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Am J Physiol Regul Integr Comp Physiol 297: R362-R369, 2009. First published June 3, 2009; doi:10.1152/ajpregu.00184.2009
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ARTICLES

Bile high-mobility group box 1 contributes to gut barrier dysfunction in experimental endotoxemia

Runkuan Yang,1 Keita Miki,1 Niku Oksala,2 Atsunori Nakao,3 Leena Lindgren,2 Meaghan E. Killeen,1 Ari Mennander,2 Mitchell P. Fink,1 and Jyrki Tenhunen2

1Department of Critical Care Medicine, University of Pittsburgh Medical School, Pittsburgh; 2Department of Intensive Care Medicine, University of Tampere Medical School, Finland; and 3Department of Surgery, University of Pittsburgh Medical School, Pittsburgh, Pennsylvania

Submitted 28 March 2009 ; accepted in final form 22 May 2009

Lipopolysaccharide (LPS) is an important factor in sepsis. LPS given by intraperitoneal injection induces intestinal hyperpermeability and bacterial translocation in animals and stimulates hepatic Kupffer cells to release TNF-{alpha} into the bile. This study aims to test the hypothesis that in response to LPS stimulation, hepatic Kupffer cells and extrahepatic macrophages release a large amount of the inflammatory cytokine high-mobility group box 1 (HMGB1) into the bile and that bile containing HMGB1 contributes to gut barrier dysfunction in experimental endotoxemia. To test this, rat common bile ducts were catheterized and bile flow rate was monitored before and during the LPS administration. Eight hours after LPS challenge, anti-HMGB1 neutralizing antibody or nonimmune (sham) IgG was injected into the duodenal lumen of endotoxemic rats; normal mice were also gavaged with normal or endotoxemic rat bile (bile collected from LPS-treated rats). We found that after LPS challenge, the bile flow rate in rats was significantly decreased at the 4- to 12-h time points, TNF-{alpha} concentration in the bile was markedly elevated at the 3- to 4-h time points, and bile HMGB1 levels were significantly increased at the 8- to 12-h time points. Duodenal injection with anti-HMGB1 antibody reversed LPS-induced gut barrier dysfunction in rats. In addition, feeding endotoxemic rat bile to normal mice significantly increased both mucosal permeability and bacterial translocation. The increase in permeability and bacterial translocation was reversible following removal of HMGB1 from the endotoxemic rat bile. These findings document that bile HMGB1 mediates gut barrier dysfunction in experimental endotoxemia.

endotoxemia; gut barrier function


Address for reprint requests and other correspondence: R. Yang, Dept. of Critical Care Medicine, Univ. of Pittsburgh Medical School, 1055 Scaife Hall, 3550 Terrace St., Pittsburgh, PA 15261 (e-mail: yangr{at}ccm.upmc.edu)






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