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脊髓5-羟色胺2受体亚型在胸段脊髓低位横断后喹哌嗪诱导的后肢运动中的作用。

Role of spinal 5-HT2 receptor subtypes in quipazine-induced hindlimb movements after a low-thoracic spinal cord transection.

作者信息

Ung Roth-V, Landry Eric S, Rouleau Pascal, Lapointe Nicolas P, Rouillard Claude, Guertin Pierre A

机构信息

Neuroscience Unit, Laval University Medical Center, Quebec City, QC, Canada.

出版信息

Eur J Neurosci. 2008 Dec;28(11):2231-42. doi: 10.1111/j.1460-9568.2008.06508.x. Epub 2008 Nov 3.

DOI:10.1111/j.1460-9568.2008.06508.x
PMID:19019202
Abstract

A role of serotonin receptors (5-HTRs) in spinal rhythmogenesis has been proposed several years ago based mainly upon data showing that bath-applied 5-HT could elicit locomotor-like rhythms in in vitro isolated spinal cord preparations. Such a role was partially confirmed in vivo after revealing that systemically administered 5-HTR(2) agonists, such as quipazine, could induce some locomotor-like movements (LM) in completely spinal cord-transected (Tx) rodents. However, given the limited binding selectivity of currently available 5-HTR(2) agonists, it has remained difficult to determine clearly if one receptor subtype is specifically associated with LM induction. In situ hybridization, data using tissues from L1-L2 spinal cord segments, where critical locomotor network elements have been identified in mice, revealed greater 5-HTR(2A) mRNA levels in low-thoracic Tx than non-Tx animals. This expression level remained elevated for several days, specifically in the lateral intermediate zone, where peak values were detected at 1 week post-Tx and returned to normal at 3 weeks post-Tx. Behavioral and kinematic analyses revealed quipazine-induced LM in 1-week Tx mice either non-pretreated or pretreated with selective 5-HTR(2B) and/or 5-HTR(2C) antagonists. In contrast, LM completely failed to be induced by quipazine in animals pretreated with selective 5-HTR(2A) antagonists. Altogether, these results provide strong evidence suggesting that 5-HTR(2A) are specifically associated with spinal locomotor network activation and LM generation induced by quipazine in Tx animals. These findings may contribute to design drug treatments aimed at promoting locomotor function recovery in chronic spinal cord-injured patients.

摘要

几年前就有人提出血清素受体(5 - HTRs)在脊髓节律发生中起作用,这主要基于以下数据:在体外分离的脊髓制剂中,浴加5 - 羟色胺(5 - HT)可引发类似运动的节律。在揭示全身施用5 - HTR(2)激动剂(如喹哌嗪)可在完全脊髓横断(Tx)的啮齿动物中诱导一些类似运动的运动(LM)后,这一作用在体内得到了部分证实。然而,鉴于目前可用的5 - HTR(2)激动剂的结合选择性有限,仍难以明确确定是否有一种受体亚型与LM诱导特异性相关。原位杂交数据显示,使用来自L1 - L2脊髓节段的组织(在小鼠中已确定关键的运动网络元件),低胸段Tx动物的5 - HTR(2A) mRNA水平高于未Tx动物。这种表达水平在几天内一直升高,特别是在外侧中间区,在Tx后1周检测到峰值,并在Tx后3周恢复正常。行为和运动学分析表明,喹哌嗪可在未预处理或用选择性5 - HTR(2B)和/或5 - HTR(2C)拮抗剂预处理的1周Tx小鼠中诱导LM。相反,在用选择性5 - HTR(2A)拮抗剂预处理的动物中,喹哌嗪完全无法诱导LM。总之,这些结果提供了有力证据,表明5 - HTR(2A)与Tx动物中喹哌嗪诱导的脊髓运动网络激活和LM产生特异性相关。这些发现可能有助于设计旨在促进慢性脊髓损伤患者运动功能恢复的药物治疗。

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