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Publication : Genetic deletion of the norepinephrine transporter decreases vulnerability to seizures.

First Author  Kaminski RM Year  2005
Journal  Neurosci Lett Volume  382
Issue  1-2 Pages  51-5
PubMed ID  15911120 Mgi Jnum  J:104830
Mgi Id  MGI:3612833 Doi  10.1016/j.neulet.2005.02.056
Citation  Kaminski RM, et al. (2005) Genetic deletion of the norepinephrine transporter decreases vulnerability to seizures. Neurosci Lett 382(1-2):51-5
abstractText  Norepinephrine (NE) has been reported to modulate neuronal excitability and act as endogenous anticonvulsant. In the present study we used NE transporter knock-out mice (NET-KO), which are characterized by high levels of extracellular NE, to investigate the role of endogenous NE in seizure susceptibility. Seizure thresholds for cocaine (i.p.), pentylenetetrazol (i.v.) and kainic acid (i.v.) were compared in NET-KO, heterozygous (NET-HT) and wild type (NET-WT) female mice. The dose-response curve for cocaine-induced convulsions was significantly shifted to the right in NET-KO mice, indicating higher seizure thresholds. The threshold doses of pentylenetetrazol that induced clonic and tonic seizures were also significantly higher in NET-KO when compared to NET-WT mice. Similarly, NET-KO mice displayed higher resistance to convulsions engendered by kainic acid. For all drugs tested, the response of NET-HT mice was always intermediate. These data provide further support for a role of endogenous NE in the control of seizure susceptibility.
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