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将Shaker B钾通道单侧暴露于高渗溶液中。

Unilateral exposure of Shaker B potassium channels to hyperosmolar solutions.

作者信息

Starkus J G, Schlief T, Rayner M D, Heinemann S H

机构信息

Békésy Laboratory of Neurobiology, University of Hawaii, Honolulu 96822-2359, USA.

出版信息

Biophys J. 1995 Sep;69(3):860-72. doi: 10.1016/S0006-3495(95)79960-X.

Abstract

This study tests the hypothesis that ion channels will be affected differently by external (extracellular) versus internal (cytoplasmic) exposure to hyperosmolar media. We looked first for effects on inactivation kinetics in wild-type Shaker B potassium channels. Although external hyperosmolar exposure did not alter the inactivation rate, internal exposure slowed both onset and recovery from fast inactivation. Differential effects on activation kinetics were then characterized by using a noninactivating Shaker B mutant. External hyperosmolar exposure slowed the late rising phase of macroscopic current without affecting the initial delay or early rising phase kinetics. By contrast, internal exposure slowed the initial steps in channel activation with only minimal changes in the later part of the rising phase. Neither external nor internal hyperosmolar exposure affected tail current rates in these noninactivating channels. Additionally, suppression of peak macroscopic current was approximately twofold smaller during external, as compared with internal, hyperosmolar exposure. Single-channel currents, observed under identical experimental conditions, showed a differential suppression equivalent to that seen in macroscopic currents. Apparently, during unilateral hyperosmolar exposure, changes in macroscopic peak current arise primarily from changes in single-channel conductance rather than from changes in equilibrium channel gating. We conclude that unilateral hyperosmolar exposure can provide information concerning the potential structural localization of functional components within ion-channel molecules.

摘要

本研究检验了以下假设

离子通道在细胞外与细胞内暴露于高渗介质时会受到不同影响。我们首先研究了野生型Shaker B钾通道失活动力学的影响。尽管细胞外高渗暴露并未改变失活速率,但细胞内暴露减缓了快速失活的起始和恢复。然后,通过使用非失活的Shaker B突变体来表征对激活动力学的差异影响。细胞外高渗暴露减缓了宏观电流的后期上升阶段,而不影响初始延迟或早期上升阶段的动力学。相比之下,细胞内暴露减缓了通道激活的初始步骤,而上升阶段后期仅有微小变化。细胞外和细胞内高渗暴露均未影响这些非失活通道的尾电流速率。此外,与细胞内高渗暴露相比,细胞外高渗暴露期间宏观电流峰值的抑制约小两倍。在相同实验条件下观察到的单通道电流显示出与宏观电流中所见相当的差异抑制。显然,在单侧高渗暴露期间,宏观峰值电流的变化主要源于单通道电导的变化,而非平衡通道门控的变化。我们得出结论,单侧高渗暴露可以提供有关离子通道分子内功能成分潜在结构定位的信息。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4ef3/1236315/28fda766aea5/biophysj00057-0133-a.jpg

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