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在渗透性利尿期间,尿素和氯化钠通过TonEBP途径以相反方向调节UT-A1尿素转运体。

Urea and NaCl regulate UT-A1 urea transporter in opposing directions via TonEBP pathway during osmotic diuresis.

作者信息

Kim Yu-Mi, Kim Wan-Young, Lee Hyun-Wook, Kim Jin, Kwon H Moo, Klein Janet D, Sands Jeff M, Kim Dongun

机构信息

Dept. of Pediatrics, The Catholic Univ. of Korea, Uijeongbu St. Mary's Hospital, 65-1 Kumoh-Dong, Uijeongbu 480-717, Republic of Korea.

出版信息

Am J Physiol Renal Physiol. 2009 Jan;296(1):F67-77. doi: 10.1152/ajprenal.00143.2008. Epub 2008 Oct 22.

DOI:10.1152/ajprenal.00143.2008
PMID:18945830
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2636911/
Abstract

In our previous studies of varying osmotic diuresis, UT-A1 urea transporter increased when urine and inner medullary (IM) interstitial urea concentration decreased. The purposes of this study were to examine 1) whether IM interstitial tonicity changes with different urine urea concentrations during osmotic dieresis and 2) whether the same result occurs even if the total urinary solute is decreased. Rats were fed a 4% high-salt diet (HSD) or a 5% high-urea diet (HUD) for 2 wk and compared with the control rats fed a regular diet containing 1% NaCl. The urine urea concentration decreased in HSD but increased in HUD. In the IM, UT-A1 and UT-A3 urea transporters, CLC-K1 chloride channel, and tonicity-enhanced binding protein (TonEBP) transcription factor were all increased in HSD and decreased in HUD. Next, rats were fed an 8% low-protein diet (LPD) or a 0.4% low-salt diet (LSD) to decrease the total urinary solute. Urine urea concentration significantly decreased in LPD but significantly increased in LSD. Rats fed the LPD had increased UT-A1 and UT-A3 in the IM base but decreased in the IM tip, resulting in impaired urine concentrating ability. The LSD rats had decreased UT-A1 and UT-A3 in both portions of the IM. CLC-K1 and TonEBP were unchanged by LPD or LSD. We conclude that changes in CLC-K1, UT-A1, UT-A3, and TonEBP play important roles in the renal response to osmotic diuresis in an attempt to minimize changes in plasma osmolality and maintain water homeostasis.

摘要

在我们之前关于不同程度渗透性利尿的研究中,当尿液和髓质内层(IM)间质尿素浓度降低时,UT-A1尿素转运体增加。本研究的目的是检验:1)在渗透性利尿期间,IM间质张力是否会随不同的尿液尿素浓度而变化;2)即使总尿溶质减少,是否会出现相同的结果。将大鼠喂食4%高盐饮食(HSD)或5%高尿素饮食(HUD)2周,并与喂食含1%氯化钠常规饮食的对照大鼠进行比较。HSD组尿液尿素浓度降低,而HUD组升高。在IM中,HSD组UT-A1和UT-A3尿素转运体、CLC-K1氯通道以及张力增强结合蛋白(TonEBP)转录因子均增加,而HUD组则减少。接下来,给大鼠喂食8%低蛋白饮食(LPD)或0.4%低盐饮食(LSD)以降低总尿溶质。LPD组尿液尿素浓度显著降低,而LSD组显著升高。喂食LPD的大鼠IM基部的UT-A1和UT-A3增加,但IM尖端减少,导致尿液浓缩能力受损。LSD大鼠IM的两个部分中UT-A1和UT-A3均减少。LPD或LSD对CLC-K1和TonEBP没有影响。我们得出结论,CLC-K1、UT-A1、UT-A3和TonEBP的变化在肾脏对渗透性利尿的反应中起重要作用,试图使血浆渗透压变化最小化并维持水平衡。

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本文引用的文献

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Forskolin stimulates phosphorylation and membrane accumulation of UT-A3.福司可林刺激UT - A3的磷酸化和膜聚集。
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