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Mice expressing markedly reduced striatal dopamine transporters exhibit increased locomotor activity,dopamine uptake turnover rate,and cocaine responsiveness
Authors:Anjali Rao  Alexander Sorkin  Nancy R Zahniser
Institution:1. Department of Pharmacology, School of Medicine, University of Colorado, , Anschutz Medical Campus, Aurora, Colorado, 80045;2. Department of Cell Biology and Physiology, University of Pittsburgh School of Medicine, , Pittsburgh, Pennsylvania, 15261
Abstract:Variations in the expression levels of the dopamine transporter (DAT) can influence responsiveness to psychostimulant drugs like cocaine. To better understand this relationship, we studied a new DAT‐low expresser (DAT‐LE) mouse model and performed behavioral and biochemical studies with it. Immunoblotting and 3H]WIN 35,428 binding analyses revealed that these mice express ~35% of wildtype (WT) mouse striatal DAT levels. Compared to WT mice, DAT‐LE mice were hyperactive in a novel open‐field environment. Despite their higher basal locomotor activity, cocaine (10 or 20 mg/kg, i.p.) induced greater locomotor activation in DAT‐LE mice than in WT mice. The maximal velocity (Vmax) of DAT‐mediated 3H]DA uptake into striatal synaptosomes was reduced by 46% in DAT‐LE mice, as compared to WT. Overall, considering the reduced number of DAT binding sites (Bmax) along with the reduced Vmax in DAT‐LE mice, a 2‐fold increase in DA uptake turnover rate (Vmax/Bmax) was found, relative to WT mice. This suggests that neuroadaptive changes have occurred in the DAT‐LE mice that would help to compensate for their low DAT numbers. Interestingly, these changes do not include a reduction in tyrosine hydroxylase levels, as was previously reported in DAT knockout homozygous and heterozygous animals. Further, these changes are not sufficient to prevent elevated novelty‐ and cocaine‐induced locomotor activity. Hence, these mice represent a unique model for studying changes of in vivo DAT function and regulation that result from markedly reduced levels of DAT expression. Synapse 67:668–677, 2013 . © 2013 Wiley Periodicals, Inc.
Keywords:SLC6  neurotransmitter transporter  low‐expresser  mouse model  psychostimulant  [3H]WIN 35  428
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