首页> 外文期刊>The Journal of Physiology >Redefining the classification of AMPA-selective ionotropic glutamate receptors.
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Redefining the classification of AMPA-selective ionotropic glutamate receptors.

机译:重新定义AMPA选择性离子型谷氨酸受体的分类。

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AMPA-type ionotropic glutamate receptors (iGluRs) represent the major excitatory neurotransmitter receptor in the developing and adult vertebrate CNS. They are crucial for the normal hardwiring of glutamatergic circuits but also fine tune synaptic strength by cycling into and out of synapses during periods of sustained patterned activity or altered homeostasis. AMPARs are grouped into two functionally distinct tetrameric assemblies based on the inclusion or exclusion of the GluA2 receptor subunit. GluA2-containing receptors are thought to be the most abundant AMPAR in the CNS, typified by their small unitary events, Ca(2+) impermeability and insensitivity to polyamine block. In contrast, GluA2-lacking AMPARs exhibit large unitary conductance, marked divalent permeability and nano- to micromolar polyamine affinity. Here, I review evidence for the existence of a third class of AMPAR which, though similarly Ca(2+) permeable, is characterized by its near-insensitivity to internal and external channel block by polyamines. This novel class of AMPAR is most notably found at multivesicular release synapses found in the avian auditory brainstem and mammalian retina. Curiously, these synapses lack NMDA-type iGluRs, which are conventionally associated with controlling AMPAR insertion. The lack of NMDARs suggests that a different set of rules may govern AMPAR cycling at these synapses. AMPARs with similar functional profiles are also found on some glial cells suggesting they may have a more widespread distribution in the mammalian CNS. I conclude by noting that modest changes to the ion-permeation pathway might be sufficient to retain divalent permeability whilst eliminating polyamine sensitivity. Consequently, this emerging AMPAR subclass need not be assembled from novel subunits, yet to be cloned, but could simply occur by varying the stoichiometry of existing proteins.
机译:AMPA型离子型谷氨酸受体(iGluRs)代表了发育中和成年脊椎动物CNS中的主要兴奋性神经递质受体。它们对于正常的谷氨酸能回路的硬接线至关重要,但在持续的模式活动或动态平衡期间,通过循环进入和退出突触来微调突触强度。根据包含或排除的GluA2受体亚基,将AMPAR分为两个功能不同的四聚体组件。含GluA2的受体被认为是中枢神经系统中最丰富的AMPAR,以其较小的单一事件,Ca(2+)不可渗透性和对多胺嵌段的不敏感性为代表。相反,缺少GluA2的AMPAR表现出大的单位电导率,明显的二价渗透性和纳摩尔至微摩尔的多胺亲和力。在这里,我回顾了存在第三类AMPAR的证据,该类虽然具有类似的Ca(2+)渗透性,但其特征是它对多胺对内部和外部通道阻滞几乎不敏感。这种新型的AMPAR最明显地发现于鸟类听觉脑干和哺乳动物视网膜中的多泡释放突触中。奇怪的是,这些突触缺乏NMDA型iGluR,而这些通常与控制AMPAR插入有关。 NMDAR的缺乏表明在这些突触处可能有不同的规则集可以控制AMPAR循环。在一些神经胶质细胞上也发现了具有相似功能特征的AMPAR,这表明它们在哺乳动物的CNS中可能分布更为广泛。我的结论是,对离子渗透途径的适度变化可能足以保留二价渗透性,同时消除了多胺敏感性。因此,这种新兴的AMPAR亚类无需从新的亚基组装而得到克隆,而可以通过改变现有蛋白质的化学计量简单地发生。

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