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首页> 外文期刊>American Journal of Physiology >Effects on sleep of microdialysis of adenosine A1 and A2a receptor analogs into the lateral preoptic area of rats.
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Effects on sleep of microdialysis of adenosine A1 and A2a receptor analogs into the lateral preoptic area of rats.

机译:腺苷A1和A2a受体类似物微渗入大鼠侧视前区对睡眠的影响。

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Evidence suggests that adenosine (AD) is an endogenous sleep factor. The hypnogenic action of AD is mediated through its inhibitory A1 and excitatory A2A receptors. Although AD is thought to be predominantly active in the wake-active region of the basal forebrain (BF), a hypnogenic action of AD has been demonstrated in several other brain areas, including the preoptic area. We hypothesized that in lateral preoptic area (LPOA), a region with an abundance of sleep-active neurons, AD acting via A1 receptors would induce waking by inhibition of sleep-active neurons and that AD acting via A2A receptors would promote sleep by stimulating the sleep-active neurons. To this end, we studied the effects on sleep of an AD transport inhibitor, nitrobenzyl-thio-inosine (NBTI) and A1 and A2A receptor agonists/antagonists by microdialyzing them into the LPOA. The results showed that, in the sleep-promoting area of LPOA: 1) A1 receptor stimulation or inhibition of AD transport by NBTI induced waking and 2) A2A receptorstimulation induced sleep. We also confirmed that NBTI administration in the wake promoting area of the BF increased sleep. The effects of AD could be mediated either directly or indirectly via interaction with other neurotransmitter systems. These observations support a hypothesis that AD mediated effects on sleep-wake cycles are site and receptor dependent.
机译:有证据表明,腺苷(AD)是一种内源性睡眠因子。 AD的催眠作用通过其抑制性A1和兴奋性A2A受体介导。尽管人们认为AD主要在基底前脑(BF)的觉醒活动区域活跃,但AD的催眠作用已在包括视光前区域在内的其他几个大脑区域得到证实。我们假设在侧视前区(LPOA)中,一个具有大量睡眠活动神经元的区域,通过A1受体作用的AD会通过抑制睡眠活动神经元而诱发清醒,而通过A2A受体作用的AD将通过刺激睡眠活动神经元来促进睡眠。睡眠活跃神经元。为此,我们通过将它们微透析到LPOA中,研究了AD转运抑制剂,硝基苄基硫代肌苷(NBTI)和A1和A2A受体激动剂/拮抗剂对睡眠的影响。结果表明,在LPOA促进睡眠的区域:1)NBTI诱导的清醒刺激A1受体或抑制AD转运; 2)刺激A2A受体诱导的睡眠。我们还证实,在BF的促醒区域中使用NBTI可以增加睡眠。 AD的作用可以通过与其他神经递质系统的相互作用直接或间接介导。这些观察结果支持一个假说,即AD介导的对睡眠-觉醒周期的影响是部位和受体依赖性的。

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