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首页> 外文期刊>Journal of Neurochemistry: Offical Journal of the International Society for Neurochemistry >Specific involvement of neurotensin type 1 receptor in the neurotensin-mediated in vivo dopamine efflux using knock-out mice.
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Specific involvement of neurotensin type 1 receptor in the neurotensin-mediated in vivo dopamine efflux using knock-out mice.

机译:使用基因敲除小鼠,神经降压素1型受体在神经降压素介导的体内多巴胺外排中的特定参与。

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Abstract Neurotensin is a tridecapeptide neurotransmitter known to be involved in psychiatric disorders, various physiological processes and several different neurobiological mechanisms, including modulation of accumbal dopamine release. Two neurotensin extracellular binding sites, namely NT1- and NT2-receptor (NT1R and NT2R), have been cloned from the rat brain. These receptors are distinguishable by their different in vitro pharmacological properties but the available pharmacological tools have weak in vivo potency and specificity. The use of genetically engineered knock-out mice has provided a powerful alternative to the classical pharmacological approach to investigate their respective roles. In this study, using in vivo differential pulse amperometry, we show that, in wild-type mice, neurotensin application into the ventral tegmental area dose-dependently evokes dopamine efflux in the nucleus accumbens. This neurotensin-mediated efflux is dramatically decreased in mice lacking NT1R while it is unaffected in NT2R-deleted mice. This finding indicates that a large part of the dopamine efflux evoked by neurotensin in the nucleus accumbens of wild-type mice is mediated via NT1R present in the ventral tegmental area.
机译:摘要神经降压素是一种三肽神经递质,已知与精神疾病,各种生理过程和几种不同的神经生物学机制有关,包括调节多巴胺的释放。从大鼠大脑中克隆了两个神经降压素细胞外结合位点,即NT1-和NT2-受体(NT1R和NT2R)。这些受体的区别在于它们的体外药理特性不同,但是可用的药理学工具在体内的效力和特异性均较弱。基因工程基因敲除小鼠的使用为经典药理方法研究其各自的作用提供了有力的替代方法。在这项研究中,使用体内差分脉冲安培法,我们显示,在野生型小鼠中,神经降压素在腹侧被盖区的应用呈剂量依赖性地引起伏隔核中的多巴胺外排。在缺乏NT1R的小鼠中,这种神经降压素介导的外排显着减少,而在缺失NT2R的小鼠中则不受影响。该发现表明野生型小鼠伏隔核中神经降压素引起的多巴胺外排大部分是通过腹侧被盖区中存在的NT1R介导的。

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