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离子交换器在近端小管介导氯化钠转运中的作用。

Role of ion exchangers in mediating NaCl transport in the proximal tubule.

作者信息

Aronson P S

机构信息

Department of Medicine, Yale University School of Medicine, New Haven, Connecticut, USA.

出版信息

Kidney Int. 1996 Jun;49(6):1665-70. doi: 10.1038/ki.1996.243.

Abstract

The reabsorption of NaCl in the proximal tubule occurs passively through the paracellular pathway, and actively by a transcellular route. Transcellular NaCl transport involves Na(+)-coupled Cl- entry across the apical membrane by two mechanisms involving Cl(-)-organic anion exchange. One mechanism is Cl(-)-formate exchange with recycling of formate from lumen to cell by H(+)-coupled formate transport in parallel with Na(+)-H+ exchange. A second mechanism is Cl(-)-oxalate exchange with recycling of oxalate from lumen to cell by oxalate-sulfate exchange in parallel with Na(+)-sulfate cotransport. Cl- exit across the basolateral membrane is most likely mediated by Cl- channels. Apical membrane Na(+)-H+ exchange is involved in mediating both NaHCO3 and NaCl reabsorption in the proximal tubule. Immunocytochemical studies indicate that NHE3 is the principal Na(+)-H+ exchanger isoform expressed on the brush border membrane. Detection of NHE3 in a subapical, intracellular, vesicular compartment in proximal tubule cells is consistent with its possible regulation by membrane trafficking. That NHE3 is the isoform responsible for apical membrane Na(+)-H+ exchange activity is supported by studies of inhibitor sensitivity, and by studies demonstrating increased expression of NHE3 protein in association with enhanced Na(+)-H+ exchange activity during renal maturation and in response to glucocorticoids and metabolic acidosis.

摘要

近端小管中NaCl的重吸收通过细胞旁途径被动发生,并通过跨细胞途径主动进行。跨细胞NaCl转运涉及通过两种涉及Cl⁻ - 有机阴离子交换的机制,通过顶膜进行Na⁺ 偶联的Cl⁻ 进入。一种机制是Cl⁻ - 甲酸交换,甲酸通过与Na⁺ - H⁺ 交换平行的H⁺ 偶联的甲酸转运从管腔循环到细胞。第二种机制是Cl⁻ - 草酸盐交换,草酸盐通过与Na⁺ - 硫酸盐共转运平行的草酸盐 - 硫酸盐交换从管腔循环到细胞。Cl⁻ 通过基底外侧膜的排出最可能由Cl⁻ 通道介导。顶膜Na⁺ - H⁺ 交换参与介导近端小管中NaHCO₃ 和NaCl的重吸收。免疫细胞化学研究表明,NHE3是在刷状缘膜上表达的主要Na⁺ - H⁺ 交换异构体。在近端小管细胞的亚顶端、细胞内、囊泡区室中检测到NHE3与其可能通过膜运输进行调节一致。NHE3是负责顶膜Na⁺ - H⁺ 交换活性的异构体,这一观点得到了抑制剂敏感性研究以及在肾脏成熟过程中以及对糖皮质激素和代谢性酸中毒反应中NHE3蛋白表达增加与Na⁺ - H⁺ 交换活性增强相关的研究的支持。

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