| Literature DB >> 12427837 |
Olivier Braissant1, Hugues Henry, Anne-Marie Villard, Marie-Gabrielle Zurich, Marc Loup, Barbara Eilers, Gianni Parlascino, Edouard Matter, Olivier Boulat, Paul Honegger, Claude Bachmann.
Abstract
Hyperammonemia in neonates and infants affects brain development and causes mental retardation. We report that ammonium impaired cholinergic axonal growth and altered localization and phosphorylation of intermediate neurofilament protein in rat reaggregated brain cell primary cultures. This effect was restricted to the phase of early maturation but did not occur after synaptogenesis. Exposure to NH4Cl decreased intracellular creatine, phosphocreatine, and ADP. We demonstrate that creatine cotreatment protected axons from ammonium toxic effects, although this did not restore high-energy phosphates. The protection by creatine was glial cell-dependent. Our findings suggest that the means to efficiently sustain CNS creatine concentration in hyperammonemic neonates and infants should be assessed to prevent impairment of axonogenesis and irreversible brain damage.Entities:
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Year: 2002 PMID: 12427837 PMCID: PMC6757846
Source DB: PubMed Journal: J Neurosci ISSN: 0270-6474 Impact factor: 6.167