服生物利用度高的促尿酸排泄药物,于 1951 年首次获批用于治疗痛风,但后来发现它对包括 SARS-CoV-2 在内的多种呼吸道病毒具有强大的广谱抗病毒活性。我们在非住院的、有症状的轻症至中度 COVID-19 患者中进行了一项 2 期随机、安慰剂对照、单盲、剂量范围确定研究。患者以 1:1:1 的比例随机分配,接受 500 mg 丙磺舒、1000 mg 丙磺舒或匹配的安慰剂,每 12 小时一次,共 5 天。评估了患者的 COVID-19 病毒载量、住院、或任何原因导致的死亡至第 28 天,以及安全性。评估 COVID-19 相关症状,在基线时以及第 3、5、10、15 和 28 天进行评估。研究的主要终点是首次 SARS-CoV-2 病毒检测(或病毒清除)的时间,以及第 5 天无症状患者的比例。共随机分配了 75 名患者,每组 25 名。所有患者均按计划完成了研究,无住院或死亡报告。丙磺舒 1000 mg 组与安慰剂组相比,病毒清除的中位时间显著缩短(分别为 7 天和 11 天;<0.0001),丙磺舒 500 mg 组与安慰剂组相比,病毒清除的中位时间也显著缩短(分别为 9 天和 11 天;<0.0001)。此外,丙磺舒 1000 mg 组与丙磺舒 500 mg 组相比,病毒清除的中位时间也显著缩短(分别为 7 天和 9 天;<0.0001)。所有患者在第 3 天和第 5 天都至少报告了一种 COVID-19 相关症状;然而,在第 10 天,接受丙磺舒 1000 mg 治疗的患者报告症状完全缓解的比例明显高于安慰剂组(分别为 68%和 20%;=0.0006),接受丙磺舒 500 mg 治疗的患者报告症状完全缓解的比例也明显高于安慰剂组(分别为 56%和 20%;=0.0087)。各组在任何不良事件的治疗期间不良反应发生率相似,均为 12%。所有事件均为轻度,无严重不良事件报告,也无因不良事件而停药。在有症状的轻症至中度 COVID-19 患者中使用丙磺舒治疗可显著缩短病毒清除时间,并显著提高第 10 天报告完全症状缓解的患者比例,且呈剂量依赖性。(由 TrippBio 公司资助;ClinicalTrials.gov 编号:NCT05442983 和 Clinical Trials Registry India 编号:CTRI/2022/07/043726)
