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Understanding the Molecular Diversity of GABAergic Synapses

机译:了解GABA能突触的分子多样性

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摘要

GABAergic synapses exhibit a high degree of subcellular and molecular specialization, which contrasts with their apparent simplicity in ultrastructural appearance. Indeed, when observed in the electron microscope, GABAergic synapses fit in the symmetric, or Gray’s type II category, being characterized by a relatively simple postsynaptic specialization. The inhibitory postsynaptic density cannot be readily isolated, and progress in understanding its molecular composition has lagged behind that of excitatory synapses. However, recent studies have brought significant progress in the identification of new synaptic proteins, revealing an unexpected complexity in the molecular machinery that regulates GABAergic synaptogenesis. In this article, we provide an overview of the molecular diversity of GABAergic synapses, and we consider how synapse specificity may be encoded by selective trans-synaptic interactions between pre- and postsynaptic adhesion molecules and secreted factors that reside in the synaptic cleft. We also discuss the importance of developing cataloguing tools that could be used to decipher the molecular diversity of synapses and to predict alterations of inhibitory transmission in the course of neurological diseases.
机译:GABA能突触表现出高度的亚细胞和分子特化,这与它们在超微结构外观上的明显简单形成鲜明对比。实际上,当在电子显微镜下观察时,GABA能突触适合对称的或格雷的II型类别,其特征是相对简单的突触后专业化。抑制性突触后密度不能容易地分离,并且在了解其分子组成方面的进展已经落后于兴奋性突触。但是,最近的研究在鉴定新的突触蛋白方面取得了重大进展,揭示了调节GABA能突触发生的分子机制中意想不到的复杂性。在本文中,我们概述了GABA能突触的分子多样性,并考虑了突触前和突触后黏附分子与​​驻留在突触间隙中的分泌因子之间的选择性反突触相互作用如何编码突触特异性。我们还讨论了开发分类工具的重要性,该工具可用于破译突触的分子多样性并预测神经疾病过程中抑制性传递的变化。

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