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猴中枢神经系统前脑的Trk免疫反应性

trk-immunoreactivity in the monkey central nervous system: forebrain.

作者信息

Kordower J H, Chen E Y, Sladek J R, Mufson E J

机构信息

Department of Neurological Sciences, Rush Presbyterian-St. Luke's Medical Center, Chicago, Illinois 60612.

出版信息

J Comp Neurol. 1994 Nov 1;349(1):20-35. doi: 10.1002/cne.903490103.

Abstract

Neurotrophins such as nerve growth factor (NGF) mediate their effects through interactions with high-affinity tropomycin-related kinase (trk) receptors. The present study employed a polyclonal antibody to characterize the distribution of trk-immunoreactive neurons within the nonhuman primate brain. Both young adult and aged cebus and rhesus monkeys displayed trk-immunoreactive neurons within all subdivisions of the basal forebrain. Colocalization studies revealed that between 66% and 76% of trk-immunoreactive basal forebrain neurons also expressed immunoreactivity for the low-affinity p75 NGF receptor, an excellent marker for cholinergic basal forebrain cells. In this experiment, most single-labeled basal forebrain neurons contained only trk immunoreactivity, whereas 4% of basal forebrain neurons expressed only the low-affinity p75 NGF receptor. Scattered trk-immunoreactive neurons also were observed within the caudate nucleus and putamen. Although dual-localization studies with choline acetyltransferase (ChAT) were not performed, striatal neurons codistributed with ChAT-immunoreactive cells, and both types of cells were similar in size and morphology. This suggests that trk immunoreactivity is expressed within cholinergic interneurons within the primate striatum. Finally, lightly stained trk-immunoreactive neurons were observed within the stratum oriens of the hippocampal formation and within the hypothalamus. These data indicate that both cholinergic and, possibly, noncholinergic forebrain neurons express the protein for the high-affinity trk receptor, which transduces the signal mediating the trophic effects of neurotrophins. In addition, the pattern of trk immunoreactivity was preserved in two aged (26 and 29 years old) rhesus monkeys, suggesting that the expression of trk, for the most part, is sustained throughout the lifetime of the organism.

摘要

神经营养因子,如神经生长因子(NGF),通过与高亲和力原肌球蛋白相关激酶(trk)受体相互作用来介导其效应。本研究采用多克隆抗体来表征非人类灵长类动物大脑中trk免疫反应性神经元的分布。成年和老年的僧帽猴和恒河猴在基底前脑的所有亚区均显示出trk免疫反应性神经元。共定位研究表明,66%至76%的trk免疫反应性基底前脑神经元也表达低亲和力p75 NGF受体的免疫反应性,p75 NGF受体是胆碱能基底前脑细胞的优良标志物。在本实验中,大多数单标记的基底前脑神经元仅含有trk免疫反应性,而4%的基底前脑神经元仅表达低亲和力p75 NGF受体。在尾状核和壳核内也观察到散在的trk免疫反应性神经元。尽管未进行与胆碱乙酰转移酶(ChAT)的双重定位研究,但纹状体神经元与ChAT免疫反应性细胞共分布,且两种类型的细胞在大小和形态上相似。这表明trk免疫反应性在灵长类纹状体内的胆碱能中间神经元中表达。最后,在海马结构的 Oriens 层和下丘脑内观察到轻度染色的trk免疫反应性神经元。这些数据表明,胆碱能和可能的非胆碱能前脑神经元均表达高亲和力trk受体的蛋白,该受体转导介导神经营养因子营养作用的信号。此外,trk免疫反应性模式在两只老年(26岁和29岁)恒河猴中得以保留,这表明trk的表达在生物体的一生中大部分时间是持续的。

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