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金属在行动:细胞调节中的锌离子和锌蛋白的配位动力学。

Metals on the move: zinc ions in cellular regulation and in the coordination dynamics of zinc proteins.

机构信息

King's College London, Diabetes and Nutritional Sciences Division, London, UK.

出版信息

Biometals. 2011 Jun;24(3):411-8. doi: 10.1007/s10534-010-9406-1. Epub 2011 Jan 11.

Abstract

Homeostatic control maintains essential transition metal ions at characteristic cellular concentrations to support their physiological functions and to avoid adverse effects. Zinc is especially widely used as a catalytic or structural cofactor in about 3000 human zinc proteins. In addition, the homeostatic control of zinc in eukaryotic cells permits functions of zinc(II) ions in regulation and in paracrine and intracrine signaling. Zinc ions are released from proteins through ligand-centered reactions in zinc/thiolate coordination environments, and from stores in cellular organelles, where zinc transporters participate in zinc loading and release. Muffling reactions allow zinc ions to serve as signaling ions (second messengers) in the cytosol that is buffered to picomolar zinc ion concentrations at steady-state. Muffling includes zinc ion binding to metallothioneins, cellular translocations of metallothioneins, delivery of zinc ions to transporter proteins, and zinc ion fluxes through cellular membranes with the result of removing the additional zinc ions from the cytosol and restoring the steady-state. Targets of regulatory zinc ions are proteins with sites for transient zinc binding, such as membrane receptors, enzymes, protein-protein interactions, and sensor proteins that control gene expression. The generation, transmission, targets, and termination of zinc ion signals involve proteins that use coordination dynamics in the inner and outer ligand spheres to control metal ion association and dissociation. These new findings establish critically important functions of zinc ions and zinc metalloproteins in cellular control.

摘要

体内平衡控制将必需的过渡金属离子维持在特征细胞浓度,以支持它们的生理功能并避免不良反应。锌特别广泛用作约 3000 个人类锌蛋白中的催化或结构辅助因子。此外,真核细胞中锌的体内平衡控制允许锌 (II) 离子在调节和旁分泌和内分泌信号中的功能。锌离子通过锌/硫醇配位环境中的配体中心反应从蛋白质中释放,并从细胞细胞器的储存中释放,其中锌转运蛋白参与锌的加载和释放。消音器反应允许锌离子作为细胞质中的信号离子(第二信使),在缓冲到稳定状态时的皮摩尔锌离子浓度下。消音器包括锌离子与金属硫蛋白结合、金属硫蛋白的细胞移位、锌离子递送至转运蛋白以及锌离子通过细胞膜的通量,结果是将额外的锌离子从细胞质中去除并恢复稳定状态。调节锌离子的靶标是具有瞬时锌结合位点的蛋白质,例如膜受体、酶、蛋白质-蛋白质相互作用和控制基因表达的传感器蛋白。锌离子信号的产生、传递、靶标和终止涉及使用内和外配位球中的配位动力学来控制金属离子缔合和解离的蛋白质。这些新发现确立了锌离子和锌金属蛋白在细胞控制中的至关重要的功能。

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