Teramoto Noriyoshi
Department of Pharmacology, Graduate School of Medical Sciences, Kyushu University, Fukuoka 812-8582, Japan.
J Physiol. 2006 May 1;572(Pt 3):617-24. doi: 10.1113/jphysiol.2006.105973.
Potassium channels that are inhibited by intracellular ATP (ATP(i)) were first identified in ventricular myocytes, and are referred to as ATP-sensitive K+ channels (i.e. K(ATP) channels). Subsequently, K+ channels with similar characteristics have been demonstrated in many other tissues (pancreatic beta-cells, skeletal muscle, central neurones, smooth muscle). Approximately one decade ago, K(ATP) channels were cloned and were found to be composed of at least two subunits: an inwardly rectifying K+ channel six family (Kir6.x) that forms the ion conducting pore and a modulatory sulphonylurea receptor (SUR) that accounts for several pharmacological properties. Various types of native K(ATP) channels have been identified in a number of visceral and vascular smooth muscles in single-channel recordings. However, little attention has been paid to the molecular properties of the subunits in K(ATP) channels and it is important to determine the relative expression of K(ATP) channel components which give rise to native K(ATP) channels in smooth muscle. The aim of this review is to briefly discuss the current knowledge available for K(ATP) channels with the main interest in the molecular basis of native K(ATP) channels, and to discuss their possible linkage with physiological functions in smooth muscle.
最初在心室肌细胞中发现了受细胞内ATP(ATP(i))抑制的钾通道,它们被称为ATP敏感性钾通道(即K(ATP)通道)。随后,已在许多其他组织(胰腺β细胞、骨骼肌、中枢神经元、平滑肌)中证实了具有类似特征的钾通道。大约十年前,K(ATP)通道被克隆出来,发现其至少由两个亚基组成:形成离子传导孔的内向整流钾通道六家族(Kir6.x)和负责多种药理特性的调节性磺脲类受体(SUR)。在单通道记录中,已在多种内脏和血管平滑肌中鉴定出各种类型的天然K(ATP)通道。然而,人们对K(ATP)通道亚基的分子特性关注甚少,确定导致平滑肌中天然K(ATP)通道的K(ATP)通道组分的相对表达很重要。本综述的目的是简要讨论关于K(ATP)通道的现有知识,主要关注天然K(ATP)通道的分子基础,并讨论它们与平滑肌生理功能的可能联系。
