受体相互作用蛋白激酶 1(RIPK1)抑制剂 eclitasertib(SAR443122)在重症 COVID-19 患者中的免疫调节和临床疗效:一项 1b 期、随机、双盲、安慰剂对照研究。
Immunomodulatory and clinical effects of receptor-interacting protein kinase 1 (RIPK1) inhibitor eclitasertib (SAR443122) in patients with severe COVID-19: a phase 1b, randomized, double-blinded, placebo-controlled study.
机构信息
Translational Medicine and Early Development (TMED)/Clinical Pharmacology (TMCP) and Neuro and Neuro-Immunology, 371 Rue du Professeur Blayac, Sanofi, Montpellier, 34080, France.
TMED Pharmacokinetics Dynamics and Metabolism, Sanofi, Montpellier, France.
出版信息
Respir Res. 2024 Feb 28;25(1):107. doi: 10.1186/s12931-024-02670-z.
BACKGROUND
Targeting receptor-interacting serine/threonine protein kinase 1 could mitigate the devastating sequelae of the hyperinflammatory state observed in severe cases of COVID-19. This study explored the immunomodulatory and clinical effects of the receptor-interacting serine/threonine protein kinase 1 inhibitor SAR443122 (eclitasertib) in patients with severe COVID-19.
METHODS
In this Phase 1b, double-blinded, placebo-controlled study (NCT04469621) a total of 82 patients were screened, of whom 68 patients were eligible and randomized (2:1) to receive eclitasertib 600 mg (300 mg twice daily) or placebo up to 14 days. Primary outcome was relative change in C-reactive protein from baseline to Day 7. Time to clinical improvement using 7-point ordinal scale, ventilator/respiratory failure-free days, change in SpO/FiO ratio, and biomarkers of severe COVID-19 were explored.
RESULTS
Geometric mean ratio (point estimate [90% confidence interval]) of the relative change from baseline in C-reactive protein with eclitasertib vs. placebo on Day 7 was 0.85 (0.49-1.45; p = 0.30). Median time to 50% decrease in C-reactive protein from baseline was 3 days vs. 5 days (p = 0.056) with eclitasertib vs. placebo. Median time to ≥ 2-point improvement on 7-point clinical symptoms scale was 8 days vs. 10 days with eclitasertib vs. placebo (p = 0.38). Mean ventilator/respiratory failure-free days, change in baseline-adjusted SpO/FiO ratio, and clinical biomarkers showed consistent numerical improvements with eclitasertib vs. placebo. The most frequently reported treatment-emergent adverse events were gastrointestinal disorders and condition aggravated/worsened COVID-19 pneumonia.
CONCLUSIONS
Eclitasertib was well tolerated with consistent trends toward more rapid resolution of inflammatory biomarkers and clinical improvement in severe COVID-19 patients than placebo.
GOV IDENTIFIER
NCT04469621, first posted on clinicaltrials.gov on July 14, 2020.
背景
靶向受体相互作用丝氨酸/苏氨酸蛋白激酶 1 可能减轻 COVID-19 重症患者观察到的过度炎症状态的破坏性后果。本研究探讨了受体相互作用丝氨酸/苏氨酸蛋白激酶 1 抑制剂 SAR443122(eclitasertib)在重症 COVID-19 患者中的免疫调节和临床效果。
方法
在这项 1b 期、双盲、安慰剂对照研究(NCT04469621)中,共筛选了 82 名患者,其中 68 名符合条件并随机(2:1)接受 eclitasertib 600mg(每日两次 300mg)或安慰剂治疗,最长 14 天。主要结局是从基线到第 7 天 C-反应蛋白的相对变化。使用 7 点序贯量表探索临床改善的时间、无呼吸机/呼吸衰竭天数、SpO/FiO 比值变化和严重 COVID-19 的生物标志物。
结果
eclitasertib 组与安慰剂组第 7 天 C-反应蛋白的几何均数比值(点估计值[90%置信区间])为 0.85(0.49-1.45;p=0.30)。eclitasertib 组与安慰剂组相比,从基线开始 C-反应蛋白降低 50%的中位时间分别为 3 天和 5 天(p=0.056)。eclitasertib 组与安慰剂组相比,7 点临床症状量表至少改善 2 分的中位时间分别为 8 天和 10 天(p=0.38)。呼吸机/呼吸衰竭无天数、基线调整后 SpO/FiO 比值变化和临床生物标志物的平均值显示出与 eclitasertib 相比一致的数值改善。最常报告的治疗后不良事件是胃肠道疾病和加重/恶化的 COVID-19 肺炎。
结论
eclitasertib 耐受性良好,与安慰剂相比,重症 COVID-19 患者的炎症标志物快速缓解和临床改善的趋势更为明显。
政府标识符
NCT04469621,于 2020 年 7 月 14 日首次在 clinicaltrials.gov 上公布。
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