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Modulation of synaptic signalling complexes by Homer proteins.

机译:荷马蛋白对突触信号复合物的调节。

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摘要

The number of neurotransmitter receptors in the postsynaptic membrane and their functional coupling to intracellular signalling cascades are important determinants of synaptic strength - and hence potential targets for plasticity related modulation. In this context, Homer/Vesl proteins have gained particular interest for three main reasons: (i) they constitute part of the molecular scaffold at postsynaptic densities of excitatory synapses in the mammalian brain; (ii) they physically link type-I metabotropic glutamate receptors to the postsynaptic density and to inositol 1,4,5-triphosphate receptors in the subsynaptic endoplasmic reticulum; and (iii) Homer-1a, which has been categorized as an immediate early gene isoform, exerts dominant-negative activity, suggesting that it is involved in activity dependent rearrangements at synaptic junctions. Although these fundamental aspects have been reviewed previously by Xiao et al., this review will address primarily more recent studies on the regulation of Homer 1a expression and on the role of Homer/Vesl proteins in spine morphogenesis and receptor targeting and signalling.
机译:突触后膜中神经递质受体的数量及其与细胞内信号传导级联的功能偶联是突触强度的重要决定因素-因此是可塑性相关调节的潜在目标。在这种情况下,荷马/ Vesl蛋白由于三个主要原因而引起了人们的特别关注:(i)它们在哺乳动物脑中的兴奋性突触的突触后密度处构成分子支架的一部分; (ii)它们将I型代谢型谷氨酸受体与突触后内质网中的突触后密度和肌醇1,4,5-三磷酸受体物理联系起来; (iii)Homer-1a已被归类为立即早期基因同工型,发挥显性负活性,表明它参与了突触连接处的活性依赖性重排。尽管这些基本方面先前已由Xiao等人进行过综述,但本综述将主要解决有关Homer 1a表达调控以及Homer / Vesl蛋白在脊柱形态发生,受体靶向和信号传导中的作用的最新研究。

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