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丘脑神经元对离子电泳施加单胺类物质的反应。

The responses of thalamic neurons to iontophoretically applied monoamines.

作者信息

Phillis J W, Tebĕcis A K

出版信息

J Physiol. 1967 Oct;192(3):715-45. doi: 10.1113/jphysiol.1967.sp008327.

DOI:10.1113/jphysiol.1967.sp008327
PMID:4293789
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1365538/
Abstract
  1. The effects of noradrenaline (NA), adrenaline, dopamine (DA) 5-hydroxytryptamine (5-HT) and a number of related drugs were tested on the extracellularly recorded responses of neurones in the feline thalamus. Substances were applied iontophoretically and tested on synaptically, antidromically and chemically evoked neuronal activity.2. NA, adrenaline, isoprenaline and 5-HT had a variety of effects, depressing some cells, exciting others and not affecting the responses of a third group. DA depressed most of the cells tested; excitation was not observed with this compound.3. The magnitude of depressant actions and their duration varied considerably. The more sensitive cells responded to extremely small amounts of catecholamine or 5-HT and recovery often took several minutes. Recovery after DA was always rapid. Neurones in the dorsal thalamus were generally more susceptible to depression than those in the ventro-basal complex.4. Excitatory responses were most marked in the ventro-basal complex of the thalamus. Desensitization occurred if NA or adrenaline was applied repeatedly and this tachyphylaxis lasted for several minutes. After desensitization to the excitatory effects, some of these cells were depressed by catecholamines. These findings suggest the presence of at least two types of membrane receptor.5. beta-adrenergic antagonists (alderlin, D-INPEA and MJ 1999) and alpha-antagonists (phentolamine, dibenzyline and chlorpromazine) had pronounced depressant actions on some thalamic neurones. With the exceptions of D-INPEA and MJ 1999 they also excited cells that were excited by the catecholamines. Alderlin and phentolamine had both excitatory and inhibitory effects on some cells.6. The monoamine oxidase inhibitor, iproniazid, depressed neurones which were sensitive to NA depression. It did not appear to potentiate the effects of NA on most of the cells tested.7. Reticular formation stimulation depressed some neurones in the thalamus and excited others. The depressant effects of NA and reticular formation stimulation were reduced or abolished by an intravenous injection of picrotoxin (1 mg/kg).8. It is suggested that NA and 5-HT may be inhibitory transmitters in the thalamus, released at the terminals of ascending pathways from the brain stem that have been defined by fluorescence microscopy. The excitatory actions of these compounds may also be related to a synaptic role.
摘要
  1. 对去甲肾上腺素(NA)、肾上腺素、多巴胺(DA)、5-羟色胺(5-HT)以及一些相关药物,在猫丘脑神经元细胞外记录的反应上进行了测试。通过离子电泳法施加这些物质,并对突触诱发、逆向诱发和化学诱发的神经元活动进行测试。

  2. NA、肾上腺素、异丙肾上腺素和5-HT具有多种效应,抑制一些细胞,兴奋另一些细胞,对第三组细胞的反应则无影响。DA抑制了大多数测试细胞;未观察到该化合物有兴奋作用。

  3. 抑制作用的强度及其持续时间差异很大。较敏感的细胞对极少量的儿茶酚胺或5-HT有反应,恢复通常需要几分钟。DA作用后的恢复总是很快。背侧丘脑的神经元通常比腹侧基底复合体中的神经元更容易受到抑制。

  4. 兴奋反应在丘脑腹侧基底复合体中最为明显。如果反复施加NA或肾上腺素会发生脱敏现象,且这种快速耐受性会持续几分钟。对兴奋作用脱敏后,这些细胞中的一些会被儿茶酚胺抑制。这些发现表明至少存在两种类型的膜受体。

  5. β-肾上腺素能拮抗剂(阿地林、D-INPEA和MJ 1999)和α-拮抗剂(酚妥拉明、双苄胺和氯丙嗪)对一些丘脑神经元有明显的抑制作用。除D-INPEA和MJ 1999外,它们还能兴奋那些被儿茶酚胺兴奋的细胞。阿地林和酚妥拉明对一些细胞既有兴奋作用又有抑制作用。

  6. 单胺氧化酶抑制剂异烟酰异丙肼抑制了对NA抑制敏感的神经元。在大多数测试细胞中,它似乎并未增强NA的作用。

  7. 网状结构刺激抑制了丘脑中的一些神经元并兴奋了另一些神经元。静脉注射印防己毒素(1毫克/千克)可减弱或消除NA和网状结构刺激的抑制作用。

  8. 有人提出,NA和5-HT可能是丘脑中的抑制性递质,在荧光显微镜已确定的来自脑干的上行通路终末释放。这些化合物的兴奋作用也可能与突触作用有关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7af8/1365538/7d102d6051b2/jphysiol01117-0143-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7af8/1365538/0a50f30e13a0/jphysiol01117-0142-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7af8/1365538/7d102d6051b2/jphysiol01117-0143-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7af8/1365538/0a50f30e13a0/jphysiol01117-0142-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7af8/1365538/7d102d6051b2/jphysiol01117-0143-a.jpg

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