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液泡(H⁺)-ATP酶的结构、功能及调控

Structure, function and regulation of the vacuolar (H+)-ATPases.

作者信息

Forgac M

机构信息

Department of Cellular and Molecular Physiology, Tufts University School of Medicine, Boston, MA 02111, USA.

出版信息

FEBS Lett. 1998 Dec 4;440(3):258-63. doi: 10.1016/s0014-5793(98)01425-2.

DOI:10.1016/s0014-5793(98)01425-2
PMID:9872382
Abstract

The vacuolar (H+)-ATPases (or V-ATPases) function to acidify intracellular compartments in eukaryotic cells, playing an important role in such processes as receptor-mediated endocytosis, intracellular membrane traffic, protein degradation and coupled transport. V-ATPases in the plasma membrane of specialized cells also function in renal acidification, bone resorption and cytosolic pH maintenance. The V-ATPases are composed of two domains. The V1 domain is a 570-kDa peripheral complex composed of 8 subunits (subunits A-H) of molecular weight 70-13 kDa which is responsible for ATP hydrolysis. The V0 domain is a 260-kDa integral complex composed of 5 subunits (subunits a-d) which is responsible for proton translocation. The V-ATPases are structurally related to the F-ATPases which function in ATP synthesis. Biochemical and mutational studies have begun to reveal the function of individual subunits and residues in V-ATPase activity. A central question in this field is the mechanism of regulation of vacuolar acidification in vivo. Evidence has been obtained suggesting a number of possible mechanisms of regulating V-ATPase activity, including reversible dissociation of V1 and V0 domains, disulfide bond formation at the catalytic site and differential targeting of V-ATPases. Control of anion conductance may also function to regulate vacuolar pH. Because of the diversity of functions of V-ATPases, cells most likely employ multiple mechanisms for controlling their activity.

摘要

液泡型(H⁺)-ATP酶(即V-ATP酶)的功能是酸化真核细胞内的区室,在受体介导的内吞作用、细胞内膜运输、蛋白质降解和偶联转运等过程中发挥重要作用。特化细胞质膜中的V-ATP酶在肾脏酸化、骨吸收和胞质pH维持中也发挥作用。V-ATP酶由两个结构域组成。V1结构域是一个570 kDa的外周复合物,由分子量为70 - 13 kDa的8个亚基(亚基A - H)组成,负责ATP水解。V0结构域是一个260 kDa的整合复合物,由5个亚基(亚基a - d)组成,负责质子转运。V-ATP酶在结构上与参与ATP合成的F-ATP酶相关。生化和突变研究已开始揭示V-ATP酶活性中各个亚基和残基的功能。该领域的一个核心问题是体内液泡酸化的调节机制。已获得的证据表明存在多种调节V-ATP酶活性的可能机制,包括V1和V0结构域的可逆解离、催化位点二硫键的形成以及V-ATP酶的差异靶向。阴离子电导的控制也可能在调节液泡pH中起作用。由于V-ATP酶功能的多样性,细胞很可能采用多种机制来控制其活性。

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