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正常大鼠肾(NRK)成纤维细胞兴奋性的离子基础。

Ionic basis for excitability of normal rat kidney (NRK) fibroblasts.

作者信息

Harks E G A, Torres J J, Cornelisse L N, Ypey D L, Theuvenet A P R

机构信息

Department of Cell Biology, University of Nijmegen, Nijmegen, The Netherlands.

出版信息

J Cell Physiol. 2003 Sep;196(3):493-503. doi: 10.1002/jcp.10346.

Abstract

Ionic membrane conductances of normal rat kidney (NRK) fibroblasts were characterized by whole-cell voltage-clamp experiments on single cells and small cell clusters and their role in action potential firing in these cells and in monolayers was studied in current-clamp experiments. Activation of an L-type calcium conductance (GCaL) is responsible for the initiation of an action potential, a calcium-activated chloride conductance (GCl(Ca)) determines the plateau phase of the action potential, and an inwardly rectifying potassium conductance (GKir) is important for the generation of a resting potential of approximately -70 mV and contributes to action potential depolarization and repolarization. The unique property of the excitability mechanism is that it not only includes voltage-activated conductances (GCaL, GKir) but that the intracellular calcium dynamics is also an essential part of it (via GCl(Ca)). Excitability was found to be an intrinsic property of a fraction (approximately 25%) of the individual cells, and not necessarily dependent on gap junctional coupling of the cells in a monolayer. Electrical coupling of a patched cell to neighbor cells in a small cluster improved the excitability because all small clusters were excitable. Furthermore, cells coupled in a confluent monolayer produced broader action potentials. Thus, electrical coupling in NRK cells does not merely serve passive conduction of stereotyped action potentials, but also seems to play a role in shaping the action potential.

摘要

通过对单个细胞和小细胞簇进行全细胞膜片钳实验,对正常大鼠肾(NRK)成纤维细胞的离子膜电导进行了表征,并在电流钳实验中研究了其在这些细胞和单层细胞动作电位发放中的作用。L型钙电导(GCaL)的激活负责动作电位的起始,钙激活氯电导(GCl(Ca))决定动作电位的平台期,内向整流钾电导(GKir)对于产生约-70 mV的静息电位很重要,并有助于动作电位的去极化和复极化。兴奋机制的独特之处在于,它不仅包括电压激活电导(GCaL、GKir),而且细胞内钙动力学也是其重要组成部分(通过GCl(Ca))。研究发现,兴奋性是一部分(约25%)单个细胞的固有特性,不一定依赖于单层细胞中的间隙连接耦合。在小细胞簇中,膜片钳记录的细胞与相邻细胞之间的电耦合提高了兴奋性,因为所有小细胞簇都是可兴奋的。此外,在汇合单层中耦合的细胞产生更宽的动作电位。因此,NRK细胞中的电耦合不仅有助于定型动作电位的被动传导,而且似乎在动作电位的形成中也发挥作用。

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