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首页> 外文期刊>Frontiers in Cellular Neuroscience >Enrichment of GABAA Receptor α-Subunits on the Axonal Initial Segment Shows Regional Differences
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Enrichment of GABAA Receptor α-Subunits on the Axonal Initial Segment Shows Regional Differences

机译:轴突初始节段上的GABA A受体α-亚基的富集显示出区域差异

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Although it is generally recognized that certain α-subunits of γ-aminobutyric acid type A receptors (GABAARs) form enriched clusters on the axonal initial segment (AIS), the degree to which these clusters vary in different brain areas is not well known. In the current study, we quantified the density, size, and enrichment ratio of fluorescently labeled α1-, α2-, or α3-subunits aggregates co-localized with the AIS-marker ankyrin G and compared them to aggregates in non-AIS locations among different brain areas including hippocampal subfields, basal lateral amygdala (BLA), prefrontal cortex (PFC), and sensory cortex (CTX). We found regional differences in the enrichment of GABAAR α-subunits on the AIS. Significant enrichment was identified in the CA3 of hippocampus for α1-subunits, in the CA1, CA3, and BLA for α2-subunits, and in the BLA for α3-subunits. Using α-subunit knock-out (KO) mice, we found that BLA enrichment of α2- and α3-subunits were physiologically independent of each other, as the enrichment of one subunit was unaffected by the genomic deletion of the other. To further investigate the unique pattern of α-subunit enrichment in the BLA, we examined the association of α2- and α3-subunits with the presynaptic vesicular GABA transporter (vGAT) and the anchoring protein gephyrin (Geph). As expected, both α2- and α3-subunits on the AIS within the BLA received prominent GABAergic innervation from vGAT-positive terminals. Further, we found that the association of α2- and α3-subunits with Geph was weaker in AIS versus non-AIS locations, suggesting that Geph might be playing a lesser role in the enrichment of α2- and α3-subunits on the AIS. Overall, these observations suggest that GABAARs on the AIS differ in subunit composition across brain regions. As with somatodendritic GABAARs, the distinctive expression pattern of AIS-located GABAAR α-subunits in the BLA, and other brain areas, likely contribute to unique forms of GABAergic inhibitory transmission and pharmacological profiles seen in different brain areas.
机译:尽管通常公认的是,γ-氨基丁酸A型受体(GABAARs)的某些α亚基在轴突起始节(AIS)上形成了富集簇,但是这些簇在不同脑区的变化程度尚不为人所知。在当前的研究中,我们量化了与AIS标记锚蛋白G共定位的荧光标记的α1,α2或α3亚基聚集体的密度,大小和富集率,并将它们与非AIS标记中的聚集体进行了比较。不同的大脑区域,包括海马亚区,基底外侧杏仁核(BLA),前额叶皮层(PFC)和感觉皮层(CTX)。我们发现AIS上GABAARα亚基富集的区域差异。在海马CA3中,对于α1亚基,CA1,CA3和BLA中对于α2-亚基以及在BLA中对于α3-亚基,都发现了显着的富集。使用α-亚基敲除(KO)小鼠,我们发现α2-和α3-亚基的BLA富集在生理上是相互独立的,因为一个亚基的富集不受另一个基因组缺失的影响。为了进一步研究BLA中α亚基富集的独特模式,我们研究了α2和α3亚基与突触前囊泡GABA转运蛋白(vGAT)和锚蛋白gephyrin(Geph)的关联。如预期的那样,BLA内AIS上的α2-和α3-亚基都接受了来自vGAT阳性末端的突出的GABA能神经支配。此外,我们发现在AIS中,α2-和α3-亚基与Geph的关联较非AIS弱,这表明Geph在AIS中α2-和α3-亚基富集中的作用可能较小。总体而言,这些观察结果表明,AIS上的GABAAR在整个大脑区域的亚基组成上有所不同。与树突状GABAAR一样,位于BLA和其他大脑区域中位于AIS的GABAARα亚基的独特表达模式,可能有助于在不同大脑区域看到的独特形式的GABA能抑制传递和药理学特征。

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