Maia Israel S, Kawano-Dourado Letícia, Tramujas Lucas, de Oliveira Neymar Elias, Souza Rafael Naoki, Signorini Dhaisi Faustino, Pincelli Mariangela Pimentel, Zandonai Cássio Luis, Blasius Regiane Tamires, Freires Fabrício, Ferreira Vanessa Marques, Romano Marcelo Luz Pereira, Miura Mieko Claudia, de Censo Caroline Maschio, Caser Eliana Bernadete, Silva Betania, Santos Bonomo Daniela Correia, Arraes Jussara Alencar, de Alencar Filho Meton Soares, Álvares Horta Jacques Gabriel, Oliveira Déborah Campos, Boschi Emerson, Costa Rafael Lessa, Westphal Glauco Adrieno, Ramos Juliano, Lacerda Fábio Holanda, Filho Conrado Roberto Hoffmann, Pinheiro Bruno Valle, de Andrade Neumamm Leonardo Bugarin, Guimarães Júnior Mário Roberto Rezende, de Souza Davi Tamamaru, Ferreira Juliana Carvalho, Ohe Louis Nakayama, Schettini Daniel Almeida, Thompson Marlus Muri, de Oliveira Maria Cristina França, Veiga Viviane Cordeiro, Negrelli Karina L, Santos Renato H N, Damiani Lucas, Gurgel Rodrigo M, Gomes Samara P C, Lima Lucas M, Miranda Tamiris A, Laranjeira Ligia N, de Barros E Silva Pedro Gabriel Melo, Machado Flávia R, Fitzgerald Mark, Bosse Anna, Marion Joe, Carvalho Carlos Roberto Ribeiro, Brochard Laurent, Lewis Roger J, Biasi Cavalcanti Alexandre
Hcor Research Institute, São Paulo, Brazil.
Brazilian Research in Intensive Care Network (BRICNet), São Paulo, Brazil.
JAMA. 2025 Mar 11;333(10):875-890. doi: 10.1001/jama.2024.26244.
High-flow nasal oxygen (HFNO) and noninvasive ventilation (NIV) are commonly used respiratory support therapies for patients with acute respiratory failure (ARF).
To assess whether HFNO is noninferior to NIV on the rates of endotracheal intubation or death at 7 days in 5 patient groups with ARF.
DESIGN, SETTING, AND PARTICIPANTS: This noninferiority, randomized clinical trial enrolled hospitalized adults (aged ≥18 years; classified as 5 patient groups with ARF: nonimmunocompromised with hypoxemia, immunocompromised with hypoxemia, chronic obstructive pulmonary disease [COPD] exacerbation with respiratory acidosis, acute cardiogenic pulmonary edema [ACPE], or hypoxemic COVID-19, which was added as a separate group on June 26, 2023) at 33 hospitals in Brazil between November 2019 and November 2023 (final follow-up: April 26, 2024).
High-flow nasal oxygen (n = 883) or NIV (n = 883).
The primary outcome was endotracheal intubation or death within 7 days assessed using a bayesian hierarchical model with dynamic borrowing across patient groups. Noninferiority was defined by a posterior probability of 0.992 or greater for an odds ratio (OR) less than 1.55.
Among 1800 patients, 1766 completed the study (mean age, 64 [SD, 17] years; 707 [40%] were women). The primary outcome of endotracheal intubation or death at 7 days occurred in 39% (344/883) in the HFNO group vs 38% (336/883) in the NIV group. In the immunocompromised with hypoxemia patient group, the primary outcome occurred in 57.1% (16/28) in the HFNO group vs 36.4% (8/22) in the NIV group; enrollment was stopped for futility (final OR, 1.07; 95% credible interval [CrI], 0.81-1.39; noninferiority posterior probability [NPP], 0.989). In the nonimmunocompromised with hypoxemia group, the primary outcome occurred in 32.5% (81/249) in the HFNO group vs 33.1% (78/236) in the NIV group (OR, 1.02 [95% CrI, 0.81-1.26]; NPP, 0.999). In the ACPE group, the primary outcome occurred in 10.3% (14/136) in the HFNO group vs 21.3% (29/136) in the NIV group (OR, 0.97 [95% CrI, 0.73-1.23]; NPP, 0.997). In the hypoxemic COVID-19 group, the primary outcome occurred in 51.3% (223/435) in the HFNO group vs 47.0% (210/447) in the NIV group (OR, 1.13 [95% CrI, 0.94-1.38]; NPP, 0.997). In the COPD exacerbation with respiratory acidosis group, the primary outcome occurred in 28.6% (10/35) in the HFNO group vs 26.2% (11/42) in the NIV group (OR, 1.05 [95% CrI, 0.79-1.36]; NPP, 0.992). However, a post hoc analysis without dynamic borrowing across the 5 ARF patient groups revealed some qualitatively different results in patients with COPD, immunocompromised patients, and patients with ACPE. The incidence of serious adverse events was similar (9.4% of patients in HFNO group vs 9.9% in NIV group).
Compared with NIV, HFNO met prespecified criteria for noninferiority for the primary outcome of endotracheal intubation or death within 7 days in 4 of the 5 patient groups with ARF. However, the small sample sizes in some patient groups and the sensitivity of the findings to the choice of analysis model suggests the need for further study in patients with COPD, immunocompromised patients, and patients with ACPE.
ClinicalTrials.gov Identifier: NCT03643939.
高流量鼻导管给氧(HFNO)和无创通气(NIV)是急性呼吸衰竭(ARF)患者常用的呼吸支持疗法。
评估在5组ARF患者中,HFNO在7天内气管插管率或死亡率方面是否不劣于NIV。
设计、设置和参与者:这项非劣效性随机临床试验纳入了巴西33家医院中住院的成年人(年龄≥18岁;分为5组ARF患者:低氧血症且无免疫功能低下、低氧血症且免疫功能低下、慢性阻塞性肺疾病(COPD)急性加重伴呼吸性酸中毒、急性心源性肺水肿(ACPE)或低氧血症型新型冠状病毒肺炎(COVID-19),COVID-19组于2023年6月26日单独设立),时间为2019年11月至2023年11月(最终随访时间:2024年4月26日)。
高流量鼻导管给氧(n = 883)或无创通气(n = 883)。
主要结局是使用跨患者组动态借用的贝叶斯分层模型评估7天内的气管插管或死亡情况。非劣效性定义为比值比(OR)小于1.55时后验概率为0.992或更高。
1800例患者中,1766例完成研究(平均年龄64岁[标准差17岁];707例[40%]为女性)。HFNO组7天内气管插管或死亡的主要结局发生率为39%(344/883),NIV组为38%(336/883)。在低氧血症且免疫功能低下患者组中,HFNO组主要结局发生率为57.1%(16/28),NIV组为36.4%(8/22);因无效而停止入组(最终OR为1.07;95%可信区间[CrI]为0.81 - 1.39;非劣效性后验概率[NPP]为0.989)。在低氧血症且无免疫功能低下组中,HFNO组主要结局发生率为32.5%(81/249),NIV组为33.1%(78/236)(OR为1.02[95% CrI为0.81 - 1.26];NPP为0.999)。在ACPE组中,HFNO组主要结局发生率为10.3%(14/136),NIV组为21.3%(29/136)(OR为0.97[95% CrI为0.73 - 1.23];NPP为0.997)。在低氧血症型COVID-19组中,HFNO组主要结局发生率为51.3%(223/435),NIV组为47.0%(210/447)(OR为1.13[95% CrI为0.94 - 1.38];NPP为0.997)。在COPD急性加重伴呼吸性酸中毒组中,HFNO组主要结局发生率为28.6%(10/35),NIV组为26.2%(11/42)(OR为1.05[95% CrI为0.79 - 1.36];NPP为0.992)。然而,一项未跨5组ARF患者组进行动态借用的事后分析显示,COPD患者、免疫功能低下患者和ACPE患者的结果在性质上有所不同。严重不良事件发生率相似(HFNO组为9.4%,NIV组为9.9%)。
与NIV相比,HFNO在5组ARF患者中的4组中,在7天内气管插管或死亡的主要结局方面达到了预先设定的非劣效性标准。然而,一些患者组样本量较小,且研究结果对分析模型选择敏感,这表明需要对COPD患者、免疫功能低下患者和ACPE患者进行进一步研究。
ClinicalTrials.gov标识符:NCT03643939。