Patent ductus arteriosus (PDA) is a very common condition in immature newborn babies and it has been associated to morbidity and mortality. Ibuprofen is the drug of choice for PDA treatment according to the last version of the Cochrane review. Nowadays the best dose regimen for ibuprofen remains uncertain. The investigators aim to perform a randomized controlled clinical trial to assess whether echocardiographically guided PDA ibuprofen treatment versus standard treatment could reduce the number of doses of ibuprofen without increasing the reopening rate and reducing the side effects associated to this medication.
Patent ductus arteriosus (PDA) is presented in 55 to 70% of the preterm infants with a gestational age lower than 30 weeks or a birth weight lower than 1000 grams. PDA has being associated to mortality or morbidity such as ischemic or hemorrhagic cerebral events, necrotising enterocolitis, renal disfunction or poor pulmonary outcome; however, it is not clear whether these are a consequence of the PDA presence, the treatment implemented for closing it, or the immaturity of these population. PDA standard treatment (ST) consists on three doses of indomethacin or ibuprofen (10-5-5mg/kg) given 24 hours apart, being the surgical closure a second line therapeutic option. In spite of ibuprofen has been pointed as the drug of choice for PDA treatment by the last version of the Cochrane review, side effects have been associated to both medication. Standard ibuprofen treatment is based on a clinical trial where the three-dose protocol seemed to be more effective than one-dose scheme for PDA closure; however, the sample size was not powered to find differences statistically significant, so nowadays the best dose regimen for ibuprofen remains uncertain. Functional echocardiographic assessment is spreading to all over the world. In this scenario, it has been proposed its implementation to guide PDA treatment in order to individualize the number of doses of indomethacin administered as a function of patient's response, limiting the doses and side effects in those where PDA presented an early constriction. The investigators hypothesized whether echocardiographically guided PDA ibuprofen treatment could reduce the number of doses of ibuprofen without increasing the reopening rate and reducing the side effects associated to this medication.
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
TREATMENT
Masking
TRIPLE
Enrollment
49
Infants in the experimental group (echoG treatment) received additional doses of ibuprofen only if PDA was still ≥ 1.5 mm at the time of the corresponding ibuprofen dose.
Infants received 3 doses of ibuprofen at 24-hour intervals, independently of ductal size, as long as additional doses were not contraindicated.
Department of Neonatology, La Paz University Hospital
Madrid, Madrid, Spain
PDA re-opening rate
PDA re-opening after echocardiographically documented closure, which the attending physician deemed amenable to additional treatment. Infants with ventilator weaning difficulty, protracted metabolic acidosis or persistent hemodynamic instability were included in this category.
Time frame: Infants will be followed for the duration of hospital stay in the Newborn Unit, an expected average of 4-8 weeks
treatment failure
PDA ≥ 1.5 mm 24 hours after a complete ibuprofen course
Time frame: Infants will be followed for the duration of hospital stay in the Newborn Unit, an expected average of 4-8 weeks
need for surgical ligation
need for surgical ligation
Time frame: Infants will be followed for the duration of hospital stay in the Newborn Unit, an expected average of 4-8 weeks
need for additional ibuprofen doses
need for additional ibuprofen doses after treatment was completed
Time frame: Infants will be followed for the duration of hospital stay in the Newborn Unit, an expected average of 4-8 weeks
urine output
urine output
Time frame: before the first ibuprofen dose was administered (between 12-72 hours of life) until 24 hours after the last dose of ibuprofen was administered (between 36-168 h of life)
serum creatinine
serum creatinine
Time frame: before the first ibuprofen dose was administered (between 12-72 hours of life) until 24 hours after the last dose of ibuprofen was administered (between 36-168 h of life)
mortality
mortality
Time frame: Infants will be followed for the duration of hospital stay in the Newborn Unit, an expected average of 4-8 weeks
bronchopulmonary dysplasia
bronchopulmonary dysplasia (O2 need at 36 postmenstrual weeks)
Time frame: Infants will be followed for the duration of hospital stay in the Newborn Unit, an expected average of 4-8 weeks
necrotising enterocolitis
necrotising enterocolitis
Time frame: Infants will be followed for the duration of hospital stay in the Newborn Unit, an expected average of 4-8 weeks
intraventricular hemorrhage
intraventricular hemorrhage
Time frame: Infants will be followed for the duration of hospital stay in the Newborn Unit, an expected average of 4-8 weeks
White matter damage
White matter damage
Time frame: Infants will be followed for the duration of hospital stay in the Newborn Unit, an expected average of 4-8 weeks
Laser therapy for retinopathy
Laser therapy for retinopathy
Time frame: Infants will be followed for the duration of hospital stay in the Newborn Unit, an expected average of 4-8 weeks
peak systolic velocity
peak systolic velocity measured by means of cerebral Doppler ultrasonography in the anterior and middle cerebral arteries
Time frame: before each ibuprofen dose should be administered (3 days) and 24 hours after the last dose of ibuprofen was administered
end-diastolic velocity
end-diastolic velocity measured by means of cerebral Doppler ultrasonography in the anterior and middle cerebral arteries
Time frame: before each ibuprofen dose should be administered (3 days) and 24 hours after the last dose of ibuprofen was administered
resistance index
resistance index measured by means of cerebral Doppler ultrasonography in the anterior and middle cerebral arteries
Time frame: before each ibuprofen dose should be administered (3 days) and 24 hours after the last dose of ibuprofen was administered
pulsatility index
pulsatility index measured by means of cerebral Doppler ultrasonography in the anterior and middle cerebral arteries
Time frame: before each ibuprofen dose should be administered (3 days) and 24 hours after the last dose of ibuprofen was administered
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