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氯离子与带3蛋白的阴离子转运结合位点的结合:一项³⁵Cl核磁共振研究。

Chloride binding to the anion transport binding sites of band 3. A 35Cl NMR study.

作者信息

Falke J J, Pace R J, Chan S I

出版信息

J Biol Chem. 1984 May 25;259(10):6472-80.

PMID:6725260
Abstract

Band 3 is an integral membrane protein that exchanges anions across the red cell membrane. Due to the abundance and the high turnover rate of the band 3 transport unit, the band 3 system is the most heavily used ion-transport system in a typical vertebrate organism. Here we show that 35Cl NMR enables direct and specific observation of substrate Cl- binding to band 3 transport sites, which are identified by a variety of criteria: (a) the sites are inhibited by 4,4'- dinitrostilbene -2,2'-disulfonate, which is known to inhibit competitively Cl- binding to band 3 transport sites; (b) the sites have affinities for 4,4'- dinitrostilbene -2,2'-disulfonate and Cl- that are quantitatively similar to the known affinities of band 3 transport sites for these anions; and (c) the sites have relative affinities for Cl-, HCO-3, F-, and I- that are quantitatively similar to the known relative affinities of band 3 transport sites for these anions. The 35Cl NMR assay also reveals a class of low affinity Cl- binding sites (KD much greater than 0.5 M) that are not affected by 4,4'- dinitrostilbene -2,2'-disulfonate. These low affinity sites may be responsible for the inhibition of band 3 catalyzed anion exchange that has been previously observed at high [Cl-]. In the following paper the 35Cl NMR assay is used to resolve the band 3 transport sites on opposite sides of the membrane, thereby enabling direct observation of the transmembrane recruitment of transport sites.

摘要

带3是一种整合膜蛋白,可跨红细胞膜交换阴离子。由于带3转运单元数量丰富且周转率高,带3系统是典型脊椎动物机体中使用最为频繁的离子转运系统。在此我们表明,35Cl核磁共振能够直接且特异性地观察底物Cl-与带3转运位点的结合情况,这些位点可通过多种标准来确定:(a)这些位点受到4,4'-二硝基芪-2,2'-二磺酸盐的抑制,已知该物质可竞争性抑制Cl-与带3转运位点的结合;(b)这些位点对4,4'-二硝基芪-2,2'-二磺酸盐和Cl-的亲和力在数量上与带3转运位点对这些阴离子的已知亲和力相似;(c)这些位点对Cl-、HCO-3、F-和I-的相对亲和力在数量上与带3转运位点对这些阴离子的已知相对亲和力相似。35Cl核磁共振分析还揭示了一类低亲和力的Cl-结合位点(解离常数KD远大于0.5 M),这些位点不受4,4'-二硝基芪-2,2'-二磺酸盐的影响。这些低亲和力位点可能是先前在高[Cl-]浓度下观察到的抑制带3催化阴离子交换的原因。在接下来的论文中,35Cl核磁共振分析用于解析膜两侧的带3转运位点,从而能够直接观察转运位点的跨膜募集情况。

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