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角膜上皮擦伤后中性粒细胞迁移的两波反应:不同的黏附分子需求

Two waves of neutrophil emigration in response to corneal epithelial abrasion: distinct adhesion molecule requirements.

作者信息

Li Zhijie, Burns Alan R, Smith C Wayne

机构信息

Section of Leukocyte Biology, Department of Pediatrics, Children's Nutrition Research Center, Baylor College of Medicine, Houston, Texas 77030, USA.

出版信息

Invest Ophthalmol Vis Sci. 2006 May;47(5):1947-55. doi: 10.1167/iovs.05-1193.

Abstract

PURPOSE

Corneal abrasion results in an inflammatory response characterized by leukocyte emigration into the corneal stroma. Adhesion molecules play a critical role in leukocyte emigration to wound sites, but differences are evident in different vascular beds. In this study, the contributions of two families of adhesion molecules to neutrophil emigration into the cornea were investigated.

METHODS

Re-epithelialization, patterns of neutrophil influx and CXC chemokine production were assessed in C57Bl/6 mice after removal of a 2-mm diameter area of central corneal epithelium. Comparisons were made between wild-type (WT) mice and mice with targeted deletions of genes for CD18 (CD18(-/-)) or P- and E-selectin (P/E-sel(-/-)) or in mice with antibody-induced neutropenia.

RESULTS

Wild-type mice exhibited neutrophil emigration in two waves, the first peaking at 18 hours and the second at 30 hours after wounding, 6 hours after epithelial wound closure and peak levels of corneal CXCL1. In CD18(-/-) animals, only a single wave of neutrophil influx was seen, and it was temporally and quantitatively equivalent to the second wave in WT. In P/E-sel(-/-) mice, neutrophil influx was markedly depressed throughout the 48-hour observation period. Re-epithelialization was significantly delayed in mice with adhesion molecule deletions and in neutropenic animals. Transfer of wild-type leukocytes into CD18(-/-) mice resulted in neutrophil emigration into the injured cornea within 18 hours of wounding and improved closure of the epithelium.

CONCLUSIONS

Neutrophil emigration into corneal stroma after epithelial abrasion occurs in two waves. The first is dependent on CD18 integrins and selectins, whereas the second is CD18-independent but requires selectins. Early leukocyte emigration appears to promote re-epithelialization.

摘要

目的

角膜擦伤会引发炎症反应,其特征为白细胞迁移至角膜基质。黏附分子在白细胞迁移至伤口部位的过程中起关键作用,但在不同血管床中存在明显差异。在本研究中,调查了两类黏附分子对中性粒细胞迁移至角膜的作用。

方法

在C57Bl/6小鼠中,去除直径2毫米的中央角膜上皮区域后,评估再上皮化、中性粒细胞流入模式和CXC趋化因子的产生。对野生型(WT)小鼠与CD18基因靶向缺失(CD18(-/-))或P-和E-选择素基因靶向缺失(P/E-sel(-/-))的小鼠,或抗体诱导的中性粒细胞减少的小鼠进行比较。

结果

野生型小鼠中性粒细胞迁移呈两波,第一波在受伤后18小时达到峰值,第二波在30小时达到峰值,此时上皮伤口已闭合,角膜CXCL1达到峰值水平。在CD18(-/-)动物中,仅观察到一波中性粒细胞流入,其时间和数量与野生型中的第二波相当。在P/E-sel(-/-)小鼠中,在整个48小时观察期内中性粒细胞流入明显减少。黏附分子缺失的小鼠和中性粒细胞减少的动物中,再上皮化明显延迟。将野生型白细胞转移至CD18(-/-)小鼠中,导致受伤后18小时内中性粒细胞迁移至受伤角膜,并改善了上皮的闭合。

结论

上皮擦伤后中性粒细胞迁移至角膜基质呈两波。第一波依赖于CD18整合素和选择素,而第二波不依赖CD18但需要选择素。早期白细胞迁移似乎促进了再上皮化。

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