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Stabilization of ion selectivity filter by pore loop ion pairs in an inwardly rectifying potassium channel

机译:向内整流钾通道中的孔环离子对稳定离子选择性过滤器

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摘要

Ion selectivity is critical for the biological functions of voltage-dependent cation channels and is achieved by specific ion binding to a pore region called the selectivity filter. In voltage-gated K+, Na+ and Ca2+ channels, the selectivity filter is formed by a short polypeptide loop (called the H5 or P region) between the fifth and sixth transmembrane segments, donated by each of the four subunits or internal homologous domains forming the channel. While mutagenesis studies on voltage-gated K+ channels have begun to shed light on the structural organization of this pore region, little is known about the physical and chemical interactions that maintain the structural stability of the selectivity filter. Here we show that in an inwardly rectifying K+ (IRK) channel, IRK1, short range interactions of an ion pair in the H5 pore loop are crucial for pore structure and ion permeation. The two residues, a glutamate and an arginine, appear to form exposed salt bridges in the tetrameric channel. Alteration or disruption of such ion pair interactions dramatically alters ion selectivity and permeation. Since this ion pair is conserved in all IRK channels, it may constitute a general mechanism for maintaining the stability of the pore structure in this channel superfamily.
机译:离子选择性对于依赖电压的阳离子通道的生物学功能至关重要,它是通过将特定的离子与称为选择性过滤器的孔区域结合而实现的。在电压门控的K + ,Na + 和Ca 2 + 通道中,选择性过滤器由一个短的多肽环形成(称为H5第五和第六个跨膜片段之间的“ P”或“ P”区域),由形成通道的四个亚基或内部同源域中的每一个提供。尽管对电压门控K + 通道的诱变研究开始阐明该孔区域的结构组织,但对维持选择性滤膜结构稳定性的物理和化学相互作用了解甚少。在这里我们表明,在向内整流的K + (IRK)通道IRK1中,H5孔环中离子对的短程相互作用对于孔结构和离子渗透至关重要。谷氨酸和精氨酸这两个残基似乎在四聚体通道中形成暴露的盐桥。这种离子对相互作用的改变或破坏极大地改变了离子的选择性和渗透性。由于该离子对在所有IRK通道中均是保守的,因此它可以构成维持该通道超族中孔结构稳定性的一般机制。

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