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幼年猴子室旁核和视上核中血管加压素神经元上的阿片类突触。

Opioid synapses on vasopressin neurons in the paraventricular and supraoptic nuclei of juvenile monkeys.

作者信息

Goldsmith P C, Boggan J E, Thind K K

机构信息

Reproductive Endocrinology Center, University of California, School of Medicine, San Francisco 94143-0556.

出版信息

Neuroscience. 1991;45(3):709-19. doi: 10.1016/0306-4522(91)90283-t.

Abstract

Opioid peptide- as well as vasopressin-containing neurons synapse on gonadotropin releasing hormone neurons in juvenile macaques. In this study we performed double-label immunostaining for opioid and vasopressin neurons in the paraventricular and supraoptic nuclei in order to assess their interrelationships. Neuroendocrine neurons in the hypothalamus were prelabeled by microinjection of electron-dense retrograde tracer into the median eminence, and were easily identified in frontal Vibratome sections. Sections through the paraventricular and supraoptic nuclei were immunostained for vasopressin with the peroxidase-antiperoxidase technique, and for opioids using the indirect immunogold method. By light microscopy, opioid-immunoreactive inputs appeared to innervate an average of 39% of the vasopressin neurons in the paraventricular nucleus and 33% in the supraoptic nucleus, and were more prevalent anteriorly. Clusters of opioid afferents formed cup-like calices around major processes of many vasopressin neurons, especially in the paraventricular nucleus. Electron microscopy revealed that these groups of opioid axon terminals made frequent symmetrical and fewer asymmetrical synapses on both neuroendocrine and non-neuroendocrine vasopressinergic cell bodies and dendrites. Our study did not reveal vasopressin-opioid synapses in these hypothalamic nuclei, but this does not preclude the possibility of their existence elsewhere. These results indicate that opioid afferents modulate vasopressin neuronal activity in the monkey paraventricular and supraoptic nuclei. Previous results have suggested that corticotropin releasing hormone acts via vasopressinergic neurons to stimulate opioid neuronal activity and to inhibit gonadotropin releasing hormone release. Taken together, the data suggest that stressful stimuli could initiate a series of neuropeptidergic interactions which ultimately alter pulsatile gonadotropin releasing hormone secretion and thus gonadotropin secretion in primates.

摘要

阿片肽以及含血管加压素的神经元与幼年猕猴的促性腺激素释放激素神经元形成突触。在本研究中,我们对室旁核和视上核中的阿片肽和血管加压素神经元进行了双重免疫染色,以评估它们之间的相互关系。通过向正中隆起微量注射电子致密逆行示踪剂对下丘脑的神经内分泌神经元进行预标记,在额叶振动切片中很容易识别这些神经元。通过过氧化物酶-抗过氧化物酶技术对穿过室旁核和视上核的切片进行血管加压素免疫染色,使用间接免疫金法对阿片肽进行免疫染色。通过光学显微镜观察,阿片肽免疫反应性输入似乎支配了室旁核中平均39%的血管加压素神经元和视上核中33%的血管加压素神经元,且在前方更为普遍。阿片肽传入纤维簇在许多血管加压素神经元的主要突起周围形成杯状杯,尤其是在室旁核中。电子显微镜显示,这些阿片肽轴突终末组在神经内分泌和非神经内分泌血管加压素能细胞体及树突上形成频繁的对称突触和较少的不对称突触。我们的研究未在这些下丘脑核中发现血管加压素-阿片肽突触,但这并不排除它们在其他部位存在的可能性。这些结果表明,阿片肽传入纤维调节猴室旁核和视上核中血管加压素神经元的活动。先前的结果表明,促肾上腺皮质激素释放激素通过血管加压素能神经元发挥作用,刺激阿片肽神经元活动并抑制促性腺激素释放激素释放。综合来看,这些数据表明应激刺激可能引发一系列神经肽相互作用,最终改变灵长类动物促性腺激素释放激素的脉冲式分泌,从而改变促性腺激素的分泌。

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