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对氯苯丙胺对三叉神经运动核5-羟色胺能神经支配的神经毒性作用:一项逆行运输研究。

Neurotoxic effects of p-chloroamphetamine on the serotoninergic innervation of the trigeminal motor nucleus: a retrograde transport study.

作者信息

Fritschy J M, Lyons W E, Molliver M E, Grzanna R

机构信息

Johns Hopkins University School of Medicine, Department of Neuroscience, Baltimore, MD 21205.

出版信息

Brain Res. 1988 Nov 15;473(2):261-70. doi: 10.1016/0006-8993(88)90855-4.

Abstract

The rat forebrain receives projections from both dorsal and median raphe nuclei. It has recently been shown that serotoninergic axons arising from the dorsal raphe nucleus, but not those from the median raphe nucleus, degenerate following systemic administration of p-chloroamphetamine (PCA). The present study was conducted to determine (i) whether the motor nucleus of the trigeminal nerve is innervated by overlapping projections from multiple serotonin cell groups and (ii) whether a particular subset of serotoninergic axon terminals in the trigeminal motor nucleus are sensitive to the neurotoxic effects of PCA. Retrograde transport was used in combination with immunofluorescence to identify the serotonin-positive cells that project to the trigeminal motor nucleus both in control rats and in rats previously treated with PCA. In untreated rats, an average of 95 retrogradely labeled serotonin-positive neurons were found in the dorsal raphe nucleus, 135 in the nucleus raphe obscurus, 132 in the nucleus raphe pallidus and 63 in the ventrolateral medulla. After treatment with PCA, there was a marked decrease (-77%) in the number of retrogradely labeled serotoninergic neurons in the dorsal raphe nucleus, whereas the number of labeled neurons was unchanged in the raphe obscurus and raphe pallidus. These results demonstrate that PCA selectively lesions serotonin axon terminals arising from the dorsal raphe nucleus, while sparing projections from the raphe obscurus and raphe pallidus to the trigeminal motor nucleus. This conclusion is in agreement with previous findings that in the forebrain only axons from the dorsal raphe are vulnerable to PCA. The data provide further evidence that serotoninergic axons originating in the dorsal raphe nucleus differ from other serotoninergic axons in their pharmacological properties and that the dorsal raphe may contain a functionally unique subset of serotonin neurons.

摘要

大鼠前脑接受来自背侧和中缝核的投射。最近有研究表明,系统给予对氯苯丙胺(PCA)后,起源于背侧中缝核的5-羟色胺能轴突会发生退化,而起源于中缝正中核的轴突则不会。本研究旨在确定:(i)三叉神经运动核是否由多个5-羟色胺细胞群的重叠投射所支配;(ii)三叉神经运动核中特定的5-羟色胺能轴突终末亚群是否对PCA的神经毒性作用敏感。采用逆行运输结合免疫荧光技术,以鉴定对照组大鼠和先前经PCA处理的大鼠中投射至三叉神经运动核的5-羟色胺阳性细胞。在未处理的大鼠中,平均有95个逆行标记的5-羟色胺阳性神经元位于背侧中缝核,135个位于中缝隐核,132个位于中缝苍白核,63个位于延髓腹外侧。经PCA处理后,背侧中缝核中逆行标记的5-羟色胺能神经元数量显著减少(-77%),而中缝隐核和中缝苍白核中标记神经元的数量未发生变化。这些结果表明,PCA选择性地损伤起源于背侧中缝核的5-羟色胺轴突终末,同时保留中缝隐核和中缝苍白核至三叉神经运动核的投射。这一结论与先前的研究结果一致,即在大脑前叶,只有来自背侧中缝核的轴突易受PCA影响。这些数据进一步证明,起源于背侧中缝核的5-羟色胺能轴突在药理学特性上不同于其他5-羟色胺能轴突,并且背侧中缝核可能包含功能独特的5-羟色胺能神经元亚群。

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