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B细胞中葡萄糖诱导的电活动的pH调节:Na/H和HCO3/Cl反向转运体的作用

pH modulation of glucose-induced electrical activity in B-cells: involvement of Na/H and HCO3/Cl antiporters.

作者信息

Pace C S, Tarvin J T

出版信息

J Membr Biol. 1983;73(1):39-49. doi: 10.1007/BF01870339.

Abstract

Regulation of intracellular pH is an essential function and may be especially significant in the B-cell in which the influence of glucose on electrical activity is modulated by alterations in pH. Two possible regulatory processes have been examined: Na/H and HCO3/Cl exchange, by using inhibitors, an ionophore, and changes of ionic concentrations. In the presence of 11.1 mM glucose we found that DIDS, an inhibitor of anion exchange, elicited a dose-response increase in the relative duration of the active phase with an ED50 of 99 microM. Probenecid (0.5 mM), an inhibitor of anion fluxes, also augmented the electrical activity (EA) due to glucose. Withdrawal of HCO-3 elicited constant spike activity followed by a resumption of burst activity with a greater duration of the active phase compared to control. These data are consistent with predicted cellular acidification. However, reduction of Cl-o by isethionate substitution produced no marked effect on EA. In contrast, SO-4- substitution for Cl- resulted in variable effects characterized by constant spike activity or a decrease in the duration of the active and silent phases along with silent hyperpolarization. Tributyltin, a Cl/OH, ionophore enhanced EA at 0.25 microM with 120 mM Cl-o, but reduced EA with 10 mM Cl- as would be predicted with either cellular acidification or alkalinization, respectively. Amiloride at 100 microM elicited constant spike activity perhaps due to inhibition of Na/H exchange. Reduction of Na+o from 142.8 to 40.8 mM had a similar effect and enhanced the influence of amiloride. It appears therefore that interference with putative pH regulatory mechanisms in the B-cell are consistent with the hypothesis that cell pH is involved in regulation of EA.

摘要

细胞内pH的调节是一项基本功能,在B细胞中可能尤为重要,因为葡萄糖对电活动的影响会受到pH变化的调节。我们研究了两种可能的调节过程:Na/H和HCO3/Cl交换,采用了抑制剂、离子载体以及离子浓度的变化。在11.1 mM葡萄糖存在的情况下,我们发现阴离子交换抑制剂DIDS能引起活动期相对持续时间的剂量反应性增加,半数有效剂量(ED50)为99 microM。阴离子通量抑制剂丙磺舒(0.5 mM)也增强了由葡萄糖引起的电活动(EA)。去除HCO-3会引发持续的锋电位活动,随后恢复爆发活动,与对照相比,活动期持续时间更长。这些数据与预测的细胞酸化一致。然而,用羟乙基磺酸替代Cl-以降低Cl-o对EA没有显著影响。相反,用SO-4-替代Cl-会产生不同的影响,其特征为持续的锋电位活动,或活动期和静息期持续时间缩短以及静息超极化。三丁基锡是一种Cl/OH离子载体,在120 mM Cl-o时,0.25 microM的三丁基锡增强了EA,但在10 mM Cl-时降低了EA,这分别与细胞酸化或碱化的预测结果相符。100 microM的氨氯吡咪可能由于抑制Na/H交换而引发持续的锋电位活动。将Na+o从142.8 mM降至40.8 mM有类似的效果,并增强了氨氯吡咪的影响。因此,干扰B细胞中假定的pH调节机制与细胞pH参与EA调节的假说一致。

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