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大鼠脑中GABAB受体剪接变体GB1a和GB1b:发育调控、细胞分布及突触外定位

GABAB-receptor splice variants GB1a and GB1b in rat brain: developmental regulation, cellular distribution and extrasynaptic localization.

作者信息

Fritschy J M, Meskenaite V, Weinmann O, Honer M, Benke D, Mohler H

机构信息

Institute of Pharmacology, Swiss Federal Institute of Technology (ETH),University of Zürich, Switzerland.

出版信息

Eur J Neurosci. 1999 Mar;11(3):761-8. doi: 10.1046/j.1460-9568.1999.00481.x.

Abstract

GABAB (gamma-aminobutyric acid)-receptors have been implicated in central nervous system (CNS) functions, e.g. cognition and pain perception, and dysfunctions including spasticity and absence epilepsy. To permit an analysis of the two known GABAB-receptor splice variants GABAB-R1a (GB1a) and GABAB-R1b (GB1b), their distribution pattern has been differentiated in the rat brain, using Western blotting and immunohistochemistry with isoform-specific antisera. During postnatal maturation, the expression of the two splice variants was differentially regulated with GB1a being preponderant at birth. In adult brain, GB1b-immunoreactivity (-IR) was predominant, and the two isoforms largely accounted for the pattern of GABAB-receptor binding sites in the brain. Receptor heterogeneity was pronounced in the hippocampus, where both isoforms occurred in CA1, but only GB1b in CA3. Similarly, in the cerebellum, GB1b was exclusively found in Purkinje cells in a zebrin-like pattern. The staining was most pronounced in Purkinje cell dendrites and spines. Using electron microscopy, over 80% of the spine profiles in which a synaptic contact with a parallel fibre was visible contained GB1b-IR at extrasynaptic sites. This subcellular localization is unrelated to GABAergic inputs, indicating that the role of GABAB-receptors in vivo extends beyond synaptic GABAergic neurotransmission and may, in the cerebellum, involve taurine as a ligand.

摘要

γ-氨基丁酸(GABAB)受体与中枢神经系统(CNS)功能有关,如认知和痛觉感知,以及包括痉挛和失神癫痫在内的功能障碍。为了分析两种已知的GABAB受体剪接变体GABAB-R1a(GB1a)和GABAB-R1b(GB1b),利用蛋白质免疫印迹法和针对亚型的抗血清进行免疫组织化学,在大鼠脑中区分了它们的分布模式。在出生后成熟过程中,两种剪接变体的表达受到不同调节,GB1a在出生时占优势。在成体脑中,GB1b免疫反应性(-IR)占主导,这两种亚型在很大程度上构成了脑中GABAB受体结合位点的模式。受体异质性在海马体中很明显,两种亚型都出现在CA1区,但CA3区只有GB1b。同样,在小脑中,GB1b仅以斑马蛋白样模式存在于浦肯野细胞中。染色在浦肯野细胞树突和棘中最为明显。利用电子显微镜,超过80%与平行纤维有突触接触的棘状突起在突触外位点含有GB1b-IR。这种亚细胞定位与GABA能输入无关,表明GABAB受体在体内的作用超出了突触GABA能神经传递,在小脑中可能涉及牛磺酸作为配体。

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