Intravenous sildenafil for postoperative pulmonary hypertension in children with congenital heart disease

From October 2003 to January 2005, a randomized, multicenter, double-blind, placebo-controlled, dose-ranging, parallel-group study was conducted in children undergoing corrective cardiac surgery who developed postoperative PH. Patients were randomized to one of three doses of intravenous sildenafil, or placebo, for a minimum of 24 h.

The study was conducted in compliance with the Declaration of Helsinki and the International Conference on Harmonisation Good Clinical Practices guidelines. The study protocol was reviewed and approved by the local institutional ethics committees. Patients believed to be at high risk for developing postoperative PH were identified before surgery. Written informed consent was obtained prior to initiation of protocol-specified procedures from each patient’s parent or legal guardian, and patient consent was obtained (when applicable) within the 2 weeks before surgery.

All infants or children aged 0 (≥34 weeks gestational age) to 17 years undergoing corrective cardiac surgery with a clinical diagnosis of postoperative PH within 48 h of the end of surgery and systolic PAP >50% of systolic arterial blood pressure (>75% for neonates ≤28 days) were eligible (Fig. 1). PH was confirmed by Doppler echocardiogram using the modified Bernoulli equation to the peak velocity of tricuspid regurgitation [p = 4v ², where p = peak pressure drop from the right ventricle to the right atrium and v = peak velocity of tricuspid regurgitation (m/s)] that has been correlated with invasive transcatheter measurements [8], or pulmonary artery (PA) catheter at baseline. The exclusion criteria included: use of postoperative treatment solely for the purpose of treating or preventing PH, including agents used at relatively high doses for the purpose of deep/heavy sedation, such as fentanyl; agents used for continued paralysis, such as pancuronium (except when used to manage clinical situations such as open chest or critical airway); alkalinization by methods such as hyperventilation (pCO₂ <30 mmHg) or bicarbonate (HCO₃) infusion; vasodilators; meeting the criteria for extracorporeal membrane oxygenation (ECMO); receipt of concomitant nitrates or NO donors, open-label sildenafil within 48 h prior to surgery or any time postoperatively; supplemental arginine, long-acting α-blockers, endothelin antagonists (e.g., bosentan), or potent cytochrome P450 3A4 inhibitors such as ritonavir or nicorandil. Additional exclusion criteria were: occurrence of postoperative complications that resulted in hypoxemia (other than PH) due to lung disease; serious postoperative bleeding resulting in hypotension; impaired renal function [serum creatinine >2.5 times the upper limit of normal (ULN)] or hepatic function (alanine transaminase or aspartate transaminase >3.0 ULN; conjugated bilirubin >2.0 ULN; total bilirubin >2.0 ULN); and leukopenia (WBC <2,500/μl). Permitted medications included inotropes, milrinone, and other medication used to treat congestive heart failure.

The patients, parents, all clinical staff, and the investigators were blinded to study drug allocation. An automated interactive voice response system was used to assign patients to treatment. Randomization was stratified by age (neonate or non-neonate) and by study center to ensure a balance across treatment groups. The minimization approach with biased coin assignment was used for stratification. The sponsor (Pfizer Inc.) provided 50-ml vials containing sildenafil 1.0 mg/ml. Placebo was provided as bags of 5% dextrose in water. The research pharmacist or other qualified individual received the randomized treatment assignment and prepared the bolus dose and maintenance infusion. The dilution was calculated according to the patient’s weight such that the assigned concentration (low, medium, or high) was infused at the same rate for all patients of a particular weight so that the staff remained blinded to the study dose.

Baseline echocardiograms were performed to verify the presence of PH. Baseline hemodynamic parameters (in patients with a pulmonary artery, left atrial, and/or right atrial/central venous catheter), inotrope score [16], and vital signs were measured, and blood samples were collected for serum lactate measurement. Final study assessments were performed at discharge or 7 days after study drug infusion, whichever occurred first. There was a follow-up telephone call 28 days after study drug infusion.

Three intravenous sildenafil dosage regimens were selected to achieve target sildenafil plasma concentrations of approximately 40, 120, and 360 ng/ml in the low-, medium-, and high-dose groups, respectively. Selection of sildenafil doses for neonates and infants <60 days of age was to be based on pharmacokinetic data in neonates obtained from a clinical trial that was ongoing at the time [17, 18]. Each intravenous sildenafil dose regimen consisted of a bolus loading dose infused over 5 min followed immediately by a maintenance infusion over 24–72 h (Supplementary Table 2). After 30 min of study drug infusion, additional therapy for PH was to be initiated if clinically indicated based on protocol-defined rules (see Supplementary Material). If the patient was judged clinically stable at 24 h or longer after randomization, the infusion was discontinued. The infusion of study drug continued for a minimum of 24 and maximum of 72 h.

Plasma sample extracts were analyzed using liquid chromatography and tandem mass spectrometry for separation and detection of the analytes. The overall method imprecision values for the analysis of plasma quality control samples at concentrations of 3, 30, and 350 ng/ml were 6.2%, 4.5%, and 6.1%, respectively, for sildenafil.

Data are expressed as mean ± standard deviation (SD) if normally distributed or as median (range). Comparisons between groups were made with independent t tests and Wilcoxon tests for continuous variables, exact log-rank tests for times to event, and chi-square tests for frequencies. A p value <0.05 was considered significant.

Assuming that 75% of the placebo patients and 40% of patients at the highest sildenafil dose would require additional therapy within 24 h of the start of infusion, a sample size of 228 patients (57 per treatment arm) was required to detect this difference with 90% power with a one-sided type I error rate of 0.025 (corresponding to a two-sided level of 0.05), using a Hochberg adjustment for multiple comparisons that results in the minimum one-sided per-comparison error rate of 0.0085. Allowing for a postrandomization withdrawal rate of 10%, 252 patients were required to be randomized.

The primary endpoint was the receipt of any additional therapy for treatment of postoperative PH within 24 h of start of study drug infusion. The secondary endpoints were duration of mechanical ventilation and length of postoperative hospital stay. Tertiary endpoints included total duration of administration of additional therapy for PH, change from baseline in postoperative inotrope scores at postbaseline assessment times, length of stay in an intensive care unit (ICU), and deaths within 28 days of follow-up or during hospital stay. Also, change from baseline in serum lactate levels and change from baseline in hemodynamic parameters (PAP, left atrial, right atrial/central venous pressure) were determined.