Calculated free bilirubin levels and neurotoxicity

Daood, Monica J.; McDonagh, Antony F.; Watchko, Jon F.

doi:10.1038/jp.2008.218

Cited by 29 publications

(16 citation statements)

References 53 publications

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“…There is a growing body of evidence that serum free or unbound bilirubin (UB) levels are a better indicator of neurologic dysfunction [63], and more specifically, auditory system damage [35,64,65] than TB, especially in preterm neonates. The UB level describes how much unconjugated bilirubin is not bound to albumin in the circulation.…”

Section: Introductionmentioning

confidence: 99%

Audiologic impairment associated with bilirubin-induced neurologic damage

Olds

Oghalai

2015

Seminars in Fetal and Neonatal Medicine

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SUMMARY Hyperbilirubinemia is occurs very frrequently among neonates and is usually mild and transient, with no long-lasting sequelae. However, bilirubin-induced neurologic damage may occur in some infants. The auditory pathway is the most sensitive part of the central nervous system to bilirubin-induced toxicity, and permanent sequelae may result from only moderately elevated total serum/plasma bilirubin levels. The damage to the auditory system occurs primarily within the brainstem and cranial nerve VIII, and manifests clinically as auditory neuropathy spectrum disorder.

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Section: Introductionmentioning

confidence: 99%

Audiologic impairment associated with bilirubin-induced neurologic damage

Olds

Oghalai

2015

Seminars in Fetal and Neonatal Medicine

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“…In vitro experiments have been elucidating the mechanisms of UCB neurotoxicity (Brites et al, 2009; Brites, 2011), while in vivo studies have almost exclusively focused on homozygous (jj) Gunn rats (Rice and Shapiro, 2008; Daood et al, 2009), the kernicterus classic model. Hyperbilirubinemic Gunn rats have a congenital deficiency of the bilirubin liver conjugating enzyme uridine-diphosphate-glucuronosyltransferase 1A1 (UGT1A1) and present neurological abnormalities similar to kernicterus (Billing, 1972) when acute bilirubin encephalopathy is induced by the administration of phenylhydrazine (Rice and Shapiro, 2008) or sulfadimethoxine (Daood et al, 2009).…”

Section: Introductionmentioning

confidence: 99%

The Evolving Landscape of Neurotoxicity by Unconjugated Bilirubin: Role of Glial Cells and Inflammation

Brites¹

2012

Front. Pharmacol.

109

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Unconjugated hyperbilirubinemia is a common condition in the first week of postnatal life. Although generally harmless, some neonates may develop very high levels of unconjugated bilirubin (UCB), which may surpass the protective mechanisms of the brain in preventing UCB accumulation. In this case, both short-term and long-term neurodevelopmental disabilities, such as acute and chronic UCB encephalopathy, known as kernicterus, or more subtle alterations defined as bilirubin-induced neurological dysfunction (BIND) may be produced. There is a tremendous variability in babies’ vulnerability toward UCB for reasons not yet explained, but preterm birth, sepsis, hypoxia, and hemolytic disease are comprised as risk factors. Therefore, UCB levels and neurological abnormalities are not strictly correlated. Even nowadays, the mechanisms of UCB neurotoxicity are still unclear, as are specific biomarkers, and little is known about lasting sequelae attributable to hyperbilirubinemia. On autopsy, UCB was shown to be within neurons, neuronal processes, and microglia, and to produce loss of neurons, demyelination, and gliosis. In isolated cell cultures, UCB was shown to impair neuronal arborization and to induce the release of pro-inflammatory cytokines from microglia and astrocytes. However, cell dependent sensitivity to UCB toxicity and the role of each nerve cell type remains not fully understood. This review provides a comprehensive insight into cell susceptibilities and molecular targets of UCB in neurons, astrocytes, and oligodendrocytes, and on phenotypic and functional responses of microglia to UCB. Interplay among glia elements and cross-talk with neurons, with a special emphasis in the UCB-induced immunostimulation, and the role of sepsis in BIND pathogenesis are highlighted. New and interesting data on the anti-inflammatory and antioxidant activities of different pharmacological agents are also presented, as novel and promising additional therapeutic approaches to BIND.

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“…This and other methods such as inhibition of NADPH oxidase or neutralizing antibodies to specific cytokines would help delineate which deleterious effects of UBR and BOXes are direct effects of these molecules and which are due to their interaction with microglia and astrocytes. This distinction is important because UBR is directly neurotoxic (31). …”

Section: Discussionmentioning

confidence: 99%

A novel brain injury mechanism after intracerebral hemorrhage: The interaction between heme products and the immune system

2010

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In this paper we hypothesize a novel mechanism by which brain injury occurs after intracerebral hemorrhage. We propose the following mechanism: 1) heme derived from extravasated erythrocytes is degraded into bilirubin and bilirubin oxidation products (BOXes). 2) Bilirubin and BOXes activate microglia and astrocytes, which are cells with immune functions in the brain. This activation leads to release of cytokines and activation of leukocyte adhesion molecules on the luminal surface of cerebral endothelial cells. 3) Leukocytes then traffic into the brain. 4) Leukocytes, activated glial cells and cytokines contribute to injury processes. We present preliminary data in support of our hypothesis that BOXes activate glia.

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Calculated free bilirubin levels and neurotoxicity

Cited by 29 publications

References 53 publications

Audiologic impairment associated with bilirubin-induced neurologic damage

Audiologic impairment associated with bilirubin-induced neurologic damage

The Evolving Landscape of Neurotoxicity by Unconjugated Bilirubin: Role of Glial Cells and Inflammation

A novel brain injury mechanism after intracerebral hemorrhage: The interaction between heme products and the immune system

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