Fabrizio Bar scite author profile

Evidence of an increased nitric oxide production in primary biliary cirrhosis. / Battista S; Bar F; Mengozzi G; Pollet C; Torchio M; Cavalli G; Rosina F; David E; Cutrin JC; Cavalieri B; Poli G; Molino G.. -In: AMERICAN JOURNAL OF GASTROENTEROLOGY. -ISSN 0002-9270. -96(2001), pp. 869-875. Original Citation:Evidence of an increased nitric oxide production in primary biliary cirrhosis. Terms of use:Open Access (Article begins on next page) Anyone can freely access the full text of works made available as "Open Access". Works made available under a Creative Commons license can be used according to the terms and conditions of said license. Use of all other works requires consent of the right holder (author or publisher) if not exempted from copyright protection by the applicable law. Availability: This is the author's manuscriptAlthough possible implications of nitric oxide in the pathophysiology of liver cirrhosis have been extensively studied, until now few articles have addressed the assessment of nitric oxide production in primary biliary cirrhosis. This study was directed to evaluate circulating nitrosyl-hemoglobin levels as well as neutrophil elastase and soluble adhesion molecule concentrations in this condition, by assuming these parameters as possible markers of either inflammatory response or neutrophil activation. METHODS:Laboratory investigations were performed in 30 patients with primary biliary cirrhosis, in 13 patients with postviral and/or alcoholic cirrhosis, and in a group of eight subjects with chronic hepatitis. RESULTS:Although no difference was detected with respect to chronic hepatitis subjects, higher levels of nitrosyl-hemoglobin adducts were found in primary biliary cirrhosis patients than in postviral or alcoholic cirrhotics and in normal subjects (3.55 Ϯ 1.75 arbitrary units vs 1.95 Ϯ 0.57 and 0.84 Ϯ 0.34, p ϭ 0.0004 and p Ͻ 0.0001, respectively). Similarly, more elevated concentrations of neutrophil elastase (213.7 Ϯ 192.0 g/L vs 51.1 Ϯ 34.3 and 38.0 Ϯ 11.5, p Ͻ 0.0001 and p Ͻ 0.0001, respectively) as well as of soluble forms of intercellular adhesion molecule 1 and endothelial-leukocyte adhesion molecule 1 were shown in primary biliary cirrhosis patients than in subjects with cirrhosis of other etiologies and in controls. CONCLUSIONS:Highly enhanced nitric oxide production in primary biliary cirrhosis could be related to the development of strong inflammation and at least partially to neutrophil activation, thus suggesting a putative role of these cellular mediators in the development of liver damage owing to their ability to synthesize and release a wide variety of important factors, including elastase and nitric oxide. (Am J Gastroenterol 2001;96:869 -875.

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Fabrizio Bar

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Evidence of an increased nitric oxide production in primary biliary cirrhosis

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