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Modification of dopaminergic markers expression in the striatum by neonatal exposure to glutamate during development
Author(s) -
LópezPérez S.J.,
Vergara P.,
VenturaValenzuela J.P.,
UreñaGuerrero M.E.,
Segovia J.,
BeasZárate C.
Publication year - 2005
Publication title -
international journal of developmental neuroscience
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.761
H-Index - 88
eISSN - 1873-474X
pISSN - 0736-5748
DOI - 10.1016/j.ijdevneu.2004.12.010
Subject(s) - striatum , substantia nigra , tyrosine hydroxylase , dopaminergic , medicine , endocrinology , glutamate receptor , dopamine , dopamine transporter , basal ganglia , biology , nigrostriatal pathway , receptor , central nervous system
Monosodium l ‐glutamate (MSG) was administered subcutaneously to male neonatal rats, and the effect on developmental profile of tyrosine hydroxylase (TH), D1, D2 receptors, and dopamine (DA) transporter expression in the striatum was examined using Western blot. In addition, TH‐immunopositive neurons at substantia nigra (SN) were also examined. MSG treatment (4 mg/g of body weight, administered on postnatal days 1, 3, 5, and 7) resulted in a reduction of D1 and D2 receptor expression from 30 days of age and persisted to adulthood (120 days of age), while DA transporter expression was significantly reduced from 14 days of age to adulthood. TH immunopositive neurons at SN showed a significant reduction, as well as TH expression on postnatal days 10, 30, 60, and 120 at striatum was reduced. No changes of TH were observed at 14 days of age. Results indicate that an over‐stimulation of the glutamatergic system by neonatal exposure to a high glutamate concentration induces a partial loss in TH‐positive neurons in the SN and an important reduction in dopaminergic markers expression in the striatum, suggesting that early excitotoxicity could contribute to developmental alterations in the nigrostriatal pathway, which may be associated with various disorders of the basal ganglia.