| Literature DB >> 17510494 |
Shuji Ohsugi1, Yoshinobu Iwasaki, Yoshizumi Takemura, Kazuhiro Nagata, Hidehiko Harada, Ichiro Yokomura, Shigekuni Hosogi, Tatsuya Yuba, Naomi Niisato, Hiroaki Miyazaki, Hiroaki Matsubara, Shinji Fushiki, Yoshinori Marunaka.
Abstract
Excessive nitric oxide (NO) generated by inducible nitric oxide synthase (iNOS) aggravates acute lung injury (ALI) by producing peroxynitrite. We previously showed by immunostaining that the expression of iNOS was suppressed by inhalation of N(G)-nitro-L-arginine methyl ester in mice with Candida-induced ALI. This study tested the hypothesis that a novel iNOS inhibitor suppresses not only iNOS expression, but also iNOS messenger RNA (mRNA) production by interrupting a positive feedback loop at the time of NO production in Candida-induced ALI. Mice were pretreated by inhalation of saline or ONO-1714, a selective iNOS inhibitor, and were given an intravenous injection of Candida albicans to induce ALI. After inhalation of 1 mM aerosolized ONO-1714, the nitrite-nitrate concentration in bronchoalveolar lavage fluid (BALF) at 24 h was significantly lower than that after inhalation of saline. Tumor necrosis factor-alpha (TNF-alpha) and interleukin-1beta (IL-1beta) levels and neutrophils in BALF were decreased by inhalation of ONO-1714. Inhalation of ONO-1714 markedly suppressed nitrotyrosine production and inhibited the expression of iNOS mRNA as well as proteins in the lung. Survival was prolonged by inhalation of ONO-1714. We conclude that pretreatment with inhaled ONO-1714 suppresses the production of peroxinitrite and decreases oxidative stress associated with peroxinitrite in Candida-induced ALI.Entities:
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Year: 2007 PMID: 17510494 DOI: 10.2220/biomedres.28.91
Source DB: PubMed Journal: Biomed Res ISSN: 0388-6107 Impact factor: 1.203