Anti-CD14 Treatment in Patients With Severe COVID-19 Clinical and Biological Effects in a Phase 2 Randomized Open-Label Adaptive Platform Clinical Trial

CHEST critical care Pub Date : 2025-03-01 DOI:10.1016/j.chstcc.2024.100117

F. Linzee Mabrey MD, MSc , Thomas R. Martin MD , Carolyn S. Calfee MD , Kathleen D. Liu MD , Benjamin LaCombe BS , Lamorna Brown-Swigart PhD , Andrea Discacciati PhD , Martin Eklund PhD , Susan R. Heckbert MD , Michael A. Matthay MD , Laura Esserman MD , Mark M. Wurfel MD, PhD

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Abstract

Background

Cluster of differentiation 14 (CD14)-dependent innate immunity contributes to poor outcomes in COVID-19 pneumonia.

Research Question

What are the clinical and biological effects of a blocking anti-CD14 monoclonal antibody (IC14) for treatment of severe COVID-19 pneumonia and what is the usefulness of a biomarker of CD14 pathway activation in predicting outcome?

Study Design And Methods

We report a preplanned secondary analysis of the Investigation of Serial Studies to Predict Your Therapeutic Response With Imaging and Molecular Analysis to Coronavirus Disease of 2019 (I-SPY COVID) trial, which enrolled hospitalized patients with severe COVID-19 pneumonia who required high-level respiratory support at 19 medical centers in the United States. Participants were randomized to receive either IV IC14 (4 mg/kg on day 1, then 2 mg/kg on days 2-4; n = 67) or standard care (n = 76). Primary end points included time to recovery, defined as the first 2-day period with ≤ 6 L/min of oxygen, and mortality. In predefined secondary analyses, we tested the association between IC14 treatment and mortality in patients with high or low baseline plasma presepsin, a biomarker of CD14 pathway activity, and the effects of IC14 on plasma biomarkers of pharmacodynamics, injury, and inflammation.

Results

IC14 treatment did not improve time to recovery or 28-day mortality in the overall population, and the trial was stopped because of meeting futility criteria for the time-to-recovery end point. However, a predefined subgroup analysis showed that IC14 treatment was associated with a numerical reduction in 28-day mortality in participants with high (above median) baseline presepsin levels (n = 47; hazard ratio for mortality [HRm], 0.52; 95% credible interval, 0.22-1.22; posterior probability [Pr] HRm < 1 (Pr(HRm < 1 | data)) = 0.93). IC14 treatment increased plasma sCD14, a pharmacodynamic marker, and decreased plasma inflammatory biomarkers, including IL-8, receptor for advanced glycation end products, vascular endothelial growth factor, and presepsin.

Interpretation

Although IC14 treatment did not improve overall clinical outcomes, this new secondary analysis showed that IC14 produced the expected pharmacodynamic and biological effects and that baseline plasma presepsin concentrations may identify patients likely to respond to IC14 treatment. Further trials are needed to determine the efficacy of IC14 treatment in acute lung injury and the value of presepsin to identify patients most likely to respond.

Clinical Trial Registry

ClinicalTrials.gov; No.: NCT04488081; URL: www.clinicaltrials.gov

查看原文本刊更多论文

在一项 2 期随机开放标签自适应平台临床试验中，对重度 COVID-19 患者进行抗 CD14 治疗的临床和生物效应研究

CD14依赖性先天免疫与COVID-19肺炎预后不良有关。阻断性抗CD14单克隆抗体（IC14）治疗重症COVID-19肺炎的临床和生物学效应是什么？ CD14途径激活的生物标志物在预测预后方面的有用性是什么？研究设计和方法我们报告了一项预先计划的二次分析，该研究是通过影像学和分子分析预测2019年冠状病毒病（I-SPY COVID）治疗反应的系列研究调查，该试验纳入了美国19个医疗中心的重症COVID-19肺炎住院患者，这些患者需要高水平的呼吸支持。参与者随机接受IV IC14(第1天为4mg /kg，第2-4天为2mg /kg；N = 67)或标准护理（N = 76）。主要终点包括恢复时间（定义为前2天血氧≤6 L/min）和死亡率。在预先确定的二次分析中，我们测试了IC14治疗与基线血浆前压素（CD14通路活性的生物标志物）高或低的患者死亡率之间的关系，以及IC14对药理学、损伤和炎症的血浆生物标志物的影响。结果ic14治疗没有改善总体人群的恢复时间或28天死亡率，由于满足恢复时间终点的无效标准，该试验停止。然而，预先确定的亚组分析显示，IC14治疗与基线高血压素水平高（高于中位数）的参与者28天死亡率的数值降低相关(n = 47；死亡率风险比[HRm]， 0.52；95%可信区间为0.22-1.22；后验概率[r] h & t；1 (r)；1 |数据))= 0.93)。IC14治疗增加了血浆sCD14（一种药效学标志物），降低了血浆炎症生物标志物，包括IL-8（晚期糖基化终产物受体）、血管内皮生长因子和presepsin。虽然IC14治疗并没有改善总体临床结果，但这项新的二级分析表明，IC14产生了预期的药效学和生物学效应，并且基线血浆前压素浓度可以识别可能对IC14治疗有反应的患者。需要进一步的试验来确定IC14治疗急性肺损伤的疗效，以及压菌素在识别最有可能对其有反应的患者中的价值。ClinicalTrial RegistryClinicalTrials.gov；否。: NCT04488081;URL: www.clinicaltrials.gov

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来源期刊

CHEST critical care Critical Care and Intensive Care Medicine, Pulmonary and Respiratory Medicine

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