Abstract
Therapies to prevent severe neonatal unconjugated hyperbilirubinemia and kernicterus are phototherapy and, in unresponsive cases, exchange transfusion, which has significant morbidity and mortality risks. Neurotoxicity is caused by the fraction of unconjugated bilirubin not bound to albumin (free bilirubin, Bf). Human serum albumin (HSA) administration was suggested to increase plasma bilirubin-binding capacity. However, its clinical use is infrequent due to difficulties to address its potential preventive and curative benefits, and to the absence of reliable markers to monitor bilirubin neurotoxicity risk. We used a genetic mouse model of unconjugated hyperbilirubinemia showing severe neurological impairment and neonatal lethality. We treated mutant pups with repeated HSA administration since birth, without phototherapy application. Daily intraperitoneal HSA administration completely rescued neurological damage and lethality, depending on dosage and administration frequency. Albumin infusion increased plasma bilirubin-binding capacity, mobilizing bilirubin from tissues to plasma. This resulted in reduced plasma Bf, forebrain and cerebellum bilirubin levels. We showed that, in our experimental model, Bf is the best marker to determine the risk of developing neurological damage. These results support the potential use of albumin administration in severe acute hyperbilirubinemia conditions to prevent or treat bilirubin neurotoxicity in situations in which exchange transfusion may be required.
Highlights
Jaundice is normally treated with phototherapy (PT), which for most patients has sufficient efficacy and convenience, with high safety and low costs
human serum albumin (HSA) administration of 2.5 g/kg every 24 h (HSA 2.5 g/kg/24 h) resulted in higher survival of mice (50% mortality at P22), with one out of 11 treated mice surviving beyond 30 days
Daily treatment with HSA 5.0 g/kg (HSA 5.0 g/kg/24 h) or 7.5 g/ kg (HSA 7.5 g/kg/24 h) resulted in about 95% survival of mice beyond 30 days (Fig. 1). These results strongly underscored that HSA administration reduces mortality in this mouse model in a dose and time-dependent manner
Summary
Jaundice is normally treated with phototherapy (PT), which for most patients has sufficient efficacy and convenience, with high safety and low costs. We performed one crucial step forward: we tested the long-term benefits of albumin administration in a more severe and clinically relevant lethal mouse model of neonatal hyperbilirubinemia[36,37], without the application of the standard phototherapy treatment. These mice lack bilirubin-conjugation activity and develop severe hyperbilirubinemia soon after birth[36,37], closely mimicking the human pathology. The present work provides evidence that in our experimental model Bf is the best predictor of neurological damage induced by bilirubin, among the most commonly used clinical markers
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