Tocilizumab, sarilumab and anakinra in critically ill patients with COVID-19: a randomised, controlled, open-label, adaptive platform trial.

IF 9 1区医学 Q1 RESPIRATORY SYSTEM

Thorax Pub Date : 2025-05-13 DOI:10.1136/thorax-2024-222488

Lennie Derde,Anthony C Gordon,Paul R Mouncey,Farah Al-Beidh,Kathryn M Rowan,Alistair D Nichol,Yaseen M Arabi,Djillali Annane,Abigail Beane,Richard Beasley,Marc J M Bonten,Charlotte A Bradbury,Frank M Brunkhorst,Adrian Buzgau,Meredith Buxton,Allen C Cheng,Nicola Cooper,Matthew Cove,Olaf L Cremer,Michelle A Detry,Eamon J Duffy,Lise J Estcourt,Mark Fitzgerald,James Galea,Herman Goossens,Rashan Haniffa,Thomas E Hills,David T Huang,Nao Ichihara,Andrew King,François Lamontagne,Patrick R Lawler,Helen L Leavis,Roger J Lewis,Edward Litton,John C Marshall,Florian B Mayr,Daniel F McAuley,Anna McGlothlin,Shay P McGuinness,Bryan J McVerry,Susan C Morpeth,Srinivas Murthy,Mihai G Netea,Kayode Ogungbenro,Katrina Orr,Rachael L Parke,Jane C Parker,Asad E Patanwala,Ville Pettila,Luis Felipe Reyes,Hiroki Saito,Marlene S Santos,Christina T Saunders,Christopher W Seymour,Manu Shankar-Hari,Wendy I Sligl,Alexis F Turgeon,Anne M Turner,Steven Y C Tong,Suvi Vaara,Taryn Youngstein,Ryan Zarychanski,Cameron Green,Alisa M Higgins,Colin J McArthur,Lindsay R Berry,Elizabeth Lorenzi,Scott Berry,Steve A Webb,Derek C Angus,Frank L van de Veerdonk

{"title":"Tocilizumab, sarilumab and anakinra in critically ill patients with COVID-19: a randomised, controlled, open-label, adaptive platform trial.","authors":"Lennie Derde,Anthony C Gordon,Paul R Mouncey,Farah Al-Beidh,Kathryn M Rowan,Alistair D Nichol,Yaseen M Arabi,Djillali Annane,Abigail Beane,Richard Beasley,Marc J M Bonten,Charlotte A Bradbury,Frank M Brunkhorst,Adrian Buzgau,Meredith Buxton,Allen C Cheng,Nicola Cooper,Matthew Cove,Olaf L Cremer,Michelle A Detry,Eamon J Duffy,Lise J Estcourt,Mark Fitzgerald,James Galea,Herman Goossens,Rashan Haniffa,Thomas E Hills,David T Huang,Nao Ichihara,Andrew King,François Lamontagne,Patrick R Lawler,Helen L Leavis,Roger J Lewis,Edward Litton,John C Marshall,Florian B Mayr,Daniel F McAuley,Anna McGlothlin,Shay P McGuinness,Bryan J McVerry,Susan C Morpeth,Srinivas Murthy,Mihai G Netea,Kayode Ogungbenro,Katrina Orr,Rachael L Parke,Jane C Parker,Asad E Patanwala,Ville Pettila,Luis Felipe Reyes,Hiroki Saito,Marlene S Santos,Christina T Saunders,Christopher W Seymour,Manu Shankar-Hari,Wendy I Sligl,Alexis F Turgeon,Anne M Turner,Steven Y C Tong,Suvi Vaara,Taryn Youngstein,Ryan Zarychanski,Cameron Green,Alisa M Higgins,Colin J McArthur,Lindsay R Berry,Elizabeth Lorenzi,Scott Berry,Steve A Webb,Derek C Angus,Frank L van de Veerdonk","doi":"10.1136/thorax-2024-222488","DOIUrl":null,"url":null,"abstract":"INTRODUCTION\r\nTocilizumab improves outcomes in critically ill patients with COVID-19. Whether other immune-modulator strategies are equally effective or better is unknown.\r\n\r\nMETHODS\r\nWe investigated treatment with tocilizumab, sarilumab, anakinra and no immune modulator in these patients. In this ongoing, adaptive platform trial in 133 sites in 9 countries, we randomly assigned patients with allocation ratios dependent on the number of interventions available at each site. The primary outcome was an ordinal scale combining in-hospital mortality (assigned -1) and days free of organ support to day 21 in survivors. The trial used a Bayesian statistical model with predefined triggers for superiority, inferiority, efficacy, equivalence or futility.\r\n\r\nRESULTS\r\nOf 2274 critically ill participants enrolled between 25 March 2020 and 10 April 2021, 972 were assigned to tocilizumab, 485 to sarilumab, 378 to anakinra and 418 to control. Median organ support-free days were 7 (IQR -1, 16), 9 (IQR -1, 17), 0 (IQR -1, 15) and 0 (IQR -1, 15) for tocilizumab, sarilumab, anakinra and control, respectively. Median adjusted ORs were 1.46 (95% credible intervals (CrI) 1.13, 1.87), 1.50 (95% CrI 1.13, 2.00) and 0.99 (95% CrI 0.74, 1.35) for tocilizumab, sarilumab and anakinra relative to control, yielding 99.8%, 99.8% and 46.6% posterior probabilities of superiority, respectively, compared with control. All treatments appeared safe.\r\n\r\nCONCLUSIONS\r\nIn critically ill patients with COVID-19, tocilizumab and sarilumab have equivalent effectiveness at reducing duration of organ support and death. Anakinra is not effective in this population.\r\n\r\nTRIAL REGISTRATION NUMBER\r\nNCT02735707.","PeriodicalId":23284,"journal":{"name":"Thorax","volume":"20 1","pages":""},"PeriodicalIF":9.0000,"publicationDate":"2025-05-13","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":null,"platform":"Semanticscholar","paperid":null,"PeriodicalName":"Thorax","FirstCategoryId":"3","ListUrlMain":"https://doi.org/10.1136/thorax-2024-222488","RegionNum":1,"RegionCategory":"医学","ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":null,"EPubDate":"","PubModel":"","JCR":"Q1","JCRName":"RESPIRATORY SYSTEM","Score":null,"Total":0}

引用次数: 0

Abstract

INTRODUCTION Tocilizumab improves outcomes in critically ill patients with COVID-19. Whether other immune-modulator strategies are equally effective or better is unknown. METHODS We investigated treatment with tocilizumab, sarilumab, anakinra and no immune modulator in these patients. In this ongoing, adaptive platform trial in 133 sites in 9 countries, we randomly assigned patients with allocation ratios dependent on the number of interventions available at each site. The primary outcome was an ordinal scale combining in-hospital mortality (assigned -1) and days free of organ support to day 21 in survivors. The trial used a Bayesian statistical model with predefined triggers for superiority, inferiority, efficacy, equivalence or futility. RESULTS Of 2274 critically ill participants enrolled between 25 March 2020 and 10 April 2021, 972 were assigned to tocilizumab, 485 to sarilumab, 378 to anakinra and 418 to control. Median organ support-free days were 7 (IQR -1, 16), 9 (IQR -1, 17), 0 (IQR -1, 15) and 0 (IQR -1, 15) for tocilizumab, sarilumab, anakinra and control, respectively. Median adjusted ORs were 1.46 (95% credible intervals (CrI) 1.13, 1.87), 1.50 (95% CrI 1.13, 2.00) and 0.99 (95% CrI 0.74, 1.35) for tocilizumab, sarilumab and anakinra relative to control, yielding 99.8%, 99.8% and 46.6% posterior probabilities of superiority, respectively, compared with control. All treatments appeared safe. CONCLUSIONS In critically ill patients with COVID-19, tocilizumab and sarilumab have equivalent effectiveness at reducing duration of organ support and death. Anakinra is not effective in this population. TRIAL REGISTRATION NUMBER NCT02735707.

查看原文本刊更多论文

Tocilizumab、sarilumab和anakinra在COVID-19危重患者中的应用：一项随机、对照、开放标签、适应性平台试验

托珠单抗可改善COVID-19危重患者的预后。其他免疫调节剂策略是否同样有效或更好尚不清楚。方法研究托珠单抗、沙伐单抗、阿那单抗在不使用免疫调节剂的情况下的治疗效果。在这项正在进行的适应性平台试验中，我们在9个国家的133个地点随机分配患者，分配比例取决于每个地点可用的干预措施的数量。主要终点是住院死亡率（赋值为-1）和幸存者第21天无器官支持天数的顺序量表。该试验使用贝叶斯统计模型，该模型具有预定义的优势、劣势、功效、等效或无效的触发因素。在2020年3月25日至2021年4月10日期间入组的2274名危重患者中，972人被分配到tocilizumab组，485人被分配到sarilumab组，378人被分配到anakinra组，418人被分配到对照组。托珠单抗、沙伐单抗、阿那单抗和对照组的中位器官支持无天数分别为7 （IQR - 1,16）、9 （IQR - 1,17）、0 （IQR - 1,15）和0 （IQR - 1,15）。tocilizumab， sarilumab和anakinra相对于对照组的校正后中位数or分别为1.46(95%可信区间（CrI） 1.13, 1.87), 1.50（95%可信区间（CrI） 1.13, 2.00）和0.99 (95% CrI 0.74, 1.35)，与对照组相比分别产生99.8%，99.8%和46.6%的后验优势概率。所有的治疗似乎都是安全的。结论在COVID-19危重患者中，托珠单抗与沙伐单抗在缩短器官支持时间和减少死亡方面具有相同的效果。阿那金在这一人群中无效。试验注册号：02735707。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

求助全文

约1分钟内获得全文求助全文

来源期刊

Thorax 医学-呼吸系统

CiteScore

16.10

自引率

2.00%

发文量

197

审稿时长

1 months

期刊介绍： Thorax stands as one of the premier respiratory medicine journals globally, featuring clinical and experimental research articles spanning respiratory medicine, pediatrics, immunology, pharmacology, pathology, and surgery. The journal's mission is to publish noteworthy advancements in scientific understanding that are poised to influence clinical practice significantly. This encompasses articles delving into basic and translational mechanisms applicable to clinical material, covering areas such as cell and molecular biology, genetics, epidemiology, and immunology.