TREOCAPA: prophylactic treatment of the ductus arteriosus in preterm infants by acetaminophen-statistical analysis plan for the randomized phase III group sequential trial.
[en] BACKGROUND: Persistent patency of the ductus arteriosus (PDA) has challenged neonatologists for more than 40 years. Controversies persist about the management of PDA in extremely preterm infants. PDA is associated with morbidities, but no therapeutic strategy has resulted in an improved neonatal outcome. Acetaminophen appears to be a promising alternative with possibly fewer adverse effects. The primary objective is to determine whether a prophylactic pharmacological intervention with acetaminophen may increase the survival without severe morbidity at postmenstrual age of 36 weeks. METHODS AND ANALYSIS: TREOCAPA phase III is a randomized, multicenter, double-blind, stratified, placebo-controlled superiority trial, two arms in a 1:1 ratio performed in 43 NICUs of 14 European countries, evaluating whether the intervention increases the survival without severe morbidity by 10%, from 50% in control arm to 60% in treatment arm, until the age of 36 postmenstrual weeks. To detect this difference, 794 patients were required using a group sequential design. Recruitment has been closed, with 803 patients enrolled. Patients eligible for inclusion are preterm infants with a gestational age between 23 and 28 weeks. In the acetaminophen group, 20 mg/kg loading dose within 12 h after birth, followed by 7.5 mg/kg quarter in die (QID) for 5 days, will be administered to the 27-28 weeks gestational age group, and 25 mg/kg loading dose then 10 mg/kg QID will be administered to the 23-26 weeks gestational age group. The severe morbidities include severe bronchopulmonary dysplasia (BPD grade 3) according to NIH consensus, necrotizing enterocolitis (NEC) of Bell's stage II or III, intraventricular hemorrhage (IVH) grade III-IV according to Papile classification, or cystic leukomalacia. DISCUSSION: Whatever the results, the conclusions of this study should be informative for the neonatal scientific community. The results will either confirm the benefit of treatment in increasing survival without severe morbidity, or indicate a worsening of outcomes with prophylactic acetaminophen treatment, or show no difference in the primary outcome. In the latter case, ultrasonographic assessments of ductus arteriosus status on day 7 may help explain the absence of a difference. This could indicate that acetaminophen is ineffective in promoting ductal closure or that early closure of the ductus arteriosus is inconsequential if, despite more frequent closures, there is no associated improvement in outcomes. ETHICS AND DISSEMINATION: Ethical approval of the trial has been performed in each of the 14 countries after approval, at the European level, by the Voluntary Harmonization Procedure committee on 04/07/2020. Results will be disseminated through articles in peer-reviewed journals. TRIAL REGISTRATION: European Clinical Trials Database: EudraCT Number: 2019-004297-26. CLINICALTRIALS: gov: NCT04459117, registered on July 7, 2020. [fr] CONTEXTE : La persistance de la perméabilité du canal artériel (PDA) est un défi pour les néonatologistes depuis plus de 40 ans. Des controverses persistent quant à la prise en charge du CAP chez les grands prématurés. Le CAP est associé à des morbidités, mais aucune stratégie thérapeutique n'a permis d'améliorer l'issue néonatale. L'acétaminophène semble être une alternative prometteuse avec peut-être moins d'effets indésirables. L'objectif principal est de déterminer si une intervention pharmacologique prophylactique avec de l'acétaminophène peut augmenter la survie sans morbidité grave à l'âge post-menstruel de 36 semaines. MÉTHODES ET ANALYSE : TREOCAPA phase III est un essai de supériorité randomisé, multicentrique, en double aveugle, stratifié, contrôlé par placebo, avec deux bras dans un rapport 1:1, réalisé dans 43 unités de soins intensifs néonatals de 14 pays européens, évaluant si l'intervention augmente la survie sans morbidité sévère de 10%, de 50% dans le bras de contrôle à 60% dans le bras de traitement, jusqu'à l'âge de 36 semaines post-menstruelles. Pour détecter cette différence, 794 patientes devaient être incluses dans un groupe séquentiel. Le recrutement est terminé, avec 803 patients inscrits. Les patients éligibles à l'inclusion sont des enfants prématurés dont l'âge gestationnel se situe entre 23 et 28 semaines. Dans le groupe acétaminophène, une dose de charge de 20 mg/kg dans les 12 heures suivant la naissance, suivie d'une dose de 7,5 mg/kg quatre fois par jour (QID) pendant 5 jours, sera administrée au groupe d'âge gestationnel de 27-28 semaines, et une dose de charge de 25 mg/kg puis une dose QID de 10 mg/kg seront administrées au groupe d'âge gestationnel de 23-26 semaines. Les morbidités graves comprennent la dysplasie broncho-pulmonaire sévère (BPD grade 3) selon le consensus du NIH, l'entérocolite nécrosante (NEC) de stade II ou III de Bell, l'hémorragie intraventriculaire (IVH) de grade III-IV selon la classification de Papile, ou la leucomalacie kystique. DISCUSSION : Quels que soient les résultats, les conclusions de cette étude devraient être instructives pour la communauté scientifique néonatale. Les résultats confirmeront le bénéfice du traitement en augmentant la survie sans morbidité sévère, ou indiqueront une aggravation des résultats avec un traitement prophylactique à l'acétaminophène, ou ne montreront aucune différence dans le résultat primaire. Dans ce dernier cas, les évaluations échographiques de l'état du canal artériel au jour 7 peuvent aider à expliquer l'absence de différence. Cela pourrait indiquer que l'acétaminophène est inefficace pour favoriser la fermeture du canal ou que la fermeture précoce du canal artériel est sans conséquence si, malgré des fermetures plus fréquentes, il n'y a pas d'amélioration associée des résultats. ETHIQUE ET DIFFUSION : L'approbation éthique de l'essai a été effectuée dans chacun des 14 pays après approbation, au niveau européen, par le comité de la procédure d'harmonisation volontaire le 04/07/2020. Les résultats seront diffusés par le biais d'articles dans des revues à comité de lecture. ENREGISTREMENT DE L'ESSAI : Base de données européenne des essais cliniques : Numéro EudraCT : 2019-004297-26. CLINICALTRIALS : gov : NCT04459117, enregistré le 7 juillet 2020.
Disciplines :
Pediatrics
Author, co-author :
Ursino, Moreno; Université Paris Cité, AP-HP, Unité d'épidémiologie clinique, Inserm, CIC-EC 1426, Paris, France. ; Centre de Recherche des Cordeliers, INSERM, Sorbonne Université, USPC, Université Paris Cité, Paris, France. ; Inria, HeKA, Paris, France.
Alberti, Corinne; Université Paris Cité, AP-HP, Unité d'épidémiologie clinique, Inserm, CIC-EC 1426, Paris, France.
Cambonie, Gilles; Université de Montpellier, CHU de Montpelllier, Montpellier, France.
Kemp, Ruth; European Foundation for the Care of Newborn Infants (EFCNI), Munich, Germany.
Vanhecke, Aure; Institut de Santé Publique, Pôle Recherche Clinique, INSERM, Paris, France.
Levoyer, Lea; Clinical Trial Safety and Public Health, ANRS| Emerging Infectious Diseases, Paris, France. ; Clinical Research Safety Department, INSERM, Paris, France.
Diallo, Alpha; Clinical Trial Safety and Public Health, ANRS| Emerging Infectious Diseases, Paris, France. ; Clinical Research Safety Department, INSERM, Paris, France.
Hallman, Mikko; Department of Pediatrics and Adolescent Medicine, Oulu University Hospital, and Research Unit of Clinical Medicine and MRC Oulu, University of Oulu, Oulu, Finland.
TREOCAPA: prophylactic treatment of the ductus arteriosus in preterm infants by acetaminophen-statistical analysis plan for the randomized phase III group sequential trial.
Alternative titles :
[fr] TREOCAPA : traitement prophylactique du canal artériel chez les prématurés par l'acétaminophène - plan d'analyse statistique pour l'essai séquentiel randomisé de phase III.
Publication date :
13 February 2025
Journal title :
Trials
eISSN :
1745-6215
Publisher :
BioMed Central, Gb
Volume :
26
Issue :
1
Pages :
52
Peer reviewed :
Peer Reviewed verified by ORBi
Commentary :
Open access on publisher website's: https://trialsjournal.biomedcentral.com/articles/10.1186/s13063-025-08751-8
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