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Neuroendocrinology: programming the projections.

机译:神经内分泌学:对预测进行编程。

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The neurotransmitters GABA and glycine mediate fast synaptic inhibition by activating ligand-gated chloride channels--namely, type A GABA (GABA(A)) and glycine receptors. Both types of receptors are anchored postsynaptically by gephyrin, which self-assembles into a scaffold and interacts with the cytoskeleton. Current research indicates that postsynaptic gephyrin clusters are dynamic assemblies that are held together and regulated by multiple protein-protein interactions. Moreover, post-translational modifications of gephyrin regulate the formation and plasticity of GABAergic synapses by altering the clustering properties of postsynaptic scaffolds and thereby the availability and function of receptors and other signalling molecules. Here, we discuss the formation and regulation of the gephyrin scaffold, its role in GABAergic and glycinergic synaptic function and the implications for the pathophysiology of brain disorders caused by abnormal inhibitory neurotransmission.
机译:神经递质GABA和甘氨酸通过激活配体门控的氯离子通道(即A型GABA(GABA(A))和甘氨酸受体)介导快速的突触抑制。两种类型的受体都由gephyrin突触地锚定,gephyrin自组装成支架并与细胞骨架相互作用。当前的研究表明,突触后的gephyrin簇是动态的程序集,由多个蛋白质-蛋白质相互作用保持在一起并受其调控。此外,通过改变突触后支架的聚集特性,进而改变受体和其他信号分子的可用性和功能,gephyrin的翻译后修饰调节了GABA能突触的形成和可塑性。在这里,我们讨论了gephyrin支架的形成和调控,其在GABA能和甘氨酸能突触功能中的作用以及异常抑制性神经传递引起的脑部疾病的病理生理学意义。

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