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首页> 外文期刊>Neuroscience: An International Journal under the Editorial Direction of IBRO >Differential sensitivity of the perioculomotor urocortin-containing neurons to ethanol, psychostimulants and stress in mice and rats.
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Differential sensitivity of the perioculomotor urocortin-containing neurons to ethanol, psychostimulants and stress in mice and rats.

机译:在小鼠和大鼠中,含运动神经胶质的含尿皮质激素的神经元对乙醇,精神刺激药和压力的敏感性不同。

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The perioculomotor urocortin-containing population of neurons (pIIIu: otherwise known as the non-preganglionic Edinger-Westphal nucleus) is sensitive to alcohol and is involved in the regulation of alcohol intake. A recent study indicated that this brain region is also sensitive to psychostimulants. Since pIIIu has been shown to respond to stress, we investigated how psychostimulant-induced pIIIu activation compares to stress- and ethanol-induced activation, and whether it is independent from a generalized stress response. Several experiments were performed to test how the pIIIu responds to psychostimulants by quantifying the number of Fos immunoreactive nuclei after acute i.p. injections of saline, 10-30 mg/kg cocaine, 5 mg/kg methamphetamine, 5 mg/kg amphetamine, 2.5 g/kg ethanol, 2 h of restraint stress, 10 min of swim stress, or six applications of mild foot shock in male C57BL/6 J mice. We also compared Fos immunoreactivity in pIIIu after acute (20 mg/kg cocaine) and repeated cocaine exposure (7 days of 20 mg/kg cocaine) injections in male C57BL/6 J mice in order to investigate the potential habituation of this response. Finally, we quantified the number of Fos immunoreactive nuclei in pIIIu after administration of saline, 2.5 g/kg ethanol, 20 mg/kg cocaine, or 2 h of restraint stress in male Sprague-Dawley rats. We found that exposure to psychostimulants and ethanol induced significantly higher Fos levels in pIIIu compared to stress in mice. Furthermore, repeated cocaine injections did not decrease Fos immunoreactivity as would be expected if this response were due to stress. In rats, exposure to ethanol, psychostimulant and restraint stress all induced pIIIu Fos immunoreactivity compared to saline-injected controls. In both mice and rats, ethanol- and cocaine-induced Fos immunoreactivity occurred exclusively in urocortin 1-positive, but not in tyrosine hydroxylase-positive, cells. These results provide evidence that the pIIIu Fos-response to psychostimulants is independent of a generalized stress in mice, but not rats. They additionally show that the pIIIu response to stress differs significantly between species.
机译:含运动素尿皮质素的神经元群体(pIIIu:也称为非神经节前的爱丁格-韦斯特法尔核)对酒精敏感,并参与酒精摄入的调节。最近的一项研究表明,这个大脑区域对精神刺激药也很敏感。由于pIIIu已显示出对压力的响应,因此我们研究了精神刺激剂诱导的pIIIu激活与压力和乙醇诱导的激活相比,以及它是否独立于普遍的应激反应。进行了一些实验,通过量化急性腹腔注射后Fos免疫反应性核的数量来测试pIIIu对精神刺激药的反应。注射生理盐水,10-30 mg / kg可卡因,5 mg / kg甲基苯丙胺,5 mg / kg苯丙胺,2.5 g / kg乙醇,2 h束缚压力,10分钟的游泳压力或六次轻度足部休克的注射雄性C57BL / 6 J小鼠。我们还比较了雄性C57BL / 6 J小鼠在急性(20 mg / kg可卡因)和重复注射可卡因暴露后(20 mg / kg可卡因7天)后在pIIIu中的Fos免疫反应性,以研究这种应答的潜在习惯。最后,我们在雄性Sprague-Dawley大鼠中,于生理盐水,2.5 g / kg乙醇,20 mg / kg可卡因或束缚应激2小时后,定量了pIIIu中Fos免疫反应核的数目。我们发现,与小鼠应激相比,暴露于精神兴奋剂和乙醇会导致pIIIu中的Fos水平明显升高。此外,重复注射可卡因并没有降低Fos免疫反应性,如果这种反应是由于压力引起的话,这是可以预期的。在大鼠中,与注射生理盐水的对照组相比,暴露于乙醇,精神刺激药和束缚应激均可诱导pIIIu Fos免疫反应。在小鼠和大鼠中,乙醇和可卡因诱导的Fos免疫反应仅在尿皮质素1阳性细胞中发生,而不在酪氨酸羟化酶阳性细胞中发生。这些结果提供了证据,表明对精神兴奋剂的pIIIu Fos反应与小鼠而非大鼠中的普遍应激无关。他们还表明,pIIIu对胁迫的反应在物种之间存在显着差异。

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