首页> 外文期刊>Journal of Leukocyte Biology: An Official Publication of the Reticuloendothelial Society >Combinatorial requirements for adhesion molecules in mediating neutrophil emigration during bacterial peritonitis in mice.
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Combinatorial requirements for adhesion molecules in mediating neutrophil emigration during bacterial peritonitis in mice.

机译:在小鼠细菌性腹膜炎期间介导嗜中性粒细胞迁移的粘附分子的组合要求。

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摘要

To investigate the requirements for adhesion molecules in neutrophil emigration during peritonitis, mice received intraperitoneal injections of Streptococcus pneumoniae while the functions of multiple adhesion molecules were blocked. Emigration after 4 h was compromised by antibodies against ICAM-1 or genetic deficiency of ICAM-1. Anti-CD11a/CD18 antibodies decreased emigration in ICAM-1 mutant mice, suggesting that ICAM-1 independent emigration requires CD11/CD18 complexes. In contrast, mice mutant in ICAM-1 plus E-selectin showed no defect in emigration, suggesting that E-selectin commits neutrophils to an ICAM-1-dependent pathway during streptococcal peritonitis. However, in mutant mice lacking the three endothelial adhesion molecules E-selectin, P-selectin, and ICAM-1, emigration after 4 h was significantly compromised. Thus, P-selectin is essential to ICAM-1- and E-selectin-independent acute peritoneal inflammation. After 24 h of peritonitis, there were no differences between WT and E-selectin/P-selectin/ICAM-1 mutant mice, demonstrating that these endothelial adhesion molecules are not essential to neutrophil emigration during later stages of peritonitis.
机译:为了研究腹膜炎期间嗜中性粒细胞迁移中粘附分子的需求,小鼠腹膜内注射了肺炎链球菌,同时多种粘附分子的功能被阻断。 4小时后的迁移受到针对ICAM-1的抗体或ICAM-1基因缺陷的损害。抗CD11a / CD18抗体减少了ICAM-1突变小鼠的移出,表明ICAM-1独立的移出需要CD11 / CD18复合物。相比之下,ICAM-1加上E-选择素的突变小鼠在迁徙中没有显示出缺陷,这表明在链球菌性腹膜炎期间E-选择素使嗜中性粒细胞参与了ICAM-1依赖性途径。但是,在缺少三个内皮粘附分子E-选择素,P-选择素和ICAM-1的突变小鼠中,4小时后的迁移受到显着损害。因此,P-选择素对于ICAM-1-和E-选择素非依赖性急性腹膜炎症至关重要。腹膜炎24小时后,WT和E-选择素/ P-选择素/ ICAM-1突变小鼠之间没有差异,表明这些内皮粘附分子对于腹膜炎后期的中性粒细胞迁移不是必需的。

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