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底物结合力在仅交换运输系统中的作用:II. 对红细胞阴离子交换机制的启示。

Role of substrate binding forces in exchange-only transport systems: II. Implications for the mechanism of the anion exchanger of red cells.

作者信息

Krupka R M

机构信息

Agriculture Canada, Research Centre, London, Ontario.

出版信息

J Membr Biol. 1989 Jul;109(2):159-71. doi: 10.1007/BF01870855.

Abstract

The transition-state theory of exchange-only membrane transport is applied to experimental results in the literature on the anion exchanger of red cells. Two central features of the system are in accord with the theory: (i) forming the transition state in translocation involves a carrier conformational change; (ii) substrate specificity is expressed in transport rates rather than affinities. The expression of specificity is consistent with other evidence for a conformational intermediate (not the transition state) formed in the translocation of all substrates. The theory, in conjunction with concepts derived from the chemistry of macrocyclic ion inclusion complexes, prescribes certain essential properties in the transport site. Separate subsites are required for the preferred substrates, Cl- and HCO3-, to account for tight binding in the transition state (Kdiss congruent to 1 microM). Further, the following mechanism is suggested. A substrate anion initially forms a loose surface complex at one subsite, but in the transition state the subsites converge to form an inclusion complex in which the binding forces are greatly increased through a chelation effect. The conformational change at the substrate site, which is driven by the mounting forces of binding, sets in train a wider conformational change that converts the carrier from an immobile to a mobile form. Though simple, this composite-site mechanism explains many unusual features of the system. It accounts for substrate inhibition, partially noncompetitive inhibition of one substrate by another, and "tunneling," which is net transport under conditions where exchange should prevail, according to other models. All three types of behavior result from the formation of a ternary complex in which substrate anions are bound at both subsites. The mechanism also accounts for the enormous range of substrate structures accepted by the system, for the complex inhibition by the organic sulfate NAP-taurine, and for the involvement of several cationic side chains and two different protein domains in the transport site.

摘要

仅交换膜运输的过渡态理论被应用于文献中关于红细胞阴离子交换器的实验结果。该系统的两个核心特征与该理论相符:(i)转运过程中形成过渡态涉及载体构象变化;(ii)底物特异性通过转运速率而非亲和力来体现。特异性的这种表现与其他证据一致,即在所有底物的转运过程中形成了构象中间体(而非过渡态)。该理论结合从大环离子包合配合物化学衍生出的概念,规定了转运位点的某些基本性质。对于优先底物Cl-和HCO3-,需要单独的亚位点来解释过渡态中的紧密结合(解离常数约为1 microM)。此外,提出了以下机制。底物阴离子最初在一个亚位点形成松散的表面复合物,但在过渡态时,亚位点会合形成包合配合物,其中结合力通过螯合效应大大增强。由不断增加的结合力驱动的底物位点的构象变化引发了更广泛的构象变化,将载体从固定形式转变为可移动形式。尽管简单,但这种复合位点机制解释了该系统的许多不寻常特征。它解释了底物抑制、一种底物对另一种底物的部分非竞争性抑制以及“隧道效应”,根据其他模型,“隧道效应”是指在交换应占主导的条件下的净转运。所有这三种行为都是由三元复合物的形成导致的,其中底物阴离子在两个亚位点都有结合。该机制还解释了该系统所接受的底物结构的巨大范围、有机硫酸盐NAP-牛磺酸的复杂抑制作用以及转运位点中几个阳离子侧链和两个不同蛋白质结构域的参与。

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