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NMDA channel antagonist MK-801 does not protect against bilirubin neurotoxicity. | LitMetric
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NMDA channel antagonist MK-801 does not protect against bilirubin neurotoxicity.

Steven M Shapiro Sompong Sombati Angela Geiger Ann C Rice

Neonatology

Department of Neurology, Virginia Commonwealth University, Richmond, VA 23298-0599, USA.

Published: December 2007

AI Article Synopsis

  • Bilirubin encephalopathy, also known as kernicterus, is a serious risk for newborns with high bilirubin levels, and the way bilirubin harms the brain is still unclear.
  • Researchers studied how the NMDA receptor antagonist MK-801 affects bilirubin toxicity in both lab settings and living subjects.
  • The results showed that MK-801 did not protect brain cells from bilirubin's harmful effects, indicating that NMDA receptor activation may not play a significant role in bilirubin neurotoxicity.

Article Abstract

Background: Bilirubin encephalopathy or kernicterus is a potentially serious complication of neonatal hyperbilirubinemia. The mechanism of bilirubin-induced neurotoxicity is not known. Many neurological insults are mediated through NMDA receptor activation.

Objective: We assessed the effect of the NMDA channel antagonist, MK-801 on bilirubin neurotoxicity in vivo and in vitro.

Methods: Bilirubin toxicity in vitro was assessed using trypan blue staining. Sulfadimethoxine injected (i.p.) jaundiced Gunn rat pups exhibit many neurological sequelae observed in human hyperbilirubinemia. Brainstem auditory-evoked potentials (BAEPs), a noninvasive sensitive tool to assess auditory dysfunction due to bilirubin neurotoxicity, were used to assess neuroprotection with MK-801 (i.p.) in vivo.

Results: In primary cultures of hippocampal neurons, 20 min exposure to 64:32 microM bilirubin:human serum albumin reduced the cell viability by approximately 50% ten hours later. MK-801 treatment did not protect the cells. MK-801 pretreatment doses ranging from 0.1-4.0 mg/kg did not protect against BAEP abnormalities in Gunn rat pups 6 h after sulfadimethoxine injection.

Conclusion: Our findings suggest that bilirubin neurotoxicity is not mediated through NMDA receptor activation.

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 Source
http://dx.doi.org/10.1159/000103743DOI Listing

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