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钠氢交换对大鼠髓袢钠重吸收的作用:一项微灌注研究

Contribution of Na+-H+ exchange to sodium reabsorption in the loop of henle: a microperfusion study in rats.

作者信息

Shirley D G, Walter S J, Unwin R J, Giebisch G

机构信息

Division of Biomedical Sciences, Imperial College School of Medicine, Charing Cross Hospital, London W6 8RF, UK.

出版信息

J Physiol. 1998 Nov 15;513 ( Pt 1)(Pt 1):243-9. doi: 10.1111/j.1469-7793.1998.243by.x.

Abstract
  1. The contribution of apical Na+-H+ exchange to sodium reabsorption in the thick ascending limb of the loop of Henle (TALH) in vivo was examined in anaesthetized rats by perfusing loops of Henle of superficial nephrons with solutions containing the Na+-H+ exchange inhibitor, ethyl isopropyl amiloride (EIPA). 2. Using a standard perfusate, no statistically significant effect of EIPA on net sodium reabsorption (JNa) was detected. However, when sodium reabsorption in the pars recta of the proximal tubule was minimized by using a low-sodium perfusate, EIPA reduced JNa from 828 +/- 41 to 726 +/- 37 pmol min-1 (P < 0.05), indicating that apical Na+-H+ exchange can make a small contribution to net sodium reabsorption in the TALH in vivo. This contribution appears to be dependent on the bicarbonate load, since an increase in the latter led to an enhancement of EIPA-sensitive sodium transport. 3. Addition of the Na+-K+-2Cl- cotransport inhibitor, bumetanide, to the low-sodium perfusate reduced baseline JNa to 86 +/- 27 pmol min-1. In this setting, EIPA reduced JNa further, to -24 +/- 18 pmol min-1 (P < 0.05), an effect similar to that seen in the absence of bumetanide. This finding argues against previous suggestions (based on in vitro evidence) that inhibition of the Na+-K+-2Cl- cotransporter leads to an increase in apical Na+-H+ exchange in the TALH.
摘要
  1. 在麻醉大鼠体内,通过向浅表肾单位的髓袢升支粗段(TALH)灌注含有钠氢交换抑制剂乙基异丙基氨氯吡咪(EIPA)的溶液,研究顶端钠氢交换对髓袢升支粗段钠重吸收的贡献。2. 使用标准灌注液时,未检测到EIPA对钠净重吸收(JNa)有统计学显著影响。然而,当使用低钠灌注液使近端小管直部的钠重吸收减至最小时,EIPA使JNa从828±41降至726±37 pmol·min⁻¹(P<0.05),表明顶端钠氢交换对体内TALH的钠净重吸收有小贡献。这种贡献似乎依赖于碳酸氢盐负荷,因为后者增加会导致EIPA敏感的钠转运增强。3. 向低钠灌注液中添加钠钾氯共转运抑制剂布美他尼,使基线JNa降至86±27 pmol·min⁻¹。在此情况下,EIPA使JNa进一步降至 -24±18 pmol·min⁻¹(P<0.05),这一效应与未用布美他尼时相似。这一发现与先前基于体外证据提出的观点相悖,即抑制钠钾氯共转运体会导致TALH中顶端钠氢交换增加。

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