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大脑中氟硝西泮结合与去甲肾上腺素能神经支配密度的平行变化。

Parallel changes in brain flunitrazepam binding and density of noradrenergic innervation.

作者信息

Medina J H, Novas M L

出版信息

Eur J Pharmacol. 1983 Apr 8;88(4):377-82. doi: 10.1016/0014-2999(83)90589-7.

Abstract

The neonatal injection of neurotoxic compounds such as 6-hydroxydopa (6-OH-DOPA) and DSP 4 (N-(2-chloroethyl)-N-ethyl-2-bromobenzylamine hydrochloride) produces marked changes in the development of central noradrenergic neurons, i.e. permanent denervation of the cerebral cortex and hyperinnervation of the brain stem and the cerebellum. Adult animals treated at birth with both neurotoxins were used to study the binding of [3H]flunitrazepam (FNZ) to membranes isolated from these regions. The administration of both toxins produced a marked and similar increase in the number of FNZ binding sites in the cerebellum. In the brain stem, 6-OH-DOPA increased the density of these receptors much more than DSP 4 (33% vs. 13%), a difference similar to that observed between the effects of both compounds on brain stem NA. In the cerebral cortex, both compounds reduced the maximal number of FNZ binding sites. No changes were observed in the affinity of FNZ binding sites in the different structures. When adult rats treated at birth with 6-OH-DOPA received an injection of DSP 4 7 days later, the number of FNZ binding sites was reduced by 43% in the cerebellum, 53% in the brain stem and 11% in the cerebral cortex. In these structures, DSP 4 reduced the absolute number of FNZ binding sites to the same level both in rats treated at birth with 6-OH-DOPA and in non-treated animals receiving DSP 4 7 days before killing. These results are further support for the existence of close parallelism between the density of benzodiazepine receptors, as demonstrated by FNZ binding, and the density of brain noradrenergic innervation.

摘要

新生动物注射神经毒性化合物,如6-羟基多巴胺(6-OH-DOPA)和DSP 4(N-(2-氯乙基)-N-乙基-2-溴苄胺盐酸盐),会使中枢去甲肾上腺素能神经元的发育产生显著变化,即大脑皮质永久性去神经支配以及脑干和小脑的神经支配过度。用这两种神经毒素在出生时处理成年动物,以研究[3H]氟硝西泮(FNZ)与从这些区域分离的膜的结合情况。两种毒素的施用均使小脑中FNZ结合位点的数量显著且类似地增加。在脑干中,6-OH-DOPA比DSP 4更能增加这些受体的密度(分别为33%和13%),这一差异类似于两种化合物对脑干去甲肾上腺素(NA)作用所观察到的差异。在大脑皮质中,两种化合物均降低了FNZ结合位点的最大数量。在不同结构中,FNZ结合位点的亲和力未观察到变化。当出生时用6-OH-DOPA处理的成年大鼠在7天后注射DSP 4时,小脑中FNZ结合位点的数量减少了43%,脑干中减少了53%,大脑皮质中减少了11%。在这些结构中,DSP 4将FNZ结合位点的绝对数量降低到与出生时用6-OH-DOPA处理的大鼠以及在处死前7天接受DSP 4处理的未处理动物相同的水平。这些结果进一步支持了通过FNZ结合所证明的苯二氮䓬受体密度与脑去甲肾上腺素能神经支配密度之间存在密切平行关系。

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