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锌-配体相互作用调节胰岛素六聚体的组装与稳定性——综述

Zinc-ligand interactions modulate assembly and stability of the insulin hexamer -- a review.

作者信息

Dunn Michael F

机构信息

Department of Biochemistry, University of California, Riverside, CA 92521, USA.

出版信息

Biometals. 2005 Aug;18(4):295-303. doi: 10.1007/s10534-005-3685-y.

Abstract

Zinc and calcium ions play important roles in the biosynthesis and storage of insulin. Insulin biosynthesis occurs within the beta-cells of the pancreas via preproinsulin and proinsulin precursors. In the golgi apparatus, proinsulin is sequestered within Zn(2+)- and Ca(2+)-rich storage/secretory vesicles and assembled into a Zn(2+) and Ca(2+) containing hexameric species, (Zn(2+))(2)(Ca(2+))(Proin)(6). In the vesicle, (Zn(2+))(2)(Ca(2+))(Proin)(6) is converted to the insulin hexamer, (Zn(2+))(2)(Ca(2+))(In)(6), by excision of the C-peptide through the action of proteolytic enzymes. The conversion of (Zn(2+))(2)(Ca(2+))(Proin)(6)to (Zn(2+))(2)(Ca(2+))(In)(6) significantly lowers the solubility of the hexamer, causing crystallization within the vesicle. The (Zn(2+))(2)(Ca(2+))(In)(6) hexamer is an allosteric protein that undergoes ligand-mediated interconversion among three global conformation states designated T(6), T(3)R(3) and R(6). Two classes of allosteric sites have been identified; hydrophobic pockets (3 in T(3)R(3) and 6 in R(6)) that bind phenolic ligands, and anion sites (1 in T(3)R(3) and 2 in R(6)) that bind monovalent anions. The allosteric states differ widely with respect to the physical and chemical stability of the insulin subunits. Fusion of the vesicle with the plasma membrane results in the expulsion of the insulin crystals into the intercellular fluid. Dissolution of the crystals, dissociation of the hexamers to monomer and transport of monomers to the liver and other tissues then occurs via the blood stream. Insulin action then follows binding to the insulin receptors. The role of Zn(2+) in the assembly, structure, allosteric properties, and dynamic behavior of the insulin hexamer will be discussed in relation to biological function.

摘要

锌离子和钙离子在胰岛素的生物合成及储存过程中发挥着重要作用。胰岛素的生物合成通过胰岛素原和胰岛素前体在胰腺的β细胞内进行。在高尔基体中,胰岛素原被隔离在富含锌离子(Zn(2+))和钙离子(Ca(2+))的储存/分泌囊泡内,并组装成含有锌离子和钙离子的六聚体物种,即(Zn(2+))(2)(Ca(2+))(Proin)(6)。在囊泡中,通过蛋白水解酶的作用切除C肽,(Zn(2+))(2)(Ca(2+))(Proin)(6)转变为胰岛素六聚体(Zn(2+))(2)(Ca(2+))(In)(6)。(Zn(2+))(2)(Ca(2+))(Proin)(6)向(Zn(2+))(2)(Ca(2+))(In)(6)的转变显著降低了六聚体的溶解度,导致其在囊泡内结晶。(Zn(2+))(2)(Ca(2+))(In)(6)六聚体是一种变构蛋白,在三种全局构象状态(分别称为T(6)、T(3)R(3)和R(6))之间经历配体介导的相互转化。已鉴定出两类变构位点:结合酚类配体的疏水口袋(T(3)R(3)中有3个,R(6)中有6个)和结合单价阴离子的阴离子位点(T(3)R(3)中有1个,R(6)中有2个)。这些变构状态在胰岛素亚基的物理和化学稳定性方面有很大差异。囊泡与质膜融合导致胰岛素晶体被排出到细胞间液中。然后晶体溶解,六聚体解离为单体,并通过血流将单体运输到肝脏和其他组织。胰岛素与胰岛素受体结合后发挥作用。锌离子(Zn(2+))在胰岛素六聚体的组装、结构、变构性质和动态行为方面的作用将结合生物学功能进行讨论。

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