Regulation of Renal Sodium Transporters during Severe Inflammation

doi:10.1681/ASN.2006050454


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Published ahead of print on February 21, 2007
J Am Soc Nephrol 18: 1072-1083, 2007
© 2007 American Society of Nephrology
doi: 10.1681/ASN.2006050454

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Cell and Transport Physiology

Regulation of Renal Sodium Transporters during Severe Inflammation

Christoph Schmidt^*, Klaus Höcherl, Frank Schweda, Armin Kurtz and Michael Bucher^*

Departments of ^* Anesthesiology, Pharmacology, and Physiology, Regensburg University, Regensburg, Germany

Address correspondence to: Dr. Michael Bucher, Department of Anesthesiology, Regensburg University, 93042 Regensburg, Germany. Phone: +49-941-944-7801; Fax: +49-941-944-7802; E-mail: michael.bucher{at}klinik.uni-regensburg.de

Received for publication May 10, 2006. Accepted for publication January 5, 2007.

Sepsis-associated acute renal failure is characterized by decreasedGFR and tubular dysfunction. The pathogenesis of endotoxemictubular dysfunction with failure in urine concentration andincreased fractional sodium excretion is poorly understood.This study investigated the regulation of renal sodium transportersduring severe inflammation in vivo and in vitro. Injection ofhigh-dosage LPS reduced BP and GFR, increased fractional sodiumexcretion, and strongly decreased the expression of Na⁺/H⁺-exchanger,renal outer medullary potassium channel, Na⁺-K⁺-2Cl^– co-transporter,epithelial sodium channel, and Na⁺/K⁺-ATPase in mice. Also,injection of TNF- ${alpha}$ , IL-1 $beta$ , or IFN- ${gamma}$ decreased renal function andexpression of renal sodium transporters. LPS-induced downregulationof sodium transporters was not affected in cytokine-knockoutmice. However, supplementary glucocorticoid treatment, whichinhibited LPS-induced increase of tissue cytokine concentrations,attenuated LPS-induced renal dysfunction and downregulationof tubular sodium transporters. Injection of low-dosage LPSincreased renal tissue cytokines and downregulated renal sodiumtransporters without arterial hypotension. In vitro, in corticalcollecting duct cells, cytokines also decreased expression ofrenal outer medullary potassium channel, epithelial sodium channel,and Na⁺/K⁺-ATPase. Renal hypoperfusion by renal artery clippingdid not influence renal sodium transporter expression, in contrastto renal ischemia-reperfusion injury, which depressed transporterexpression. These findings demonstrate downregulation of renalsodium transporters that likely accounts for tubular dysfunctionduring inflammation. These data suggest that alteration of renalsodium transporters during LPS-induced acute renal failure ismediated by cytokines rather than renal ischemia. However, ina complex in vivo model of severe inflammation, the possiblepresence and influence of renal hypoperfusion and reperfusionon the expression of renal sodium transporters cannot be completelyexcluded.

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				S. de Seigneux, V. Leroy, H. Ghzili, M. Rousselot, S. Nielsen, B. C. Rossier, P.-Y. Martin, and E. Feraille NF-{kappa}B Inhibits Sodium Transport via Down-regulation of SGK1 in Renal Collecting Duct Principal Cells J. Biol. Chem., September 12, 2008; 283(37): 25671 - 25681. [Abstract] [Full Text] [PDF]

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