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NHE3在促进近端小管中甲酸依赖的NaCl重吸收方面的重要作用。

Essential role of NHE3 in facilitating formate-dependent NaCl absorption in the proximal tubule.

作者信息

Wang T, Yang C L, Abbiati T, Shull G E, Giebisch G, Aronson P S

机构信息

Department of Cellular and Molecular Physiology, Yale University School of Medicine, New Haven, Connecticut 06520-8029, USA.

出版信息

Am J Physiol Renal Physiol. 2001 Aug;281(2):F288-92. doi: 10.1152/ajprenal.2001.281.2.F288.

Abstract

The absorption of NaCl in the proximal tubule is markedly stimulated by formate. This stimulation of NaCl transport is consistent with a cell model involving Cl(-)-formate exchange in parallel with pH-coupled formate recycling due to nonionic diffusion of formic acid or H(+)-formate cotransport. The formate recycling process requires H(+) secretion. Although Na(+)-H(+) exchanger isoform NHE3 accounts for the largest component of H(+) secretion in the proximal tubule, 40-50% of the rates of HCO absorption or cellular H(+) extrusion persist in NHE3 null mice. The purpose of the present investigation is to use NHE3 null mice to directly test the role of apical membrane NHE3 in mediating NaCl absorption stimulated by formate. We demonstrate that formate stimulates NaCl absorption in the mouse proximal tubule microperfused in vivo, but the component of NaCl absorption stimulated by formate is absent in NHE3 null mice. In contrast, stimulation of NaCl absorption by oxalate is preserved in NHE3 null mice, indicating that oxalate-stimulated NaCl absorption is independent of Na(+)-H(+) exchange. The virtually complete dependence of formate-induced NaCl absorption on NHE3 activity raises the possibility that NHE3 and the formate transporters are functionally coupled in the brush border membrane.

摘要

近端小管中NaCl的吸收受到甲酸盐的显著刺激。这种对NaCl转运的刺激与一种细胞模型一致,该模型涉及Cl⁻-甲酸盐交换,同时由于甲酸的非离子扩散或H⁺-甲酸盐共转运而存在pH偶联的甲酸盐循环。甲酸盐循环过程需要分泌H⁺。尽管Na⁺-H⁺交换体异构体NHE3在近端小管H⁺分泌中占最大比例,但在NHE3基因敲除小鼠中,仍有40 - 50%的HCO吸收或细胞H⁺排出速率存在。本研究的目的是利用NHE3基因敲除小鼠直接测试顶端膜NHE3在介导甲酸盐刺激的NaCl吸收中的作用。我们证明,甲酸盐可刺激体内微灌注的小鼠近端小管对NaCl的吸收,但在NHE3基因敲除小鼠中,甲酸盐刺激的NaCl吸收成分缺失。相反,草酸盐刺激的NaCl吸收在NHE3基因敲除小鼠中得以保留,这表明草酸盐刺激的NaCl吸收独立于Na⁺-H⁺交换。甲酸盐诱导的NaCl吸收几乎完全依赖于NHE3活性,这增加了NHE3与甲酸盐转运体在刷状缘膜上功能偶联的可能性。

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