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酸敏感离子通道1中的离子传导与选择性

Ion conduction and selectivity in acid-sensing ion channel 1.

作者信息

Yang Lei, Palmer Lawrence G

机构信息

Department of Physiology and Biophysics, Weill Cornell Medical College, New York, NY 10065 Department of Physiology, Harbin Medical University, Harbin 150081, China.

Department of Physiology and Biophysics, Weill Cornell Medical College, New York, NY 10065

出版信息

J Gen Physiol. 2014 Sep;144(3):245-55. doi: 10.1085/jgp.201411220. Epub 2014 Aug 11.

Abstract

The ability of acid-sensing ion channels (ASICs) to discriminate among cations was assessed based on changes in conductance and reversal potential with ion substitution. Human ASIC1a was expressed in Xenopus laevis oocytes, and acid-induced currents were measured using two-electrode voltage clamp. Replacement of extracellular Na(+) with Li(+), K(+), Rb(+), or Cs(+) altered inward conductance and shifted the reversal potentials consistent with a selectivity sequence of Li ∼ Na > K > Rb > Cs. Permeability decreased more rapidly than conductance as a function of atomic size, with P(K)/P(Na) = 0.1 and G(K)/G(Na) = 0.7 and P(Rb)/P(Na) = 0.03 and G(Rb)/G(Na) = 0.3. Stimulation of Cl(-) currents when Na(+) was replaced with Ca(2+), Sr(2+), or Ba(2+) indicated a finite permeability to divalent cations. Inward conductance increased with extracellular Na(+) in a hyperbolic manner, consistent with an apparent affinity (K(m)) for Na(+) conduction of 25 mM. Nitrogen-containing cations, including NH4(+), NH3OH(+), and guanidinium, were also permeant. In addition to passing through the channels, guanidinium blocked Na(+) currents, implying competition for a site within the pore. The role of negative charges in an external vestibule of the pore was evaluated using the point mutation D434N. The mutant channel had a decreased single-channel conductance, measured in excised outside-out patches, and a macroscopic slope conductance that increased with hyperpolarization. It had a weakened interaction with Na(+) (K(m) = 72 mM) and a selectivity that was shifted toward larger atomic sizes. We conclude that the selectivity of ASIC1 is based at least in part on interactions with binding sites both within and internal to the outer vestibule.

摘要

基于离子置换时电导和反转电位的变化,评估了酸敏感离子通道(ASICs)区分阳离子的能力。人类ASIC1a在非洲爪蟾卵母细胞中表达,并使用双电极电压钳测量酸诱导电流。用Li⁺、K⁺、Rb⁺或Cs⁺替代细胞外Na⁺会改变内向电导,并使反转电位发生偏移,这与Li ∼ Na > K > Rb > Cs的选择性序列一致。随着原子尺寸的增加,渗透率比电导下降得更快,P(K)/P(Na) = 0.1,G(K)/G(Na) = 0.7,P(Rb)/P(Na) = 0.03,G(Rb)/G(Na) = 0.3。当用Ca²⁺、Sr²⁺或Ba²⁺替代Na⁺时刺激Cl⁻电流,表明对二价阳离子有一定的渗透率。内向电导随细胞外Na⁺以双曲线方式增加,这与Na⁺传导的表观亲和力(K(m))为25 mM一致。含氮阳离子,包括NH₄⁺、NH₃OH⁺和胍盐,也是可渗透的。除了通过通道外,胍盐还会阻断Na⁺电流,这意味着在孔内存在对位点的竞争。使用点突变D434N评估了孔外部前庭中负电荷的作用。在切除的外侧向外膜片中测量,突变通道的单通道电导降低,宏观斜率电导随超极化增加。它与Na⁺的相互作用减弱(K(m) = 72 mM),选择性向更大原子尺寸偏移。我们得出结论,ASIC1的选择性至少部分基于与外部前庭内部和内部结合位点的相互作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e830/4144671/ba1401046c29/JGP_201411220_Fig1.jpg

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