Effect of inhaled KP-496, a novel dual antagonist of the cysteinyl leukotriene and thromboxane A2 receptors, on a bleomycin-induced pulmonary fibrosis model in mice
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作者:
Kurokawa, Shigeo
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Kaken Pharmaceut Co Ltd, Dept Pharmacol, Cent Res Labs, Yamashina Ku, Kyoto 6078042, JapanKaken Pharmaceut Co Ltd, Dept Pharmacol, Cent Res Labs, Yamashina Ku, Kyoto 6078042, Japan
Kurokawa, Shigeo
[1
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Suda, Masahiro
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Kaken Pharmaceut Co Ltd, Dept Pharmacol, Cent Res Labs, Yamashina Ku, Kyoto 6078042, JapanKaken Pharmaceut Co Ltd, Dept Pharmacol, Cent Res Labs, Yamashina Ku, Kyoto 6078042, Japan
Suda, Masahiro
[1
]
Okuda, Toshiaki
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Kaken Pharmaceut Co Ltd, Dept Pharmacol, Cent Res Labs, Yamashina Ku, Kyoto 6078042, JapanKaken Pharmaceut Co Ltd, Dept Pharmacol, Cent Res Labs, Yamashina Ku, Kyoto 6078042, Japan
Okuda, Toshiaki
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]
Miyake, Yoshihide
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Kaken Pharmaceut Co Ltd, Dept Pharmacol, Cent Res Labs, Yamashina Ku, Kyoto 6078042, JapanKaken Pharmaceut Co Ltd, Dept Pharmacol, Cent Res Labs, Yamashina Ku, Kyoto 6078042, Japan
Miyake, Yoshihide
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Matsumura, Yuzuru
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Kaken Pharmaceut Co Ltd, Dept Pharmacol, Cent Res Labs, Yamashina Ku, Kyoto 6078042, JapanKaken Pharmaceut Co Ltd, Dept Pharmacol, Cent Res Labs, Yamashina Ku, Kyoto 6078042, Japan
Matsumura, Yuzuru
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Ishimura, Masakazu
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Kaken Pharmaceut Co Ltd, Dept Pharmacol, Cent Res Labs, Yamashina Ku, Kyoto 6078042, JapanKaken Pharmaceut Co Ltd, Dept Pharmacol, Cent Res Labs, Yamashina Ku, Kyoto 6078042, Japan
Ishimura, Masakazu
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Saito, Ryota
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Kaken Pharmaceut Co Ltd, Dept Pharmacol, Cent Res Labs, Yamashina Ku, Kyoto 6078042, JapanKaken Pharmaceut Co Ltd, Dept Pharmacol, Cent Res Labs, Yamashina Ku, Kyoto 6078042, Japan
Saito, Ryota
[1
]
Nakamura, Tsutomu
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Kaken Pharmaceut Co Ltd, Dept Pharmacol, Cent Res Labs, Yamashina Ku, Kyoto 6078042, JapanKaken Pharmaceut Co Ltd, Dept Pharmacol, Cent Res Labs, Yamashina Ku, Kyoto 6078042, Japan
Nakamura, Tsutomu
[1
]
机构:
[1] Kaken Pharmaceut Co Ltd, Dept Pharmacol, Cent Res Labs, Yamashina Ku, Kyoto 6078042, Japan
Cysteinyl-leukotrienes (cysLTs) and thromboxane A(2) (TXA(2)) are important mediators in inflammatory lung diseases such as bronchial asthma and idiopathic pulmonary fibrosis (IPF). We examined the effects of inhaled KP-496, a novel dual antagonist of the cysLTs and TXA(2) receptors, on bleomycin-induced IPF in mice. Mice were intravenously injected bleomycin on day 0, and 0.5% of KP-496 was inhaled twice a day (30 min/time) for the entire experimental period. The effects of KP-496 were evaluated by the number of infiltrated cells in bronchoalveolar lavage fluid (BALF), hydroxyl-L-proline content in the lung, and histopathology. Analyses of BALF on days 7 and 21 revealed that inhaled KP-496 significantly decreased total cell numbers, macrophages, neutrophils, and eosinophils on both days. KP-496 significantly decreased hydroxyl-L-proline content in the lung on day 21. Histopathological analyses of lungs on day 21 demonstrated that KP-496 significantly suppressed inflammatory and fibrotic changes. Our results suggested that the suppression of cysLTs and TXA(2) pathways by KP-496 could control airway inflammation and pulmonary fibrosis, and that KP-496 could be a new therapeutic agent for lung diseases with inflammation and fibrogenesis such as IPF and chronic obstructive pulmonary disease. (C) 2010 Elsevier Ltd. All rights reserved.