首页> 美国卫生研究院文献>The Journal of Neuroscience >Cell Type-Specific Long-Term Plasticity at Glutamatergic Synapses onto Hippocampal Interneurons Expressing either Parvalbumin or CB1 Cannabinoid Receptor
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Cell Type-Specific Long-Term Plasticity at Glutamatergic Synapses onto Hippocampal Interneurons Expressing either Parvalbumin or CB1 Cannabinoid Receptor

机译:在谷氨酰胺能突触到表达小白蛋白或CB1大麻受体的海马中间神经元上的细胞类型特定的长期可塑性。

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摘要

Different GABAergic interneuron types have specific roles in hippocampal function, and anatomical as well as physiological features vary greatly between interneuron classes. Long-term plasticity of interneurons has mostly been studied in unidentified GABAergic cells and is known to be very heterogeneous. Here we tested whether cell type-specific plasticity properties in distinct GABAergic interneuron types might underlie this heterogeneity. We show that long-term potentiation (LTP) and depression (LTD), two common forms of synaptic plasticity, are expressed in a highly cell type-specific manner at glutamatergic synapses onto hippocampal GABAergic neurons. Both LTP and LTD are generated in interneurons expressing parvalbumin (PV+), whereas interneurons with similar axon distributions but expressing cannabinoid receptor-1 show no lasting plasticity in response to the same protocol. In addition, LTP or LTD occurs in PV+ interneurons with different efferent target domains. Perisomatic-targeting PV+ basket and axo-axonic interneurons express LTP, whereas glutamatergic synapses onto PV+ bistratified cells display LTD. Both LTP and LTD are pathway specific, independent of NMDA receptors, and occur at synapses with calcium-permeable (CP) AMPA receptors. Plasticity in interneurons with CP-AMPA receptors strongly modulates disynaptic GABAergic transmission onto CA1 pyramidal cells. We propose that long-term plasticity adjusts the synaptic strength between pyramidal cells and interneurons in a cell type-specific manner and, in the defined CA1 interneurons, shifts the spatial pattern of inhibitory weight from pyramidal cell dendrites to the perisomatic region.
机译:不同的GABA能型中间神经元在海马功能中具有特定作用,并且中间神经元类别之间的解剖学和生理学特征差异很大。中间神经元的长期可塑性主要在未鉴定的GABA能细胞中进行了研究,并且已知其非常异质。在这里,我们测试了在不同的GABA能中间神经元类型中特定于细胞类型的可塑性属性是否可能是这种异质性的基础。我们显示长期增强(LTP)和抑郁(LTD),两种常见形式的突触可塑性,以高度细胞类型特异性的方式在谷氨酸能突触上表达到海马GABA能神经元上。 LTP和LTD都是在表达小白蛋白(PV +)的中间神经元中产生的,而具有相似轴突分布但表达大麻素受体1的中间神经元则对同一协议没有持久的可塑性。此外,LTP或LTD发生在具有不同传出靶域的PV +中间神经元中。靶向过氧化物酶的PV +篮和轴突-轴突间神经元表达LTP,而在PV +复层细胞上的谷氨酸能突触显示LTD。 LTP和LTD都是特定于途径的,独立于NMDA受体,并与钙可渗透(CP)AMPA受体发生突触。具有CP-AMPA受体的中间神经元的可塑性强烈调节突触GABA能传递到CA1锥体细胞上。我们提出,长期可塑性以细胞类型特异性的方式调节锥体细胞和中间神经元之间的突触强度,并且在定义的CA1中间神经元中,抑制重量的空间模式从锥体细胞树突转移到周边区域。

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