Delayed inflammation decrease is associated with mortality in Tocilizumab-treated critically ill SARS-CoV-2 patients: A retrospective matched-cohort analysis.

IF 2.8 4区 医学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY Innate Immunity Pub Date : 2022-01-01 Epub Date: 2022-01-28 DOI:10.1177/17534259211064602
Tomas Urbina, Jean-Rémi Lavillegrand, Marc Garnier, Arsene Mekinian, Jerome Pacanowski, Nathalie Mario, Guillaume Dumas, Geoffroy Hariri, Antoine Pilon, Lucie Darrivère, Muriel Fartoukh, Bertrand Guidet, Eric Maury, Judith Leblanc, Yannick Chantran, Olivier Fain, Karine Lacombe, Guillaume Voiriot, Hafid Ait-Oufella
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引用次数: 1

Abstract

Little is known about the immuno-inflammatory response to Tocilizumab and its association with outcome in critically-ill SARS-CoV2 pneumonia. In this multicenter retrospective cohort of SARS-CoV-2 patients admitted to three intensive care units between March and April 2020, we matched on gender and SAPS II 21 Tocilizumab-treated patients to 42 non-treated patients. Need for mechanical ventilation was 76% versus 79%. IL-6, C-reactive protein, and fibrinogen had been collected within the first days of admission (T1), 3 d (T2) and 7 d (T3) later. Tocilizumab-treated patients had persistently higher IL-6 plasma levels and persistently lower C-Reactive protein and fibrinogen levels. Among Tocilizumab-treated patients, baseline levels of inflammatory biomarkers were not different according to outcome. Conversely, C-reactive protein and fibrinogen decrease was delayed in non-survivors. C-Reactive protein decreased at T1 in survivors (45 [30-98] vs 170 [69-204] mg/l, P < 0.001) but only at T2 in non-survivors (37 [13-74] vs 277 [235-288], P = 0.03). Fibrinogen decreased at T2 in survivors (4.11 [3.58-4.69] vs 614 [5.61-7.85] g/l, P = 0.005) but not in non-survivors (4.79 [4.12-7.58] vs 7.24 [6.22-9.24] g/l, P = 0.125). Tocilizumab treatment was thus associated with a persistent both increase in plasma IL-6, and decrease in C-reactive protein and fibrinogen. Among Tocilizumab-treated patients, the decrease in inflammatory biomarkers was delayed in non-survivors.

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托珠单抗治疗的重症SARS-CoV-2患者的延迟炎症减轻与死亡率相关:一项回顾性匹配队列分析
对于托珠单抗的免疫炎症反应及其与危重SARS-CoV2肺炎预后的关系知之甚少。在2020年3月至4月期间入住3个重症监护病房的SARS-CoV-2患者的多中心回顾性队列中,我们将21名接受tocilizumab治疗的患者与42名未接受治疗的患者进行性别和SAPS II匹配。需要机械通气的比例分别为76%和79%。在入院第1天(T1)、第3天(T2)和第7天(T3)采集IL-6、c反应蛋白和纤维蛋白原。tocilizumab治疗的患者血浆IL-6水平持续升高,c反应蛋白和纤维蛋白原水平持续降低。在接受tocilizumab治疗的患者中,炎症生物标志物的基线水平根据结果没有差异。相反,c反应蛋白和纤维蛋白原的减少在非幸存者中延迟。c -反应蛋白在T1时降低(45 [30-98]vs 170 [69-204] mg/l, P = 0.03)。在T2时,幸存者的纤维蛋白原降低(4.11 [3.58-4.69]vs 614 [5.61-7.85] g/l, P = 0.005),而非幸存者的纤维蛋白原降低(4.79 [4.12-7.58]vs 7.24 [6.22-9.24] g/l, P = 0.125)。因此,托珠单抗治疗与血浆IL-6持续升高、c反应蛋白和纤维蛋白原持续降低相关。在接受tocilizumab治疗的患者中,炎症生物标志物的下降在非幸存者中延迟。
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来源期刊
Innate Immunity
Innate Immunity 生物-免疫学
CiteScore
7.20
自引率
0.00%
发文量
20
审稿时长
6-12 weeks
期刊介绍: Innate Immunity is a highly ranked, peer-reviewed scholarly journal and is the official journal of the International Endotoxin & Innate Immunity Society (IEIIS). The journal welcomes manuscripts from researchers actively working on all aspects of innate immunity including biologically active bacterial, viral, fungal, parasitic, and plant components, as well as relevant cells, their receptors, signaling pathways, and induced mediators. The aim of the Journal is to provide a single, interdisciplinary forum for the dissemination of new information on innate immunity in humans, animals, and plants to researchers. The Journal creates a vehicle for the publication of articles encompassing all areas of research, basic, applied, and clinical. The subject areas of interest include, but are not limited to, research in biochemistry, biophysics, cell biology, chemistry, clinical medicine, immunology, infectious disease, microbiology, molecular biology, and pharmacology.
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