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大鼠体内视上核催产素神经元的局部阿片类物质抑制与吗啡依赖性

Local opioid inhibition and morphine dependence of supraoptic nucleus oxytocin neurones in the rat in vivo.

作者信息

Ludwig M, Brown C H, Russell J A, Leng G

机构信息

Department of Physiology, University Medical School, Edinburgh, UK.

出版信息

J Physiol. 1997 Nov 15;505 ( Pt 1)(Pt 1):145-52. doi: 10.1111/j.1469-7793.1997.145bc.x.

Abstract
  1. Single neurones of the rat supraoptic nucleus were recorded during microdialysis of naloxone onto the ventral surface of the nucleus in anaesthetized rats. We used this combination of techniques to test whether the acute or chronic effects of systemically or centrally applied opioids upon oxytocin cell activity were due to actions of the opioids within the nucleus itself. 2. Supraoptic nucleus oxytocin neurones were identified antidromically and by an excitatory response to intravenously injected cholecystokinin. Acute intravenous injection of the kappa-agonist U50488H or the mu-agonist morphine (1-5 mg kg-1) reduced the firing rate of identified oxytocin neurones by 97.7 +/- 4.8% (n = 6) and 94.1 +/- 4.1% (n = 7), respectively. The inhibition by each of these opioids was completely reversed after administration by microdialysis (retrodialysis) of the opioid antagonist naloxone (0.1-1.0 microgram microliter-1 at 2 microliters min-1) onto the exposed ventral surface of the supraoptic nucleus. 3. Retrodialysis of naloxone (0.1-10.0 micrograms microliter-1) onto the supraoptic nucleus of rats made dependent by intracerebroventricular morphine infusion for 5 days increased the firing rate of oxytocin neurones from 0.9 +/- 0.4 to 3.1 +/- 0.7 spikes s-1 (P < 0.05, n = 6). This increase in firing rate from basal was 58.5 +/- 15.1% of that following subsequent intravenously injected naloxone (5 mg kg-1). 4. Thus, the acute inhibition of supraoptic nucleus oxytocin neurones which results from systemic administration of opioid agonists primarily occurs within the supraoptic nucleus itself, since the antagonist naloxone was effective when given into the supraoptic nucleus. Furthermore, oxytocin neurones develop morphine dependence by a mechanism which is distinct from an action on their distant afferent inputs. Nevertheless, withdrawal excitation of these afferent inputs may enhance the magnitude of oxytocin neurone withdrawal excitation.
摘要
  1. 在对麻醉大鼠视上核腹面进行纳洛酮微透析期间,记录大鼠视上核的单个神经元。我们运用这种技术组合来测试全身或中枢应用阿片类药物对催产素细胞活性的急性或慢性影响是否归因于阿片类药物在视上核自身内部的作用。2. 通过逆向刺激和对静脉注射胆囊收缩素的兴奋性反应来识别视上核的催产素神经元。急性静脉注射κ激动剂U50488H或μ激动剂吗啡(1 - 5毫克/千克)分别使已识别的催产素神经元的放电频率降低97.7±4.8%(n = 6)和94.1±4.1%(n = 7)。在将阿片类拮抗剂纳洛酮(0.1 - 1.0微克/微升,以2微升/分钟的速度)通过微透析(逆向透析)施用于暴露的视上核腹面后,这些阿片类药物中的每一种所产生的抑制作用都被完全逆转。3. 对通过脑室内注入吗啡5天而产生依赖的大鼠,将纳洛酮(0.1 - 10.0微克/微升)逆向透析到视上核上,使催产素神经元的放电频率从0.9±0.4增加到3.1±0.7个动作电位/秒(P < 0.05,n = 6)。相对于基础水平的这种放电频率增加是随后静脉注射纳洛酮(5毫克/千克)后增加量的58.5±15.1%。4. 因此,全身给予阿片类激动剂导致的视上核催产素神经元的急性抑制主要发生在视上核自身内部,因为拮抗剂纳洛酮注入视上核时是有效的。此外,催产素神经元通过一种不同于作用于其远距离传入输入的机制产生吗啡依赖性。然而,这些传入输入的戒断兴奋可能会增强催产素神经元戒断兴奋的程度。
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7d48/1160100/c037ca950a9c/jphysiol00373-0150-a.jpg

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