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One aptamer two functions: the full-length aptamer inhibits AMPA receptors while the short one inhibits both AMPA and kainate receptors

机译:一种适体具有两种功能:全长适体抑制AMPA受体而一种适体抑制AMPA和红藻氨酸受体。

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摘要

AMPA and kainate receptors, along with NMDA receptors, are distinct subtypes of glutamate ion channels. Excessive activity of AMPA and kainate receptors has been implicated in neurological diseases, such as epilepsy and neuropathic pain. Antagonists that block their activities are therefore potential drug candidates. In a recent article in the Journal of Biological Chemistry by Jaremko et al. 2017, we have reported on the discovery and molecular characterization of an RNA aptamer of a dual functionality: the full-length RNA (101 nucleotide) inhibits AMPA receptors while the truncated or the short (55 nucleotide) RNA inhibits both the AMPA and kainate receptors. The full-length RNA aptamer was isolated through a specially designed, systematic evolution of ligands by exponential enrichment (SELEX) using only a single type of AMPA receptors expressed in HEK-293 cells. The design feature and the results of our recent article are highlighted here, as they demonstrate the utility of the SELEX approach and the potential of using a single AMPA receptor type to develop potent, novel RNA aptamers targeting multiple subunits and AMPA/kainate receptor subtypes with length-dependent functionalities.
机译:AMPA和海藻酸酯受体以及NMDA受体是谷氨酸离子通道的不同亚型。 AMPA和海藻酸酯受体的活性过高与神经系统疾病有关,例如癫痫和神经性疼痛。因此,阻断其活性的拮抗剂是潜在的候选药物。 Jaremko等人最近在《生物化学杂志》上发表了一篇文章。 2017年,我们报道了具有双重功能的RNA适体的发现和分子表征:全长RNA(101个核苷酸)抑制AMPA受体,而截短或短(55个核苷酸)的RNA抑制AMPA和红藻氨酸受体。全长RNA适体是通过专门设计的,系统的配体通过指数富集(SELEX)进行分离而分离的,该技术仅使用HEK-293细胞中表达的单种AMPA受体。本文重点介绍了设计功能和结果,因为它们证明了SELEX方法的实用性以及使用单个AMPA受体类型开发针对多个亚基和AMPA /红藻氨酸受体亚型的有效,新颖的RNA适体的潜力。长度相关的功能。

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