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细胞黏附分子P-选择素在活动性炎症性肠病中的表达增加。

Increased expression of cell adhesion molecule P-selectin in active inflammatory bowel disease.

作者信息

Schürmann G M, Bishop A E, Facer P, Vecchio M, Lee J C, Rampton D S, Polak J M

机构信息

Department of Histochemistry, Royal Postgraduate Medical School, London.

出版信息

Gut. 1995 Mar;36(3):411-8. doi: 10.1136/gut.36.3.411.

Abstract

The pathogenic changes of inflammatory bowel disease (IBD) depend on migration of circulating leucocytes into intestinal tissues. Although leucocyte rolling and tenuous adhesion are probably regulated by inducible selectins on vascular endothelia, little is known about the expression of these molecules in Crohn's disease and ulcerative colitis. Using immunohistochemistry on surgically resected specimens, this study investigated endothelial P-selectin (CD62, granular membrane protein-140) in frozen sections of histologically uninvolved tissues adjacent to inflammation (Crohn's disease = 10; ulcerative colitis = 10), from highly inflamed areas (Crohn's disease = 20; ulcerative colitis = 13), and from normal bowel (n = 20). By light microscopy, two forms of P-selectin immunoreactivity were detected that apparently corresponded ultrastructurally to stored and released distributions. Compared with the normal gut, there was a 3.7-fold increase of P-selectin immunoreactivity on veins (p < 0.0001), venules (p < 0.0001), and capillaries (p < 0.05) in the highly inflamed gut, without differences between Crohn's disease and ulcerative colitis. In the uninvolved gut, P-selectin expression was similar to that seen in normal controls, except for a focal increase of P-selectin in the vicinity of small lymphocyte aggregates. The dramatic upregulation of P-selectin in the inflamed tissue and its potential role in leucocyte trafficking support the concept of P-selectin blocking therapy for the control of active IBD.

摘要

炎症性肠病(IBD)的病理变化取决于循环白细胞向肠道组织的迁移。尽管白细胞滚动和微弱黏附可能受血管内皮上诱导性选择素的调节,但对于这些分子在克罗恩病和溃疡性结肠炎中的表达情况却知之甚少。本研究通过对手术切除标本进行免疫组织化学,调查了炎症旁组织学上未受累的冰冻切片(克罗恩病 = 10例;溃疡性结肠炎 = 10例)、高度炎症区域(克罗恩病 = 20例;溃疡性结肠炎 = 13例)以及正常肠段(n = 20例)中的内皮P选择素(CD62,颗粒膜蛋白-140)。通过光学显微镜,检测到两种形式的P选择素免疫反应性,在超微结构上它们显然分别对应于储存和释放分布。与正常肠道相比,高度炎症肠道中静脉(p < 0.0001)、小静脉(p < 0.0001)和毛细血管(p < 0.05)上的P选择素免疫反应性增加了3.7倍,克罗恩病和溃疡性结肠炎之间无差异。在未受累肠道中,P选择素表达与正常对照相似,只是在小淋巴细胞聚集附近有局部增加。炎症组织中P选择素的显著上调及其在白细胞运输中的潜在作用支持了P选择素阻断疗法用于控制活动性IBD的概念。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9729/1382456/c59bf9cc1f42/gut00521-0108-a.jpg

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