首页> 外文期刊>Journal of chemical neuroanatomy >Orexinergic innervation of urocortin1 and cocaine and amphetamine regulated transcript neurons in the midbrain centrally projecting Edinger-Westphal nucleus
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Orexinergic innervation of urocortin1 and cocaine and amphetamine regulated transcript neurons in the midbrain centrally projecting Edinger-Westphal nucleus

机译:urocortin1和可卡因及苯丙胺调节的转录神经元在中枢集中投射的爱丁格-威斯特法尔核的食欲神经支配

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摘要

Orexin is a neuropeptide that has been implicated in several processes, such as induction of appetite, arousal and alertness and sleep/wake regulation. Multiple lines of evidence also suggest that orexin is involved in the stress response. When orexin is administered intracerebroventricular it activates the hypothalamic pituitary adrenal (HPA)-axis, which is the main regulator of the stress response. The HPA-axis is not the only player in the stress response evidence suggests that urocortin 1 (Ucn1), a member of the corticotropin releasing factor (CRF) neuropeptide family, also plays an important role in the stress response adaptation. Ucn1 is primarily synthetized in the centrally projecting Edinger-Westphal nucleus (EWcp), which also receives dense innervation by orexin terminals. In this study we tested the hypothesis that orexin would directly shape the response of EWcp-Ucn1 neurons to acute cold stress. To test this hypothesis, we first assessed whether orexinergic axon terminals would innervate EWcp-Ucn1/CART neurons, and next we exposed orexin deficient (orexin-KO) male mice and their male wild-type (WT) littermates to acute cold stress for 2. h. We also assessed stress-associated changes in plasma corticosterone (CORT), as well as the activation of Ucn1/CART neurons in the EWcp nucleus. We found that orexin immunoreactive axon terminals were juxtaposed to EWcp-Ucn1/CART neurons, which also expressed orexin receptor 1 mRNA. Furthermore, acute stress strongly activated the EWcp-Ucn1/CART neurons and increased plasma CORT in both WT littermates and orexin-KO mice, however no genotype effect was found on these indices. Taken together our data show that orexin in general is not involved in the animal's acute stress response (plasma CORT) and it does not play a direct role in shaping the response of EWcp-Ucn1 neurons to acute stress either.
机译:食欲素是一种神经肽,已经参与了多个过程,例如食欲的诱导,唤醒和机敏以及睡眠/觉醒调节。多条证据还表明,食欲素与压力反应有关。当脑室内给予食欲肽时,它会激活下丘脑垂体肾上腺(HPA)轴,这是压力反应的主要调节器。 HPA轴并不是应激反应证据中的唯一参与者,提示促肾上腺皮质激素释放因子(CRF)神经肽家族的成员尿皮质素1(Ucn1)在应激反应适应中也起着重要作用。 Ucn1主要在中央突出的爱丁格-威斯特法尔核(EWcp)中合成,该核还通过orexin末端接受密集的神经支配。在这项研究中,我们测试了orexin会直接影响EWcp-Ucn1神经元对急性冷应激反应的假设。为了验证这一假设,我们首先评估了食欲素的轴突末端是否会支配EWcp-Ucn1 / CART神经元,然后我们将食欲素缺乏症(orexin-KO)的雄性小鼠及其雄性野生型(WT)同窝暴露于急性冷应激中2 。 H。我们还评估了血浆皮质酮(CORT)的压力相关变化,以及EWcp核中Ucn1 / CART神经元的激活。我们发现,orexin免疫反应性轴突末端与EWcp-Ucn1 / CART神经元并列,后者也表达orexin受体1 mRNA。此外,急性应激强烈激活了WT同窝幼仔和orexin-KO小鼠的EWcp-Ucn1 / CART神经元并增加了血浆CORT,但是在这些指标上未发现基因型效应。综上所述,我们的数据表明,orexin通常不参与动物的急性应激反应(血浆CORT),并且在塑造EWcp-Ucn1神经元对急性应激的反应中也没有直接作用。

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