炎症性肠病
血栓调节蛋白
内皮蛋白C受体
炎症
趋化因子
免疫学
细胞粘附分子
结肠炎
医学
溃疡性结肠炎
细胞因子
蛋白质C
内皮细胞活化
细胞间粘附分子-1
药理学
病理
凝血酶
内科学
疾病
血小板
作者
Franco Scaldaferri,Miquel Sans,Stefania Vetrano,C. Graziani,Raimondo De Cristofaro,Bruce Gerlitz,Alessandro Repici,Vincenzo Arena,Alberto Malesci,Julián Panés,Brian W. Grinnell,Silvio Danese
摘要
Endothelial protein C receptor (EPCR) and thrombomodulin (TM) are expressed at high levels in the resting microvasculature and convert protein C (PC) into its activated form, which is a potent anticoagulant and antiinflammatory molecule. Here we provide evidence that in Crohn disease (CD) and ulcerative colitis (UC), the 2 major forms of inflammatory bowel disease (IBD), there was loss of expression of endothelial EPCR and TM, which in turns caused impairment of PC activation by the inflamed mucosal microvasculature. In isolated human intestinal endothelial cells, administration of recombinant activated PC had a potent antiinflammatory effect, as demonstrated by downregulated cytokine-dependent cell adhesion molecule expression and chemokine production as well as inhibited leukocyte adhesion. In vivo, administration of activated PC was therapeutically effective in ameliorating experimental colitis as evidenced by reduced weight loss, disease activity index, and histological colitis scores as well as inhibited leukocyte adhesion to the inflamed intestinal vessels. The results suggest that the PC pathway represents a new system crucially involved in governing intestinal homeostasis mediated by the mucosal microvasculature. Restoring the PC pathway may represent a new therapeutic approach to suppress intestinal inflammation in IBD.
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