首页> 美国卫生研究院文献>The Journal of Neuroscience >Type A GABA-Receptor-Dependent Synaptic Transmission Sculpts Dendritic Arbor Structure in Xenopus Tadpoles In Vivo
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Type A GABA-Receptor-Dependent Synaptic Transmission Sculpts Dendritic Arbor Structure in Xenopus Tadpoles In Vivo

机译:爪蟾体内的A型GABA受体依赖性突触传递雕刻树突状乔木结构。

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摘要

The emergence of dendritic arbor structure in vivo depends on synaptic inputs. We tested whether inhibitory GABAergic synaptic transmission regulates Xenopus optic tectal cell dendritic arbor development in vivo by expressing a peptide corresponding to an intracellular loop (ICL) of the γ2 subunit of type A GABA receptors (GABAAR), which is required to anchor GABAA receptors to the postsynaptic scaffold. Enhanced green fluorescent protein (EGFP)-tagged ICL (EGFP-ICL) was distributed in a punctate pattern at putative inhibitory synapses, identified by vesicular GABA transporter immunoreactive puncta. ICL expression completely blocked GABAAR-mediated transmission in 36% of transfected neurons and significantly reduced GABAAR-mediated synaptic currents relative to AMPA receptor-mediated synaptic currents in the remaining transfected neurons without altering release probability or neuronal excitability. Further analysis of ICL-expressing neurons with residual GABAAR-mediated inputs showed that the capacity of benzodiazepine to enhance GABAergic synaptic responses was reduced in ICL-expressing neurons, indicating that they were likely depleted of γ2 subunit-containing GABAAR. Neurons expressing a mutant form of ICL were comparable to controls. In vivo time-lapse images showed that ICL-expressing neurons have more sparsely branched dendritic arbors, which expand over larger neuropil areas than EGFP-expressing control neurons. Analysis of branch dynamics indicated that ICL expression affected arbor growth by reducing rates of branch addition. Furthermore, we found that decreasing GABAergic synaptic transmission with ICL expression blocked visual experience dependent dendritic arbor structural plasticity. Our findings establish an essential role for inhibitory GABAergic synaptic transmission in the regulation of dendritic structural plasticity in Xenopus in vivo.
机译:体内树突状乔木结构的出现取决于突触输入。我们通过表达对应于A型GABA受体(GABAAR)的γ2亚基的细胞内环(ICL)的肽来测试抑制性GABA能突触传递是否在体内调节非洲爪蟾的视神经顶盖树突状细胞的发育,这需要将GABAA受体锚定到突触后支架。增强的绿色荧光蛋白(EGFP)标记的ICL(EGFP-ICL)呈点状分布在假定的抑制性突触上,通过水泡GABA转运蛋白免疫反应性小点识别。与其余转染的神经元中AMPA受体介导的突触电流相比,ICL表达完全阻断了36%的转染神经元中GABAAR介导的突触电流,并显着降低了GABAAR介导的突触电流,而没有改变释放概率或神经元兴奋性。带有残留GABAAR介导的输入的ICL表达神经元的进一步分析表明,在表达ICL的神经元中苯二氮卓增强GABA能突触反应的能力降低,表明它们很可能耗尽了含γ2亚基的GABAAR。表达ICL突变形式的神经元与对照组相当。体内延时图像显示,表达ICL的神经元具有较稀疏的分支树突状树突,其比表达EGFP的对照神经元在更大的神经柱区域扩展。分支动力学分析表明,ICL表达通过降低分支添加速率影响了乔木的生长。此外,我们发现,以ICL表达降低GABA能突触传递可阻断视经验依赖的树突状乔木结构可塑性。我们的发现建立了抑制GABA能突触传递在调节非洲爪蟾体内的树突状结构可塑性中的重要作用。

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