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关于β,β'-亚氨基二丙腈(IDPN)对大鼠影响的区域神经化学研究。

Regional neurochemical studies on the effect of beta, beta'-iminodipropionitrile (IDPN) in the rat.

作者信息

Langlais P J, Huang P C, Gabay S

出版信息

J Neurosci Res. 1975;1(5-6):419-35. doi: 10.1002/jnr.490010510.

Abstract

A permanent hyperkinetic syndrome, characterized by excitation, choreiform head and neck movements and circling, which has led to it being called collectively the "ECC-syndrome," is induced in rats by the daily IP administration of beta, beta'-iminodipropionitrile (IDPN), 300 mg/kg, for 7 days. The levels of the biogenic amines, norepinephrine (NE), dopamine (DA), serotonin (5-HT) and its metabolite 5-hydroxyindoleacetic acid (5-HIAA), were measured in the striatum, midbrain, medulla, cortex, and cerebellum on the day the syndrome appeared (day 7) and one week later (day 14). The biogenic amine most affected by IDPN administration was 5-HT. On day 7, striatal 5-HT levels increased and 5-HIAA levels decreased while in the medulla and midbrain, 5-HIAA levels increased. On day 14, significant reductions in both 5-HT, in the midbrain, striatum, and cortex, and 5-HIAA, in all regions except the cortex, were observed. NE was markedly increased in the medulla, midbrain, and striatum on day 7, whereas on day 14 it was found to be within the normal range in these same regions. With the exception of a slight, but significant, increase in the cortex on day 7, DA levels in all regions were found to be relatively unaffected by IDPN administration on both day 7 and day 14. In an attempt to detect degenerative changes which might be taking place in the brain and which might provide an explanation for the permanency of the behavioral disturbances, the uptake of [3H]-labeled NE, DA, and 5-HT into synaptosomal-rich preparations of striatum and the uptake of NE and 5-HT into the midbrain area were compared between normal and syndromized rats on both day 7 and day 14. Small changes were observed but they were not statistically significant. The alterations of 5-HT and 5-HIAA levels in several regions of the brain under the conditions examined may indicate that IDPN's neurotoxicity primarily affects 5-HT-containing neurones. The active membrane transporting system of the nerve endings studied, however, remained relatively intact. This latter finding eliminates the possibility that neuronal degeneration in these areas is responsible for the decreased 5-HT and 5-HIAA levels or is the pathology underlying the permanency of the syndrome. These results are evaluated in terms of a possible model for hyperkinetic disorders.

摘要

通过每天腹腔注射300毫克/千克的β,β'-亚氨基二丙腈(IDPN),连续7天,可在大鼠中诱发一种永久性运动亢进综合征,其特征为兴奋、头部和颈部的舞蹈样运动以及转圈,这使得它被统称为“ECC综合征”。在该综合征出现的当天(第7天)和一周后(第14天),测量纹状体、中脑、延髓、皮质和小脑中生物胺去甲肾上腺素(NE)、多巴胺(DA)、5-羟色胺(5-HT)及其代谢产物5-羟吲哚乙酸(5-HIAA)的水平。受IDPN给药影响最大的生物胺是5-HT。在第7天,纹状体中5-HT水平升高而5-HIAA水平降低,而在延髓和中脑中,5-HIAA水平升高。在第14天,观察到中脑、纹状体和皮质中的5-HT以及除皮质外所有区域中的5-HIAA均显著降低。在第7天,延髓、中脑和纹状体中的NE显著升高,而在第14天,发现这些相同区域中的NE处于正常范围内。除了第7天皮质中有轻微但显著的升高外,在第7天和第14天,所有区域中的DA水平相对不受IDPN给药的影响。为了检测大脑中可能正在发生的退行性变化,并为行为障碍的永久性提供解释,比较了正常大鼠和患综合征大鼠在第7天和第14天纹状体富含突触体的制剂中[3H]标记的NE、DA和5-HT的摄取以及中脑区域中NE和5-HT的摄取。观察到有小的变化,但它们没有统计学意义。在所研究的条件下,大脑几个区域中5-HT和5-HIAA水平的改变可能表明IDPN的神经毒性主要影响含5-HT的神经元。然而,所研究的神经末梢的活性膜转运系统保持相对完整。后一个发现排除了这些区域中神经元变性是5-HT和5-HIAA水平降低的原因或该综合征永久性的病理学基础的可能性。根据运动亢进性疾病的可能模型对这些结果进行了评估。

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