Differentiation of corticothalamic and collateral thalamocortical synapses on mouse reticular nucleus neurons by EPSC amplitude and AMPA receptor subunit composition

Xiao-Bo Liu, Sonia Bolea, Peyman Golshani, Edward G Jones
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引用次数: 34

Abstract

AMPA receptors mediate fast synaptic transmission at collateral synapses of corticothalamic and thalamocortical axons in the thalamic reticular nucleus (RTN). These synapses are important in generating synchrony in the thalamocortical network. Whole cell recording in the mouse thalamocortical slice preparation was combined with high-resolution immunoelectron microscopy to characterize AMPA-mediated conductances at the two synapses and to correlate these with differential expression of GluR3 and GluR4 subunits. Thalamocortical collateral (TC) synapses had larger mean EPSC amplitudes (1914±1814 pS) than corticothalamic (CT) synapses (400±257 pS), and rise and decay times of TC EPSCs were faster and less variable than CT EPSCs, probably reflecting proximal and dispersed locations of TC and CT terminals, respectively, on RTN cells. In situ hybridization and immunocytochemical studies revealed that GluR1 and GluR2 subunits are not expressed in the RTN and GluR4 subunits are expressed at higher levels than GluR3 subunits. Immunoelectron microscopy revealed gold particles representing GluR3 or GluR4 subunits concentrated at single postsynaptic densities (PSD) characteristic of CT synapses and at the two to seven split PSD segments characteristic of TC synapses. At CT synapses the number and density of GluR4 particles were 2.5 times greater than GluR3 particles. At the larger TC synapses, the number of GluR3 particles exceeded that of GluR4 particles but density of GluR4 particles was lower than at CT synapses while density of GluR3 particles was similar. Despite enrichment of GluR4 subunits at CT synapses, larger conductances prevailed at thalamocortical collateral synapses, probably reflecting both larger overall numbers of AMPA receptors and a greater number of release sites represented by the split PSDs. Variability in amplitudes of TC EPSCs may reflect variability in the number of release sites; lower variability in CT EPSC amplitudes may reflect a more constant number of release sites.

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EPSC振幅和AMPA受体亚基组成对小鼠网状核神经元皮质丘脑和侧丘脑皮质突触分化的影响
AMPA受体介导丘脑网状核(RTN)皮质丘脑和丘脑皮质轴突侧侧突触的快速突触传递。这些突触在丘脑皮质网络中产生同步是重要的。小鼠丘脑皮质切片制备中的全细胞记录与高分辨率免疫电镜相结合,以表征ampa介导的两个突触的传导,并将其与GluR3和GluR4亚基的差异表达联系起来。丘脑皮质侧支(TC)突触的EPSC平均振幅(1914±1814 pS)大于皮质丘脑(CT)突触(400±257 pS), TC EPSC的上升和衰减时间比CT EPSC更快,变化更少,可能反映了TC和CT终端分别位于RTN细胞的近端和分散位置。原位杂交和免疫细胞化学研究表明,GluR1和GluR2亚基在RTN中不表达,而GluR4亚基的表达水平高于GluR3亚基。免疫电镜显示,代表GluR3或GluR4亚基的金颗粒集中在CT突触特征的单个突触后密度(PSD)和TC突触特征的2至7个分裂的PSD节段。在CT突触处,GluR4颗粒的数量和密度是GluR3颗粒的2.5倍。在较大的TC突触中,GluR3颗粒的数量超过GluR4颗粒,但GluR4颗粒的密度低于CT突触,而GluR3颗粒的密度与TC突触相似。尽管GluR4亚基在CT突触中富集,但丘脑皮质侧支突触的传导性更大,这可能反映了AMPA受体的总体数量更多,以及分裂的psd所代表的释放位点更多。TC EPSCs振幅的变异性可能反映了释放位点数量的变异性;CT EPSC振幅的变异性较低可能反映了释放位点的数量更恒定。
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