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豚鼠心室肌细胞中氯-羟基交换的测量与建模

Measuring and modeling chloride-hydroxyl exchange in the Guinea-pig ventricular myocyte.

作者信息

Niederer S A, Swietach P, Wilson D A, Smith N P, Vaughan-Jones R D

机构信息

Burdon Sanderson Cardiac Science Centre, Department of Physiology, Anatomy and Genetics,University of Oxford, Oxford, United Kingdom.

出版信息

Biophys J. 2008 Mar 15;94(6):2385-403. doi: 10.1529/biophysj.107.118885. Epub 2007 Nov 30.

Abstract

Protons are powerful modulators of cardiac function. Their intracellular concentration is regulated by sarcolemmal ion transporters that export or import H+-ions (or their ionic equivalent: HCO3-, OH-). One such transporter, which imports H+-equivalents, is a putative Cl-/OH- exchanger (CHE). A strong candidate for CHE is SLC26A6 protein, a product of the SLC26A gene family of anion transporters, which has been detected in murine heart. SLC26A6 protein is suggested to be an electrogenic 1Cl-/2OH-(2HCO3-) exchanger. Unfortunately, there is insufficient characterization of cardiac CHE against which the properties of heterologously expressed SLC26A6 can be matched. We therefore investigated the proton, Cl-, and voltage dependence of CHE activity in guinea-pig ventricular myocytes, using voltage-clamp, intracellular pH fluorescence, and mathematical modeling techniques. We find that CHE activity is tightly regulated by intracellular and extracellular pH, is voltage-insensitive over a wide range (+/-80 mV), and displays substrate dependence suggestive of electroneutral 1Cl-/1OH- exchange. These properties exclude electrogenic SLC26A6 as sole contributor to CHE. Either the SLC26A6 product in heart is electroneutral, or CHE comprises at least two transporters with oppositely balanced voltage sensitivity. Alternatively, CHE may comprise an H+-Cl- coinflux system, which cannot be distinguished kinetically from an exchanger. Irrespective of ionic mechanism, CHE's pH sensitivity helps to define resting intracellular pH, and hence basal function in the heart.

摘要

质子是心脏功能的强大调节因子。它们的细胞内浓度由肌膜离子转运体调节,这些转运体可输出或输入H⁺离子(或其离子等价物:HCO₃⁻、OH⁻)。一种这样的输入H⁺等价物的转运体是一种假定的Cl⁻/OH⁻交换体(CHE)。CHE的一个有力候选者是SLC26A6蛋白,它是阴离子转运体SLC26A基因家族的产物,已在小鼠心脏中检测到。SLC26A6蛋白被认为是一种生电的1Cl⁻/2OH⁻(2HCO₃⁻)交换体。不幸的是,针对心脏CHE的特性描述不足,无法与异源表达的SLC26A6的特性相匹配。因此,我们使用电压钳、细胞内pH荧光和数学建模技术,研究了豚鼠心室肌细胞中CHE活性对质子、Cl⁻和电压的依赖性。我们发现,CHE活性受到细胞内和细胞外pH的严格调节,在很宽的范围内(±80 mV)对电压不敏感,并表现出底物依赖性,提示为电中性的1Cl⁻/1OH⁻交换。这些特性排除了生电的SLC26A6作为CHE的唯一贡献者。要么心脏中的SLC26A6产物是电中性的,要么CHE至少包含两种具有相反平衡电压敏感性的转运体。或者,CHE可能包含一个H⁺-Cl⁻共流入系统,在动力学上无法与交换体区分开来。无论离子机制如何,CHE的pH敏感性有助于确定静息细胞内pH,从而确定心脏的基础功能。

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