Clinical Trial: PREMILOC Trial to Prevent Bronchopulmonary Dysplasia in Very Preterm Neonates

Study Status: Completed
Recruit Status: Completed
Study Type: Interventional

Official Title: Early Prevention of Broncho-pulmonary Dysplasia and Neonatal Mortality in Very Preterm Infants Using Low Dose of Hydrocortisone: a Randomized Controlled Trial

Brief Summary: There is increasing evidence linking a fetal and early neonatal systemic inflammatory response syndrome to the subsequent development of bronchopulmonary dysplasia (BPD) and white matter injury (WMI) in very preterm infants. Babies with evidence of adrenal insufficiency early in life may not be able to control the inflammatory response and are thereby more likely to develop BPD than babies who do not show such evidence of inflammation. We designed a randomized controlled trial to test the hypothesis whether very preterm babies at high-risk of BPD, treated with low doses of HC during the first 10 days of life, are more likely to survive without BPD at 36 weeks of post-menstrual age (PMA), compared to babies treated with placebo.

Detailed Summary:

Individual patients and study procedures. Entry criteria: gestational age between 24 weeks and 27 weeks + 6 days, babies born to mother with either clinical chorioamnionitis, preterm and prelabor rupture of the membranes (PPROM), or preterm labor, written informed consent obtained before inclusion and randomization. Exclusion criteria: babies born with birth weight below the 3th percentile, PPROM before 22 weeks, major fetal anomaly or congenital malformation, mother refusal or inability to provide consent. Stratification: stratum A: 24-25 weeks and stratum B: 26-27 weeks. Centrally controlled randomization takes place between 12 and 48 hours of age and patients assigned to the HC group are treated with 0,5 mg/kg HC intravenously twice a day for seven days and once a day for the next three days. Ibuprofen is only given to babies with persistent ductus arteriosis (PDA) echocardiographically confirmed at 24 hours of age or older.

Outcome variables. The primary outcome is a dichotomous variable: survival without BPD at 36 weeks PMA. A consistent physiologic definition of BPD will be used by all participating centres (Walsh MC, Pediatrics 2004;114:1305-11). Secondary outcome variables include features of WMI on MRI performed at 40 weeks PMA and neurodevelopmental outcome at 2-year of corrected age. Other outcome variables include death before discharge, BPD at 28 days and 36 weeks, duration of mechanical ventilation and O2 supplementation, need for vasopressors, use of open-labeled postnatal steroids (HC or dexamethasone), confirmed or suspected early and late onset sepsis, PDA, gastrointestinal perforation, NEC, ROP, IVH, biological markers of the neonatal inflammatory response syndrome.


Sponsor: Assistance Publique - Hôpitaux de Paris

Current Primary Outcome: dichotomous variable: survival without BPD at 36 weeks PMA. [ Time Frame: add 8 to12 ]

Original Primary Outcome: Same as current

Current Secondary Outcome:

  • features of WMI on MRI performed between 36-40 weeks PMA [ Time Frame: 8-12 weeks ]
  • neurodevelopmental outcome [ Time Frame: 18 month-3 years ]
  • Death before discharge [ Time Frame: discharge ]
  • BPD 28 days and 36 weeks [ Time Frame: 28 days and 36 weeks ]
  • duration of mechanical ventilation and O2 supplementation [ Time Frame: inclusion to discharge ]
  • need for vasopressors [ Time Frame: inclusion to discharge ]


Original Secondary Outcome: Same as current

Information By: Assistance Publique - Hôpitaux de Paris

Dates:
Date Received: February 7, 2008
Date Started: April 2008
Date Completion:
Last Updated: August 12, 2016
Last Verified: August 2016