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V-ATPases 的调节与同工型功能。

Regulation and isoform function of the V-ATPases.

机构信息

Department of Physiology, Tufts University School of Medicine, Boston, Massachusetts 02111, USA.

出版信息

Biochemistry. 2010 Jun 15;49(23):4715-23. doi: 10.1021/bi100397s.

Abstract

The vacuolar (H(+))-ATPases are ATP-dependent proton pumps that acidify intracellular compartments and, in some cases, transport protons across the plasma membrane of eukaryotic cells. Intracellular V-ATPases play an important role in normal physiological processes such as receptor-mediated endocytosis, intracellular membrane trafficking, pro-hormone processing, protein degradation, and the coupled uptake of small molecules, such as neurotransmitters. They also function in the entry of various pathogenic agents, including many envelope viruses, like influenza virus, and toxins, like anthrax toxin. Plasma membrane V-ATPases function in renal pH homeostasis, bone resorption and sperm maturation, and various disease processes, including renal tubular acidosis, osteopetrosis, and tumor metastasis. V-ATPases are composed of a peripheral V(1) domain containing eight different subunits that is responsible for ATP hydrolysis and an integral V(0) domain containing six different subunits that translocates protons. In mammalian cells, most of the V-ATPase subunits exist in multiple isoforms which are often expressed in a tissue specific manner. Isoforms of one of the V(0) subunits (subunit a) have been shown to possess information that targets the V-ATPase to distinct cellular destinations. Mutations in isoforms of subunit a lead to the human diseases osteopetrosis and renal tubular acidosis. A number of mechanisms are employed to regulate V-ATPase activity in vivo, including reversible dissociation of the V(1) and V(0) domains, control of the tightness of coupling of proton transport and ATP hydrolysis, and selective targeting of V-ATPases to distinct cellular membranes. Isoforms of subunit a are involved in regulation both via the control of coupling and via selective targeting. This review will begin with a brief introduction to the function, structure, and mechanism of the V-ATPases followed by a discussion of the role of V-ATPase subunit isoforms and the mechanisms involved in regulation of V-ATPase activity.

摘要

液泡(H(+))-ATP 酶是一种依赖于 ATP 的质子泵,可使细胞内隔室酸化,在某些情况下,还可将质子跨真核细胞的质膜转运。细胞内 V-ATP 酶在正常生理过程中发挥着重要作用,如受体介导的内吞作用、细胞内膜运输、前激素加工、蛋白质降解以及小分子(如神经递质)的偶联摄取。它们还参与各种病原体的进入,包括许多包膜病毒,如流感病毒,以及毒素,如炭疽毒素。质膜 V-ATP 酶在肾 pH 稳态、骨吸收和精子成熟以及包括肾小管酸中毒、骨质增生症和肿瘤转移在内的各种疾病过程中发挥作用。V-ATP 酶由负责 ATP 水解的含有八个不同亚基的外周 V(1)结构域和含有六个不同亚基的整合 V(0)结构域组成,该结构域可转运质子。在哺乳动物细胞中,大多数 V-ATP 酶亚基存在于多种同工型中,这些同工型通常以组织特异性方式表达。一种 V(0)亚基(亚基 a)的同工型已被证明具有将 V-ATP 酶靶向特定细胞靶标的信息。亚基 a 的同工型突变导致人类疾病骨质增生症和肾小管酸中毒。许多机制被用来在体内调节 V-ATP 酶活性,包括 V(1)和 V(0)结构域的可逆解离、质子转运和 ATP 水解偶联的紧密性控制以及 V-ATP 酶对不同细胞膜的选择性靶向。亚基 a 的同工型通过控制偶联和选择性靶向来参与调节。这篇综述将首先简要介绍 V-ATP 酶的功能、结构和机制,然后讨论 V-ATP 酶亚基同工型的作用以及调节 V-ATP 酶活性的机制。

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