ry distress syndrome. a differential diagnosis should be made between respiratory distress syndrome (hyaline membrane disease) and cyanotic heart disease (restricted pulmonary blood flow). if full diagnostic facilities are not immediately available, cyanosis (po 2 less than 40 torr) and restricted pulmonary blood flow apparent on an x-ray are appropriate indicators of congenital heart defects. necessary monitoring in all neonates, arterial pressure should be monitored intermittently by umbilical artery catheter, auscultation, or with a doppler transducer. should arterial pressure fall significantly, decrease the rate of infusion immediately. in infants with restricted pulmonary blood flow, measure efficacy of prostin vr pediatric by monitoring improvement in blood oxygenation. in infants with restricted systemic blood flow, measure efficacy by monitoring improvement of systemic blood pressure and blood ph.

vide the lowest possible dosage that maintains the response. this may be accomplished by reducing the dosage from 0.1 to 0.05 to 0.025 to 0.01 micrograms per kilogram of body weight per minute. if response to 0.05 micrograms per kilogram of body weight per minute is inadequate, dosage can be increased up to 0.4 micrograms per kilogram of body weight per minute although, in general, higher infusion rates do not produce greater effects. dilution instructions to prepare infusion solutions, dilute 1 ml of prostin vr pediatric sterile solution with sodium chloride injection usp or dextrose injection usp. undiluted prostin vr pediatric sterile solution may interact with the plastic sidewalls of volumetric infusion chambers causing a change in the appearance of the chamber and creating a hazy solution. should this occur, the solution and the volumetric infusion chamber should be replaced. when using a volumetric infusion chamber, the appropriate amount of intravenous infusion solution should be added to the chamber first. the undiluted prostin vr pediatric sterile solution should then be added to the intravenous infusion solution, avoiding direct contact of the undiluted solution with the walls of the volumetric infusion chamber. dilute to volumes appropriate for the pump delivery system available. prepare fresh infusion solutions every 24 hours. discard any solution more than 24 hours old. sample dilutions and infusion rates to provide a dosage of 0.1 micrograms per kilogram of body weight per minute add 1 ampoule (500 micrograms) alprostadil to: approximate concentration of resulting solution (micrograms/ml) infusion rate (ml/min per kg of body weight) example: to provide 0.1 micrograms/kilogram of body weight per minute to an infant weighing 2.8 kilograms using a solution of 1 ampoule prostin vr pediatric in 100 ml of saline or dextrose: infusion rate = 0.02 ml/min per kg × 2.8 kg = 0.056 ml/min or 3.36 ml/hr. 250 ml 2 0.05 100 ml 5 0.02 50 ml 10 0.01 25 ml 20 0.005

ons have been reported in less than 1% of the patients: bradypnea, bronchial wheezing, hypercapnia, respiratory depression, respiratory distress, and tachypnea. gastrointestinal system see warnings the most common adverse reaction reported has been diarrhea in about 2% of the patients. the following reactions have been reported in less than 1% of the patients: gastric regurgitation, and hyperbilirubinemia. hematologic system the most common hematologic event reported has been disseminated intravascular coagulation in about 1% of the patients. the following events have been reported in less than 1% of the patients: anemia, bleeding, and thrombocytopenia. excretory system anuria and hematuria have been reported in less than 1% of the patients. skeletal system cortical proliferation of the long bones has been reported. see precautions . miscellaneous sepsis has been reported in about 2% of the patients. peritonitis has been reported in less than 1% of the patients. hypokalemia has been reported in about 1%, and hypoglycemia and hyperkalemia have been reported in less than 1% of the patients.

adequate blood oxygenation and lower body perfusion. in infants with restricted pulmonary blood flow, about 50% responded to alprostadil infusion with at least a 10 torr increase in blood po 2 (mean increase about 14 torr and mean increase in oxygen saturation about 23%). in general, patients who responded best had low pretreatment blood po 2 and were 4 days old or less. in infants with restricted systemic blood flow, alprostadil often increased ph in those having acidosis, increased systemic blood pressure, and decreased the ratio of pulmonary artery pressure to aortic pressure. alprostadil must be infused continuously because it is very rapidly metabolized. as much as 80% of the circulating alprostadil may be metabolized in one pass through the lungs, primarily by β- and ω- oxidation. the metabolites are excreted primarily by the kidney, and excretion is essentially complete within 24 hours after administration. no unchanged alprostadil has been found in the urine, and there is no evidence of tissue retention of alprostadil or its metabolites.