首页> 美国卫生研究院文献>Frontiers in Neuroanatomy >TRPC1 Channels Are Expressed in Pyramidal Neurons and in a Subset of Somatostatin Interneurons in the Rat Neocortex
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TRPC1 Channels Are Expressed in Pyramidal Neurons and in a Subset of Somatostatin Interneurons in the Rat Neocortex

机译:TRPC1通道在大鼠新皮层中的锥体神经元和生长抑素中间神经元子集中表达。

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摘要

Disturbances in calcium homeostasis due to canonical transient receptor potential (TRPC) and/or store-operated calcium (SOC) channels can play a key role in a large number of brain disorders. TRPC channels are plasma membrane cation channels included in the transient receptor potential (TRP) superfamily. The most widely distributed member of the TRPC subfamily in the brain is TRPC1, which is frequently linked to group I metabotropic glutamate receptors (mGluRs) and to the components of SOC channels. Proposing TRPC/SOC channels as a therapeutic target in neurological diseases previously requires a detailed knowledge of the distribution of such molecules in the brain. The aim of our study was to analyze the neuroanatomical distribution of TRPC1 in the rat neocortex. By double- and triple-labeling and confocal microscopy, we tested the presence of TRPC1 by using a series of specific neurochemical markers. TRPC1 was abundant in SMI 32-positive pyramidal neurons, and in some glutamic acid decarboxylase 67 (GAD67) interneurons, but was lacking in glial fibrillary acidic protein (GFAP)-positive glial cells. In neurons it colocalized with postsynaptic marker MAP2 in cell bodies and apical dendritic trunks and it was virtually absent in synaptophysin-immunoreactive terminals. By using a panel of antibodies to classify interneurons, we identified the GABAergic interneurons that contained TRPC1. TRPC1 was lacking in basket and chandelier parvalbumin (PVALB) cells, and a very low percentage of calretinin (CALR) or calbindin (CALB) interneurons expressed TRPC1. Moreover, 63% of somatostatin (SST) expressing-cells and 37% of reelin-positive cells expressed TRPC1. All the SST/TRPC1 double-labeled cells, many of which were presumptive Martinotti cells (MC), were positive for reelin. The presence of TRPC1 in the somata and apical dendritic trunks of neocortical pyramidal cells suggests a role for this channel in sensory processing and synaptic plasticity. Conversely in SST/reelin interneurons, TRPC1 could modulate GABAergic transmission, which is responsible for shaping the coordinated activity of the pyramidal cells in the cortical network. In future studies, it would be relevant to investigate whether TRPC1 could be involved in the expression or processing of reelin in SST inhibitory interneurons.
机译:由于典型的瞬态受体电位(TRPC)和/或钙离子操纵的钙(SOC)通道引起的钙稳态紊乱在许多脑部疾病中起关键作用。 TRPC通道是瞬时受体电位(TRP)超家族中包含的质膜阳离子通道。 TRPC亚家族在大脑中分布最广泛的成员是TRPC1,它经常与I组代谢型谷氨酸受体(mGluRs)和SOC通道的成分相关。提议将TRPC / SOC通道作为神经系统疾病的治疗靶标,以前需要对此类分子在大脑中的分布有详细的了解。我们研究的目的是分析大鼠新皮层中TRPC1的神经解剖分布。通过双重和三次标记和共聚焦显微镜,我们通过使用一系列特定的神经化学标记物测试了TRPC1的存在。 TRPC1在SMI 32阳性锥体神经元和某些谷氨酸脱羧酶67(GAD67)中间神经元中含量丰富,但在胶质原纤维酸性蛋白(GFAP)阳性胶质细胞中缺乏。在神经元中,它与突触后标记物MAP2共定位在细胞体和顶端树突状干中,并且在突触素免疫反应性终末端实际上不存在。通过使用一组抗体对中间神经元进行分类,我们鉴定了含有TRPC1的GABA能中间神经元。 TRPC1缺少篮状和枝形吊灯小白蛋白(PVALB)细胞,而钙调蛋白(CALR)或钙结合蛋白(CALB)间神经元的百分比非常低,表示TRPC1。此外,生长抑素(SST)表达细胞的63%和reelin阳性细胞的37%的细胞表达TRPC1。所有SST / TRPC1双标记细胞,其中许多是推测的马蒂诺蒂细胞(MC),对reelin呈阳性。在新皮层锥体细胞的体细胞和顶端树突状干中存在TRPC1,提示该通道在感觉过程和突触可塑性中起作用。相反地​​,在SST / reelin中间神经元中,TRPC1可以调节GABA能传递,这负责塑造皮层网络中锥体细胞的协调活性。在将来的研究中,研究TRPC1是否可能参与SST抑制性中间神经元中reelin的表达或加工将是有意义的。

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