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大鼠尾状核-壳核中含P物质受体的神经元中AMPA受体亚基的差异表达。

Differential expression of AMPA receptor subunits in substance P receptor-containing neurons of the caudate-putamen of rats.

作者信息

Hu H-J, Chen L-W, Yung K K L, Chan Y S

机构信息

Institute of Neurosciences, The Fourth Military Medical University, Xi'an 710032, PR China.

出版信息

Neurosci Res. 2004 Jul;49(3):281-8. doi: 10.1016/j.neures.2004.03.003.

Abstract

Previous evidence has suggested that glutamate-driving neurotransmission and glutamate-excitotoxicity are modulated by substance P in the basal ganglia, but the assembly of glutamate receptors mediating this process remains to be delineated. By using a double immunofluorescence, cellular expression of alpha-amino-3-hydroxy-5-methyl-4-isoxazole propionate (AMPA) receptor subunits (GluR1-4) in substance P receptor (SPR)-containing neurons was examined in the striatum of rats. It revealed that distribution of SPR-immunoreactive neurons completely overlapped with that of GluR1, 2, 3 or 4-immunoreactive neurons in the caudate-putamen. Neurons showing both SPR and AMPA receptor subunits (except of GluR3)-immunoreactivity were observed: all (100%) of SPR-positive neurons displayed GluR1-, GluR2- or GluR4-immunoreactivity, and the double-labeled neurons constituted about 33, 3 or 29% of total GluR-positive ones. In contrast, the neurons exhibiting both SPR- and GluR3-immunoreactivity were not detected, though numerous GluR3-positive neurons were still distributed in the caudate-putamen regions. Co-localization of SPR and distinct AMPA receptor subunits in the striatal neurons has provided a basis for functional modulation of neuronal APMA receptors by substance P in the caudate-putamen of rodents. Taken together with previous observations, this study has also suggested that, through interaction with AMPA receptors composed of subunits 1, 2 and 4, substance P or neurokinin peptides may play important roles in regulating neuronal properties and protecting neurons from excitotoxicity in the basal ganglia of mammals.

摘要

先前的证据表明,在基底神经节中,P物质可调节谷氨酸驱动的神经传递和谷氨酸兴奋性毒性,但介导这一过程的谷氨酸受体组装情况仍有待阐明。通过双免疫荧光法,检测了大鼠纹状体中含P物质受体(SPR)的神经元中α-氨基-3-羟基-5-甲基-4-异恶唑丙酸(AMPA)受体亚基(GluR1-4)的细胞表达。结果显示,在尾状核-壳核中,SPR免疫反应性神经元的分布与GluR1、2、3或4免疫反应性神经元的分布完全重叠。观察到同时显示SPR和AMPA受体亚基(除GluR3外)免疫反应性的神经元:所有(100%)SPR阳性神经元均显示GluR1、GluR2或GluR4免疫反应性,双标记神经元约占总GluR阳性神经元的33%、3%或29%。相比之下,尽管尾状核-壳核区域仍分布着大量GluR3阳性神经元,但未检测到同时显示SPR和GluR3免疫反应性的神经元。纹状体神经元中SPR与不同AMPA受体亚基的共定位为啮齿动物尾状核-壳核中P物质对神经元APMA受体的功能调节提供了依据。结合先前的观察结果,本研究还表明,通过与由亚基1、2和4组成的AMPA受体相互作用,P物质或神经激肽肽可能在调节哺乳动物基底神经节中神经元特性以及保护神经元免受兴奋性毒性方面发挥重要作用。

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