Novel signaling mechanisms of intracellular angiotensin II-induced NHE3 expression and activation in mouse proximal tubule cells

被引：31

作者：

Li, X. C. ^{[1
]}

Hopfer, U. ^{[2
]}

Zhuo, J. L. ^{[1
,3
,4
]}

机构：

[1] Univ Mississippi, Med Ctr, Dept Pharmacol & Toxicol, Lab Receptor & Signal Transduct, Jackson, MS 39216 USA

[2] Case Western Reserve Univ, Sch Med, Dept Physiol & Biophys, Cleveland, OH 44106 USA

[3] Univ Mississippi, Med Ctr, Dept Internal Med, Div Nephrol, Jackson, MS 39216 USA

[4] Univ Mississippi, Med Ctr, Ctr Excellence Cardiovasc Renal Res, Jackson, MS 39216 USA

来源：

AMERICAN JOURNAL OF PHYSIOLOGY-RENAL PHYSIOLOGY | 2012年 / 303卷 / 12期

关键词：

kidney; intracrine or intracellular angiotensin II; mouse proximal tubule cells; receptor and signal transduction; transporters; VASCULAR SMOOTH-MUSCLE; FACTOR-KAPPA-B; RECEPTOR-DEFICIENT MICE; AT(1) RECEPTOR; ANG-II; BLOOD-PRESSURE; FLUORESCENT FUSION; TYPE-2; RECEPTOR; AT(2) RECEPTORS; RENAL-CELLS;

D O I：

10.1152/ajprenal.00219.2012

中图分类号：

Q4 [生理学];

学科分类号：

071003 ;

摘要：

Li XC, Hopfer U, Zhuo JL. Novel signaling mechanisms of intracellular angiotensin II-induced NHE3 expression and activation in mouse proximal tubule cells. Am J Physiol Renal Physiol 303: F1617-F1628, 2012. First published October 3, 2012; doi:10.1152/ajprenal.00219.2012.- Expression of a cytosolic cyan fluorescent fusion protein of angiotensin II (ECFP/ANG II) in proximal tubules increases blood pressure in rodents. To determine cellular signaling pathways responsible for this response, we expressed ECFP/ANG II in transport-competent mouse proximal convoluted tubule cells (mPCT) from wild-type (WT) and type 1a ANG II receptor-deficient (AT(1a)-KO) mice and measured its effects on intracellular ANG II levels, surrogates of Na/H exchanger 3 (NHE3)-dependent Na+ absorption, as well as MAP kinases and NF-kappa B signaling. In WT mPCT cells, ECFP/ANG II expression doubled ANG II levels, increased NHE3 expression and membrane phospho-NHE3 proteins threefold and intracellular Na+ concentration by 65%. These responses were associated with threefold increases in phospho-ERK 1/2 and phospho-p38 MAPK, fivefold increases in p65 subunit of NF-kappa B, and threefold increases in phospho-IKK alpha/beta (Ser 176/180) proteins. These signaling responses to ECFP/ANG II were inhibited by losartan (AT(1) blocker), PD123319 (AT(2) blocker), U0126 (MEK1/MEK2 inhibitor), and RO 106-9920 (NF-kappa B inhibitor). In mPCT cells of AT(1a)-KO mice, ECFP/ANG II also increased the levels of NHE3, p-ERK1/2, and p65 proteins above their controls, but considerably less so than in WT cells. In WT mice, selective expression of ECFP/ANG II in vivo in proximal tubules significantly increased blood pressure and indices of sodium reabsorption, in particular levels of phosphorylated NHE3 protein in the membrane fraction and proton gradient-stimulated Na-22(+) uptake by proximal tubules. We conclude that intracellular ANG II may induce NHE3 expression and activation in mPCTs via AT(1a)- and AT(2) receptor-mediated activation of MAP kinases ERK 1/2 and NF-kappa B signaling pathways.

引用

页码：F1617 / F1628

页数：12

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