内源性哇巴因样物质对钠钾ATP酶的调节作用。

Regulation of Na,K-ATPase by endogenous ouabain-like materials.

作者信息

Doris P A

机构信息

Department of Cell Biology and Anatomy, Texas Tech University Health Sciences Center, Lubbock 79430.

出版信息

Proc Soc Exp Biol Med. 1994 Mar;205(3):202-12. doi: 10.3181/00379727-205-43699.

Abstract

Sodium, potassium-ATPase (NKA) is an essential energy transduction mechanism in which the free energy released by hydrolysis of ATP is transferred to an electrochemical gradient across the cell membrane. The asymmetry of sodium in this gradient is coupled to membrane transport mechanisms which affect transmembrane movement of a range of solutes and electrolytes. Recent advances in the molecular biology of NKA have revealed important new aspects of structure-function relationships as well as illuminating the basis for variations in cardiac glycoside sensitivity of the enzyme. The search for endogenous mammalian counterparts of the cardiac glycosides, which regulate the activity of the enzyme by interacting from the extracellular surface at this receptor site, has moved ahead dramatically with evidence that ouabain is an endogenous product of the mammalian adrenal cortex. These advances, and problems raised by them, are explored in this review.

摘要

钠钾 -ATP酶(NKA)是一种重要的能量转换机制,其中ATP水解释放的自由能被转移到跨细胞膜的电化学梯度上。该梯度中钠的不对称性与膜转运机制相关联,这些机制影响一系列溶质和电解质的跨膜运动。NKA分子生物学的最新进展揭示了结构 - 功能关系的重要新方面,并阐明了该酶对强心苷敏感性变化的基础。寻找强心苷的内源性哺乳动物对应物(通过在该受体位点从细胞外表面相互作用来调节酶的活性)取得了重大进展,有证据表明哇巴因是哺乳动物肾上腺皮质的内源性产物。本综述探讨了这些进展及其引发的问题。

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