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BAPTA和EGTA对棕色脂肪细胞单通道氯离子电流的非钙离子依赖性作用

Ca(2+) -independent effects of BAPTA and EGTA on single-channel Cl(-) currents in brown adipocytes.

作者信息

Sabanov Victor, Nedergaard Jan

机构信息

The Wenner-Gren Institute, The Arrhenius Laboratories F3, Stockholm University, SE-106 91, Stockholm, Sweden.

出版信息

Biochim Biophys Acta. 2007 Nov;1768(11):2714-25. doi: 10.1016/j.bbamem.2007.07.003. Epub 2007 Jul 17.

Abstract

The Cl(-) channels of brown adipocytes electrophysiologically resemble outwardly rectifying Cl(-) channels (ORCC). To study tentative Ca(2+) regulation of these channels, we attempted to control Ca(2+) levels at the cytoplasmic side of the inside-out membrane patches with Ca(2+)-chelating agents. However, we found that the commonly used Ca(2+)-chelators EGTA and BAPTA by themselves influenced the Cl(-) channel currents, unrelated to their calcium chelating effects. Consequently, in this report we delineate effects of Ca(2+)-chelators (acting from the cytoplasmic side) on the single Cl(-) channel currents in patch-clamp experiments. Using fixed (1-2 mM) concentrations of chelators, two types of Cl(-) channels were identified, as discriminated by their reaction to the Ca(2+)-chelators and by their conductance: true-blockage channels (31 pS) and quasi-blockage channels (52 pS). In true-blockage channels, EGTA and BAPTA inhibited channel activity in a classical flickery type manner. In quasi-blockage channels, chelators significantly shortened the duration of individual openings, as in a flickering block, but the overall channel activity tended to increase. This dual effect of mean open time decrease accompanied by a tendency of open probability to increase we termed a quasi-blockage. Despite the complications due to the chelators as such, we could detect a moderate inhibitory effect of Ca(2+). The anionic classical Cl(-) channel blockers DIDS and SITS could mimic the true/quasi blockage of EGTA and BAPTA. It was concluded that at least in this experimental system, standard techniques for Ca(2+) level control in themselves could fundamentally affect the behaviour of Cl(-) channels.

摘要

棕色脂肪细胞的氯离子通道在电生理方面类似于外向整流氯离子通道(ORCC)。为了研究这些通道可能存在的钙调节作用,我们尝试用钙螯合剂来控制内翻膜片细胞质侧的钙水平。然而,我们发现常用的钙螯合剂乙二醇双四乙酸(EGTA)和1,2-双(2-氨基苯氧基)乙烷-N,N,N',N'-四乙酸(BAPTA)自身会影响氯离子通道电流,这与它们的钙螯合作用无关。因此,在本报告中,我们阐述了在膜片钳实验中钙螯合剂(从细胞质侧起作用)对单个氯离子通道电流的影响。使用固定浓度(1 - 2 mM)的螯合剂,我们鉴定出两种类型的氯离子通道,通过它们对钙螯合剂的反应及其电导来区分:真阻断通道(31 pS)和准阻断通道(52 pS)。在真阻断通道中,EGTA和BAPTA以典型的闪烁型方式抑制通道活性。在准阻断通道中,螯合剂显著缩短了单个开放的持续时间,如同闪烁阻断,但总体通道活性趋于增加。这种平均开放时间减少同时开放概率有增加趋势的双重效应,我们称之为准阻断。尽管由于螯合剂本身带来了复杂性,但我们能够检测到钙的适度抑制作用。阴离子型经典氯离子通道阻滞剂4,4'-二异硫氰酸酯-2,2'-二磺酸基联苯(DIDS)和4-乙酰胺基-4'-异硫氰酸-2,2'-二磺酸基联苯(SITS)可以模拟EGTA和BAPTA的真/准阻断作用。得出的结论是,至少在这个实验系统中,控制钙水平的标准技术本身可能会从根本上影响氯离子通道的行为。

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