Chronic intestinal inflammation and angiogenesis in genetically susceptible rats is modulated by kininogen deficiency
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- 作者:Isordia-Salas ; Irma ; Pixley ; Robin A. ; Li ; Fengling ; Sainz ; Irma ; Balfour Sartor ; R. ; Adam ; Albert ; et. al.
- 关键词:Inflammatory bowel disease ; Experimental colitis ; Kallikrein&ndash ; kinin system ; Contact system
- 刊名:International Immunopharmacology
- 出版年:2002
- 出版时间:December, 2002
- 年:2002
- 卷:2
- 期:13-14
- 页码:1895-1905
- 全文大小:381 K
文摘
Genetically susceptible Lewis rats injected in the intestinal wall with peptidoglycan-polysaccharide (PG-APS) polymers develop chronic granulomatous enterocolitis associated with activation of the kallikrein–kinin system. To elucidate the role of high-molecular-weight kininogen (HK), we backcrossed Brown Norway rats having an HK deficiency with Lewis rats for five generations. Two new strains were produced, wild-type F5 (F5WT) and HK deficient (F5HKd), each with a 
97 % Lewis genome. The HK values of F5WT rat plasma and F5HKd rat plasma were 0.62±0.20 and 0.08±0.03 U/ml, respectively. Among the inflammatory changes, the mean gross gut, total intestinal histologic and liver granuloma score and the white blood count were significantly lower in the F5HKd than the F5WT rats. Plasma T-kininogen was significantly less in F5HKd. Angiogenesis (mean vascular density) in the cecum was decreased significantly in F5HKd compared to F5WT. These results indicate the importance of the kallikrein–kinin system in this model of chronic enterocolitis and systemic inflammation.
97 % Lewis genome. The HK values of F5WT rat plasma and F5HKd rat plasma were 0.62±0.20 and 0.08±0.03 U/ml, respectively. Among the inflammatory changes, the mean gross gut, total intestinal histologic and liver granuloma score and the white blood count were significantly lower in the F5HKd than the F5WT rats. Plasma T-kininogen was significantly less in F5HKd. Angiogenesis (mean vascular density) in the cecum was decreased significantly in F5HKd compared to F5WT. These results indicate the importance of the kallikrein–kinin system in this model of chronic enterocolitis and systemic inflammation.