Mariana C Baserga1, Joanna C Beachy1, Jessica K Roberts2, Robert M Ward3, Robert J DiGeronimo1, William F Walsh4, Robin K Ohls5, Jennifer Anderson5, Dennis E Mayock6, Sandra E Juul6, Robert D Christensen7, Manndi C Loertscher1, Chris Stockmann2, Catherine M T Sherwin2, Michael G Spigarelli2, Bradley A Yoder1. 1. Division of Neonatology, Department of Pediatrics, University of Utah, Salt Lake City, Utah. 2. Division of Clinical Pharmacology, Department of Pediatrics, University of Utah, Salt Lake City, Utah. 3. 1] Division of Neonatology, Department of Pediatrics, University of Utah, Salt Lake City, Utah [2] Division of Clinical Pharmacology, Department of Pediatrics, University of Utah, Salt Lake City, Utah. 4. Division of Neonatology, Department of Pediatrics, Vanderbilt University, Nashville, Tennessee. 5. Division of Neonatology, Department of Pediatrics, University of New Mexico, Albuquerque, New Mexico. 6. Division of Neonatology, Department of Pediatrics, University of Washington, Seattle, Washington. 7. Intermountain Healthcare, McKay Dee Hospital, Ogden, Utah.
Abstract
BACKGROUND: Despite therapeutic hypothermia, neonates with encephalopathy (NE) have high rates of death or disability. Darbepoetin alfa (Darbe) has comparable biological activity to erythropoietin, but has extended circulating half-life (t(1/2)). Our aim was to determine Darbe safety and pharmacokinetics as adjunctive therapy to hypothermia. STUDY DESIGN:Thirty infants (n = 10/arm) ≥36 wk gestation undergoing therapeutic hypothermia for NE were randomized to receive placebo, Darbe low dose (2 μg/kg), or high dose (10 μg/kg) given intravenously within 12 h of birth (first dose/hypothermia condition) and at 7 d (second dose/normothermia condition). Adverse events were documented for 1 mo. Serum samples were obtained to characterize Darbe pharmacokinetics. RESULTS:Adverse events (hypotension, altered liver and renal function, seizures, and death) were similar to placebo and historical controls. Following the first Darbe dose at 2 and 10 μg/kg, t(1/2) was 24 and 32 h, and the area under the curve (AUC(inf)) was 26,555 and 180,886 h*mU/ml*, respectively. In addition, clearance was not significantly different between the doses (0.05 and 0.04 l/h). At 7 d, t(1/2) was 26 and 35 h, and AUC(inf) was 10,790 and 56,233 h*mU/ml*, respectively (*P < 0.01). CONCLUSION: Darbe combined with hypothermia has similar safety profile to placebo with pharmacokinetics sufficient for weekly administration.
RCT Entities:
BACKGROUND: Despite therapeutic hypothermia, neonates with encephalopathy (NE) have high rates of death or disability. Darbepoetin alfa (Darbe) has comparable biological activity to erythropoietin, but has extended circulating half-life (t(1/2)). Our aim was to determine Darbe safety and pharmacokinetics as adjunctive therapy to hypothermia. STUDY DESIGN: Thirty infants (n = 10/arm) ≥36 wk gestation undergoing therapeutic hypothermia for NE were randomized to receive placebo, Darbe low dose (2 μg/kg), or high dose (10 μg/kg) given intravenously within 12 h of birth (first dose/hypothermia condition) and at 7 d (second dose/normothermia condition). Adverse events were documented for 1 mo. Serum samples were obtained to characterize Darbe pharmacokinetics. RESULTS: Adverse events (hypotension, altered liver and renal function, seizures, and death) were similar to placebo and historical controls. Following the first Darbe dose at 2 and 10 μg/kg, t(1/2) was 24 and 32 h, and the area under the curve (AUC(inf)) was 26,555 and 180,886 h*mU/ml*, respectively. In addition, clearance was not significantly different between the doses (0.05 and 0.04 l/h). At 7 d, t(1/2) was 26 and 35 h, and AUC(inf) was 10,790 and 56,233 h*mU/ml*, respectively (*P < 0.01). CONCLUSION: Darbe combined with hypothermia has similar safety profile to placebo with pharmacokinetics sufficient for weekly administration.
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