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Time Course of Inducible NOS Expression of Lung Tissue during Sepsis in a Rat Model  

Kim, Joong Hee (Department of Emergency Medicine, Seoul National University College of Medicine)
Kim, Seong Chun (Department of Emergency Medicine, Gyeongsang National University Hospital)
Kwon, Woon Yong (Department of Emergency Medicine, Seoul National University College of Medicine)
Suh, Gil Joon (Department of Emergency Medicine, Seoul National University College of Medicine)
Youn, Yeo Kyu (Department of Surgery, Seoul National University College of Medicine)
Publication Information
Journal of Trauma and Injury / v.21, no.2, 2008 , pp. 120-127 More about this Journal
Abstract
Purpose: Many studies on the time course of inducible nitric oxide synthase (iNOS) gene expression have been performed in the LPS (Lipopolysaccharide)-induced endotoxemic model, but there have been few experimental approaches to continuous peritonitis-induced sepsis model. We conducted this study to establish basic data for future sepsis-related research by investigating the time course of iNOS gene expression and the relationship with the production of inflammatory mediators in the early sepsis model induced by cecal ligation and puncture (CLP). Methods: Male Sprague-Dawley rats were operated on by sing the CLP method to induce of peritonitis; and then, they were sacrificed and samples of blood and lung tissues were obtained at various times (1,2,3,6,9 and 12 h after CLP). We observed the expression of iNOS mRNA from lung tissues and measured the synthesis of nitric oxide, $IL-1{\beta}$, and $TNF-{\alpha}$ from the blood. Results: iNOS mRNA began to be expressed at 3 h and was maintained untill 12 h after CLP. The nitric oxide concentration was increased significantly at 6 h, reached its peak level at 9 h, and maintained a plateau untill 12 h after CLP. $TNF-{\alpha}$ began to be detected at 3 h, increased gradually, and decreased steeply from 9 h after CLP. $IL-1{\beta}$ showed its peak level at 6 h after CLP, and tended to decrease without significance. Conclusion: We observed that the iNOS gene was expressed later in peritonitis-induced sepsis than in LPS-induced sepsis. Nitric oxide and key inflammatory mediators were also expressed later in peritonitis-induced sepsis than in LPS-induced sepsis.
Keywords
Nitric oxide synthase; Inflammation mediators; Sepsis; Peritonitis;
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