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脊椎动物红细胞中的容积敏感转运系统与容积稳态

Volume-sensitive transport systems and volume homeostasis in vertebrate red blood cells.

作者信息

Cossins A R, Gibson J S

机构信息

Integrative Physiology Research Group, School of Biological Science, University of Liverpool, UK.

出版信息

J Exp Biol. 1997 Jan;200(Pt 2):343-52. doi: 10.1242/jeb.200.2.343.

Abstract

Animal cells regulate their volume in the short term by controlling solute movements into and out of the cell. A quite of dissipative transport systems are involved which allow either regulatory volume increase (RVI) or decrease (RVD) responses depending upon the direction of the electrochemical gradients of the solutes. Many of these transporters have been identified at the molecular level and structure-function studies have identified transmembrane transport domains and cytoplasmic regulatory domains. In vertebrate red blood cells, protein phosphorylation appears to be central to the coordinated regulation of transporter activity. Inhibitors of protein phosphatases (PPs) cause inhibition of the K+/Cl- cotransporter (a transporter mediating RVD), whilst some inhibitors of protein kinases (PKs) cause activation. A sequence of potential phosphorylation sites appears to constitute a cascade of reactions leading to transporter regulation. PP and PK inhibitors have opposite effects on transporters mediating RVI responses, which is consistent with the coordinated but reciprocal regulation of transporters activated during both RVI and RVD using some common phosphorylation reactions. The transporters are sensitive to other stimuli including, in red blood cells, changes in PO2 and pH. These responses are also sensitive to PK/PP inhibitors and may involve elements of the volume-sensitive transduction pathway.

摘要

动物细胞通过控制溶质进出细胞来在短期内调节其体积。涉及多种耗散性运输系统,这些系统根据溶质电化学梯度的方向实现调节性体积增加(RVI)或减少(RVD)反应。其中许多转运蛋白已在分子水平上得到鉴定,结构 - 功能研究也已确定了跨膜运输结构域和细胞质调节结构域。在脊椎动物红细胞中,蛋白质磷酸化似乎是转运蛋白活性协同调节的核心。蛋白磷酸酶(PP)抑制剂会抑制K⁺/Cl⁻共转运蛋白(一种介导RVD的转运蛋白),而一些蛋白激酶(PK)抑制剂则会导致其激活。一系列潜在的磷酸化位点似乎构成了导致转运蛋白调节的反应级联。PP和PK抑制剂对介导RVI反应的转运蛋白有相反的作用,这与在RVI和RVD过程中使用一些常见磷酸化反应对转运蛋白进行协同但相互调节是一致的。这些转运蛋白对其他刺激敏感,包括在红细胞中对PO₂和pH的变化。这些反应也对PK/PP抑制剂敏感,并且可能涉及体积敏感转导途径的元件。

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