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首页> 外文期刊>Frontiers in Cellular Neuroscience >GABA BR-Dependent Long-Term Depression at Hippocampal Synapses between CB1-Positive Interneurons and CA1 Pyramidal Cells
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GABA BR-Dependent Long-Term Depression at Hippocampal Synapses between CB1-Positive Interneurons and CA1 Pyramidal Cells

机译:CABA阳性中间神经元和CA1锥体细胞之间海马突触的GABA B R依赖性长期抑制

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Activity induced long lasting modifications of synaptic efficacy have been extensively studied in excitatory synapses, however, long term plasticity is also a property of inhibitory synapses. Inhibitory neurons in the hippocampal CA1 region can be subdivided according to the compartment they target on the pyramidal cell. Some interneurons preferentially innervate the perisomatic area and axon hillock of the pyramidal cells while others preferentially target dendritic branches and spines. Another characteristic feature allowing functional classification of interneurons is cell type specific expression of different neurochemical markers and receptors. In the hippocampal CA1 region, nearly 90% of the interneurons expressing cannabinoid type 1 receptors (CB1R) also express cholecystokinin (CCK). Therefore, the functional presence of CB1 receptors can be used for identification of the inhibitory input from CCK positive (CCK+) interneurons to CA1 pyramidal cells. The goal of this study was to explore the nature of long term plasticity at the synapses between interneurons expressing CB1Rs (putative CCK+) and pyramidal neurons in the CA1 region of the hippocampus in vitro . We found that theta burst stimulation triggered robust long-term depression (LTD) at this synapse. The locus of LTD induction was postsynaptic and required activation of GABA_(B)receptors. We also showed that LTD at this synaptic connection involves GABA_(B)R-dependent suppression of adenylyl cyclase and consequent reduction of PKA activity. In this respect, CB1+ to pyramidal cell synapses differ from the majority of the other hippocampal inhibitory connections where theta burst stimulation results in long-term potentiation.
机译:在兴奋性突触中已经广泛研究了活性诱导的突触功效的持久修饰,但是,长期可塑性也是抑制性突触的特性。海马CA1区的抑制性神经元可以根据它们靶向锥体细胞的区室进行细分。一些中间神经优先支配锥体细胞的周边区域和轴突岗,而其他一些优先支配树突分支和棘突。允许中间神经元功能分类的另一个特征是不同神经化学标记和受体的细胞类型特异性表达。在海马CA1区,表达大麻素1型受体(CB1R)的近中神经元也表达胆囊收缩素(CCK)。因此,CB1受体的功能存在可用于鉴定从CCK阳性(CCK +)内部神经元到CA1锥体细胞的抑制性输入。这项研究的目的是探索海马CA1区表达CB1Rs(假定为CCK +)的中神经与锥体神经元突触之间长期可塑性的性质。我们发现,theta突触刺激在该突触处触发了稳健的长期抑郁(LTD)。 LTD诱导的位点是突触后,需要激活GABA_(B)受体。我们还表明,LTD在此突触连接涉及GABA_(B)R依赖的腺苷酸环化酶抑制和随之而来的PKA活性降低。在这方面,CB1 +到锥体细胞突触不同于大多数其他海马抑制连接,在这些连接中,theta爆裂刺激导致长期增强。

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