Overview

Hypoxic-Ischemic Encephalopathy (HIE) occurs in 20 per 1000 births. Only 47% of neonates treated with the state of the art therapy (induced systemic hypothermia) have normal outcomes. Therefore, other promising therapies that potentially work in synergy with hypothermia to improve neurologic outcomes need to be tested. One potential agent is melatonin. Melatonin is a naturally occurring substance produced mainly from the pineal gland. Melatonin is widely known for its role in regulating the circadian rhythm, but it has many other effects that may benefit infants with HI injury. Melatonin serves as a free radical scavenger, decreases inflammatory cytokines, and stimulates anti-oxidant enzymes. Therefore, melatonin may interrupt several key components in the pathophysiology of HIE, in turn minimizing cell death and improving outcomes. The research study will evaluate the neuroprotective properties and appropriate dose of Melatonin to give to infants undergoing therapeutic hypothermia for hypoxic ischemic encephalopathy.

Eligibility

Inclusion Criteria:

• Eligible infants are >36 0/7th weeks gestation,
• pH (cord or neonatal) <7.0,
• base deficit >16 mEq/L,
• no available blood gas,
• a cord blood/first hour of life blood gas with pH > 7.0 and < 7.15,
• base deficit between 10 and 15.9 mEq/L,
• infants must have a history of an acute perinatal event,
• either a 10-minute Apgar < 5 or a continued need for ventilation,
• All infants must have signs of encephalopathy within 6 hours of age using the modified Sarnat scoring system,
• neonates cooled within 6 hours of birth will be included in the study.

Exclusion Criteria:

• suspected inborn errors of metabolism (elevated ammonia) and hypoglycemia,
• clinical signs and symptoms consistent with meningitis detected upon sepsis evaluation,
• a diagnosis of congenital abdominal surgical problems along with multiple congenital anomalies and/or chromosomal abnormalities.