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Subunit-specific trafficking mechanisms regulating the synaptic expression of Ca2+-permeable AMPA receptors.

机译:亚单位特异的运输机制调节Ca 2+ -可渗透的AMPA受体的突触表达。

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摘要

AMPA receptors are the main excitatory neurotransmitter receptor in the brain, and hence regulating the number or properties of synaptic AMPA receptors brings about critical changes in synaptic transmission. Synaptic plasticity is thought to underlie learning and memory, and can be brought about by decreasing or increasing the number of AMPA receptors localised to synaptic sites by precisely regulating AMPA receptor trafficking. AMPA receptors are tetrameric assemblies of subunits GluA1-4, and the vast majority are GluA1/2 and GluA2/3 heteromers. The inclusion of GluA2 subunit is critical because it renders the AMPA receptor channel impermeable to Ca ions. The vast majority of synaptic AMPA receptors in the brain contain GluA2, but relatively recent discoveries indicate that an increasing number of specific forms of synaptic plasticity involve not only an alteration of the number of synaptic AMPA receptors, but also changes to their GluA2 content. The resulting change in AMPA receptor Ca permeability clearly has profound consequences for synaptic transmission and intracellular signalling events. The subunit-specific trafficking mechanisms that cause such changes represent an emerging field of research with implications for an increasing number of physiological or pathological situations, and are the topic of this review.
机译:AMPA受体是大脑中主要的兴奋性神经递质受体,因此调节突触AMPA受体的数量或特性会导致突触传递的关键变化。突触可塑性被认为是学习和记忆的基础,可以通过精确调节AMPA受体的运输来减少或增加位于突触位点的AMPA受体的数量来实现。 AMPA受体是亚基GluA1-4的四聚体组装体,绝大多数是GluA1 / 2和GluA2 / 3异聚体。包含GluA2亚基至关重要,因为它使AMPA受体通道无法渗透Ca离子。大脑中绝大多数的突触AMPA受体都含有GluA2,但是相对较新的发现表明,越来越多的特定形式的突触可塑性不仅改变了突触AMPA受体的数量,而且还改变了其GluA2的含量。 AMPA受体Ca渗透性的最终变化显然对突触传递和细胞内信号传导事件具有深远的影响。引起这种变化的特定于亚单位的贩运机制代表了一个新兴的研究领域,对越来越多的生理或病理情况具有影响,并且是本综述的主题。

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    Hanley, Jonathan;

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  • 年度 2014
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  • 原文格式 PDF
  • 正文语种 eng
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