Effect of non-invasive ventilation after extubation in critically ill patients with obesity in France: a multicentre, unblinded, pragmatic randomised clinical trial.
Journal
The Lancet. Respiratory medicine
ISSN: 2213-2619
Titre abrégé: Lancet Respir Med
Pays: England
ID NLM: 101605555
Informations de publication
Date de publication:
06 2023
06 2023
Historique:
received:
17
11
2022
revised:
15
12
2022
accepted:
16
12
2022
medline:
5
6
2023
pubmed:
25
1
2023
entrez:
24
1
2023
Statut:
ppublish
Résumé
Non-invasive ventilation (NIV) and oxygen therapy (high-flow nasal oxygen [HFNO] or standard oxygen) following extubation have never been compared in critically ill patients with obesity. We aimed to compare NIV (alternating with HFNO or standard oxygen) and oxygen therapy (HFNO or standard oxygen) following extubation of critically ill patients with obesity. In this multicentre, parallel group, pragmatic randomised controlled trial, conducted in 39 intensive care units in France, critically ill patients with obesity undergoing extubation were randomly assigned (1:1) to either the NIV group or the oxygen therapy group. Two randomisations were performed: first, randomisation to either NIV or oxygen therapy, and second, randomisation to either HFNO or standard oxygen (also 1:1), which was nested within the first randomisation. Blinding of the randomisation was not possible, but the statistician was masked to group assignment. The primary outcome was treatment failure within 3 days after extubation, a composite of reintubation for mechanical ventilation, switch to the other study treatment, or premature discontinuation of study treatment. The primary outcome was analysed by intention to treat. Effect of medical and surgical status was assessed. The reintubation within 3 days was analysed by intention to treat and after a post-hoc crossover analysis. This study is registered with ClinicalTrials.gov, number NCT04014920. From Oct 2, 2019, to July 17, 2021, of the 1650 screened patients, 981 were enrolled. Treatment failure occurred in 66 (13·5%) of 490 patients in the NIV group and in 130 (26·5%) of 491 patients in the oxygen-therapy group (relative risk 0·43; 95% CI 0·31-0·60, p<0·0001). Medical or surgical status did not modify the effect of NIV group on the treatment-failure rate. Reintubation within 3 days after extubation was similar in the non-invasive ventilation group and in the oxygen therapy group in the intention-to-treat analysis (48 (10%) of 490 patients and 59 (12%) of 491 patients, p=0·26) and lower in the NIV group than in the oxygen-therapy group in the post-hoc cross-over (51 (9%) of 560 patients and 56 (13%) of 421 patients, p=0·037) analysis. No severe adverse events were reported. Among critically ill adults with obesity undergoing extubation, the use of NIV was effective to reduce treatment-failure within 3 days. Our results are relevant to clinical practice, supporting the use of NIV after extubation of critically ill patients with obesity. However, most of the difference in the primary outcome was due to patients in the oxygen therapy group switching to NIV, and more evidence is needed to conclude that an NIV strategy leads to improved patient-centred outcomes. French Ministry of Health.
Sections du résumé
BACKGROUND
Non-invasive ventilation (NIV) and oxygen therapy (high-flow nasal oxygen [HFNO] or standard oxygen) following extubation have never been compared in critically ill patients with obesity. We aimed to compare NIV (alternating with HFNO or standard oxygen) and oxygen therapy (HFNO or standard oxygen) following extubation of critically ill patients with obesity.
METHODS
In this multicentre, parallel group, pragmatic randomised controlled trial, conducted in 39 intensive care units in France, critically ill patients with obesity undergoing extubation were randomly assigned (1:1) to either the NIV group or the oxygen therapy group. Two randomisations were performed: first, randomisation to either NIV or oxygen therapy, and second, randomisation to either HFNO or standard oxygen (also 1:1), which was nested within the first randomisation. Blinding of the randomisation was not possible, but the statistician was masked to group assignment. The primary outcome was treatment failure within 3 days after extubation, a composite of reintubation for mechanical ventilation, switch to the other study treatment, or premature discontinuation of study treatment. The primary outcome was analysed by intention to treat. Effect of medical and surgical status was assessed. The reintubation within 3 days was analysed by intention to treat and after a post-hoc crossover analysis. This study is registered with ClinicalTrials.gov, number NCT04014920.
FINDINGS
From Oct 2, 2019, to July 17, 2021, of the 1650 screened patients, 981 were enrolled. Treatment failure occurred in 66 (13·5%) of 490 patients in the NIV group and in 130 (26·5%) of 491 patients in the oxygen-therapy group (relative risk 0·43; 95% CI 0·31-0·60, p<0·0001). Medical or surgical status did not modify the effect of NIV group on the treatment-failure rate. Reintubation within 3 days after extubation was similar in the non-invasive ventilation group and in the oxygen therapy group in the intention-to-treat analysis (48 (10%) of 490 patients and 59 (12%) of 491 patients, p=0·26) and lower in the NIV group than in the oxygen-therapy group in the post-hoc cross-over (51 (9%) of 560 patients and 56 (13%) of 421 patients, p=0·037) analysis. No severe adverse events were reported.
INTERPRETATION
Among critically ill adults with obesity undergoing extubation, the use of NIV was effective to reduce treatment-failure within 3 days. Our results are relevant to clinical practice, supporting the use of NIV after extubation of critically ill patients with obesity. However, most of the difference in the primary outcome was due to patients in the oxygen therapy group switching to NIV, and more evidence is needed to conclude that an NIV strategy leads to improved patient-centred outcomes.
FUNDING
French Ministry of Health.
Identifiants
pubmed: 36693403
pii: S2213-2600(22)00529-X
doi: 10.1016/S2213-2600(22)00529-X
pii:
doi:
Substances chimiques
Oxygen
S88TT14065
Banques de données
ClinicalTrials.gov
['NCT04014920']
Types de publication
Randomized Controlled Trial
Multicenter Study
Journal Article
Research Support, Non-U.S. Gov't
Langues
eng
Sous-ensembles de citation
IM
Pagination
530-539Investigateurs
Audrey DE Jong
(A)
Anne Bignon
(A)
François Stephan
(F)
Thomas Godet
(T)
Jean-Michel Constantin
(JM)
Karim Asehnoune
(K)
Aude Sylvestre
(A)
Juliette Sautillet
(J)
Raiko Blondonnet
(R)
Martine Ferrandiere
(M)
Philippe Seguin
(P)
Sigismond Lasocki
(S)
Amelie Rolle
(A)
Pierre-Marie Fayolle
(PM)
Laurent Muller
(L)
Emmanuel Pardo
(E)
Nicolas Terzi
(N)
Severin Ramin
(S)
Boris Jung
(B)
Paer-Selim Abback
(PS)
Philippe Guerci
(P)
Benjamine Sarton
(B)
Hadrien Roze
(H)
Claire Dupuis
(C)
Joel Cousson
(J)
Marion Faucher
(M)
Virginie Lemiale
(V)
Bernard Cholley
(B)
Gerald Chanques
(G)
Fouad Belafia
(F)
Helena Huguet
(H)
Emmanuel Futier
(E)
Claudine Gniadek
(C)
Aurelie Vonarb
(A)
Albert Prades
(A)
Carine Jaillet
(C)
Xavier Capdevila
(X)
Jonathan Charbit
(J)
Thibaut Genty
(T)
Saida Rezaiguia-Delclaux
(S)
Audrey Imbert
(A)
Catherine Pilorge
(C)
Roman Calypso
(R)
Astrid Bouteau-Durand
(A)
Michel Carles
(M)
Hossen Mehdaoui
(H)
Bertrand Souweine
(B)
Laure Calvet
(L)
Matthieu Jabaudon
(M)
Benjamin Rieu
(B)
Clara Candille
(C)
Florian Sigaud
(F)
Beatrice Riu
(B)
Laurent Papazian
(L)
Sabine Valera
(S)
Djamel Mokart
(D)
Laurent Chow Chine
(L)
Magali Bisbal
(M)
Camille Pouliquen
(C)
Jean-Manuel DE Guibert
(JM)
Maxime Tourret
(M)
Damien Mallet
(D)
Marc Leone
(M)
Laurent Zieleskiewicz
(L)
Jeanne Cossic
(J)
Mona Assefi
(M)
Elodie Baron
(E)
Cyril Quemeneur
(C)
Antoine Monsel
(A)
Matthieu Biais
(M)
Alexandre Ouattara
(A)
Eline Bonnardel
(E)
Simon Monziols
(S)
Martin Mahul
(M)
Jean-Yves Lefrant
(JY)
Claire Roger
(C)
Saber Barbar
(S)
Fabien Lambiotte
(F)
Piehr Saint-Leger
(P)
Catherine Paugam
(C)
Julien Pottecher
(J)
Pierre-Olivier Ludes
(PO)
Lucie Darrivere
(L)
Marc Garnier
(M)
Eric Kipnis
(E)
Gilles Lebuffe
(G)
Matthias Garot
(M)
Jeremy Falcone
(J)
Benjamin Chousterman
(B)
Magali Collet
(M)
Etienne Gayat
(E)
Jean Dellamonica
(J)
Willy-Serge Mfam
(WS)
Evelina Ochin
(E)
Mohamed Nebli
(M)
Nejla Tilouche
(N)
Benjamin Madeux
(B)
David Bougon
(D)
Yassir Aarab
(Y)
Fanny Garnier
(F)
Elie Azoulay
(E)
Nicolas Molinari
(N)
Samir Jaber
(S)
Commentaires et corrections
Type : CommentIn
Informations de copyright
Copyright © 2023 Elsevier Ltd. All rights reserved.
Déclaration de conflit d'intérêts
Declaration of interests SJ reports receiving consulting fees from Drager, Medtronic, Mindray, Fresenius, Baxter, and Fisher & Paykel. ADJ reports receiving remuneration for presentations from Medtronic, Drager and Fisher & Paykel. VL reported being a member of a research group that has received grants from Alexion, Baxter, MSD, Gilead, Sanofi, Celgène. All other authors declare no competing interests.