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| Research article summary (published 29 Apr 2009): |
Low-dose dexamethasone-supplemented fluid resuscitation reverses endotoxin-induced acute renal failure and prevents cortical microvascular hypoxia.
Full Abstract
There is growing evidence that impairment in intrarenal oxygenation and hypoxic injury might contribute to the pathogenesis of septic renal failure. An important molecule known to act on the renal microvascular tone and therefore consequently being involved in the regulation of intrarenal oxygen supply is NO. The main production of NO under septic conditions derives from iNOS, an enzyme that can be blocked by dexamethasone (DEX). In an animal model of endotoxin-induced renal failure, we tested the hypothesis that inhibition of iNOS by low-dose DEX would improve an impaired intrarenal oxygenation and kidney function. Twenty-two male Wistar rats received a 30-min intravenous infusion of LPS (2.5 mg/kg) and consecutively developed endotoxemic shock. Two hours later, in 12 animals, fluid resuscitation was initiated. Six rats did not receive resuscitation; four animals served as time control. In addition to the fluid, six animals received a bolus of low-dose DEX (0.1 mg/kg). In these animals, the renal iNOS mRNA expression was significantly suppressed 3 h later. Dexamethasone prevented the appearance of cortical microcirculatory hypoxic areas, improved renal oxygen delivery, and significantly restored oxygen consumption. Besides a significant increase in MAP and renal blood flow, DEX restored kidney function and tubular sodium reabsorption to baseline values. In conclusion, treatment with low-dose DEX in addition to fluid resuscitation reversed endotoxin-induced renal failure associated by an improvement in intrarenal microvascular oxygenation. Therefore, low-dose DEX might have potential application in the prevention of septic acute renal failure.
Author information
Author/s: Johannes, Tanja (T); Mik, Egbert G (EG); Klingel, Karin (K); Dieterich, Hans-Jürgen (HJ); Unertl, Klaus E (KE); Ince, Can (C);
Affiliation: Department of Physiology, Academic Medical Center, University of Amsterdam, The Netherlands. Tanja.Johannes(-atsign-)uni-tuebingen.de
Journal and publication information
Publication Type: Journal Article; Research Support, Non-U.S. Gov't
Journal: Shock (Augusta, Ga.) (Shock), published in United States. (Language: eng)
Reference: 2009-May; vol 31 (issue 5) : pp 521-8
Dates: Created 2009/04/14; Completed 2009/06/29;
PMID: 18827749, status: MEDLINE (last retrieved date: 6/29/2009)
Sourced from the National Library of Medicine. Abstract text and other information may be subject to copyright.
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Associated Chemicals: Endotoxins (0) ; Dexamethasone (50-02-2) ; Oxygen (7782-44-7)Related articles
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