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成年和老年Fischer-344大鼠持续脑内注射神经生长因子后乙酰胆碱的合成与释放

Acetylcholine synthesis and release following continuous intracerebral administration of NGF in adult and aged Fischer-344 rats.

作者信息

Rylett R J, Goddard S, Schmidt B M, Williams L R

机构信息

Department of Physiology, University of Western Ontario, London, Canada.

出版信息

J Neurosci. 1993 Sep;13(9):3956-63. doi: 10.1523/JNEUROSCI.13-09-03956.1993.

Abstract

NGF promotes the survival and enhances the neurotransmitter phenotype of basal forebrain and striatal cholinergic neurons in brain of rat. The objective of the present study was to determine whether stimulations of the cholinergic neuronal markers ChAT and high-affinity choline uptake are reflected in enhanced synthesis and release of ACh. Enhancement of ACh release in brain of adult and aged rats could result in increased cholinergic neurotransmission, and altered animal behavior. NGF (1.2 micrograms/d) was administered intracerebroventricularly for 2 weeks by osmotic minipump to male Fischer-344 rats aged 4 and 24 months. Cholinergic neuronal functional parameters were measured in frontal cortex, hippocampus, and striatum. In young adult rats, increased ChAT and choline uptake activities were accompanied by enhanced ACh synthesis, basal and depolarization-induced release of both endogenous and newly synthesized transmitter, with the largest effect generally being observed in striatum. In aged animals, the responses to NGF were less uniform. Whereas the pattern for changes in ChAT activity was similar to that seen in younger animals, choline uptake activity was increased only in frontal cortex and striatum. Coincidentally, ACh synthesis was also increased only in these two brain regions. ACh content of synaptosomes was not affected by age or NGF treatment, and the ACh levels in microwaved samples of striatum and basal forebrain were not affected by NGF treatment. However, profound deficits in both basal and evoked release of newly synthesized ACh were observed in the aged rats. NGF treatment had no significant effect on the basal release of newly synthesized ACh in aged rats.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

神经生长因子(NGF)可促进大鼠脑内基底前脑和纹状体胆碱能神经元的存活并增强其神经递质表型。本研究的目的是确定胆碱能神经元标志物胆碱乙酰转移酶(ChAT)和高亲和力胆碱摄取的刺激是否反映在乙酰胆碱(ACh)合成和释放的增强上。成年和老年大鼠脑内ACh释放的增强可能导致胆碱能神经传递增加以及动物行为改变。通过渗透微型泵向4个月和24个月大的雄性Fischer-344大鼠脑室内注射NGF(1.2微克/天),持续2周。在额叶皮质、海马体和纹状体中测量胆碱能神经元功能参数。在年轻成年大鼠中,ChAT和胆碱摄取活性增加伴随着ACh合成增强,内源性和新合成递质的基础释放和去极化诱导释放均增强,其中纹状体的效应通常最大。在老年动物中,对NGF的反应不太一致。虽然ChAT活性的变化模式与年轻动物相似,但胆碱摄取活性仅在额叶皮质和纹状体中增加。巧合的是,ACh合成也仅在这两个脑区增加。突触体的ACh含量不受年龄或NGF处理的影响,纹状体和基底前脑微波处理样本中的ACh水平也不受NGF处理的影响。然而,在老年大鼠中观察到新合成ACh的基础释放和诱发释放均存在严重缺陷。NGF处理对老年大鼠新合成ACh的基础释放没有显著影响。(摘要截短至250字)

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