20立方厘米
白细胞介素8
CXCL10型
趋化因子
CXCL1型
MAPK/ERK通路
CCL5
CXCL11型
p38丝裂原活化蛋白激酶
细胞因子
细胞生物学
癌症研究
生物
信号转导
化学
分子生物学
炎症
免疫学
趋化因子受体
免疫系统
白细胞介素2受体
T细胞
作者
Jimmy W. Lee,Ping Wang,Michael G. Kattah,Sawsan Youssef,Lawrence Steinman,Kathryn DeFea,Daniel S. Straus
出处
期刊:Journal of Immunology
[American Association of Immunologists]
日期:2008-11-01
卷期号:181 (9): 6536-6545
被引量:130
标识
DOI:10.4049/jimmunol.181.9.6536
摘要
The IL-23/IL-17 pathway plays an important role in chronic inflammatory diseases, including inflammatory bowel disease. In inflammatory bowel disease, intestinal epithelial cells are an important source of chemokines that recruit inflammatory cells. We examined the effect of IL-17 on chemokine expression of HT-29 colonic epithelial cells. IL-17 strongly repressed TNF-alpha-stimulated expression of CXCL10, CXCL11, and CCL5, but synergized with TNF-alpha for induction of CXCL8, CXCL1, and CCL20 mRNAs. For CXCL10, IL-17 strongly inhibited promoter activity but had no effect on mRNA stability. In contrast, for CXCL8, IL-17 slightly decreased promoter activity but stabilized its normally unstable mRNA, leading to a net increase in steady-state mRNA abundance. IL-17 synergized with TNF-alpha in transactivating the epidermal growth factor receptor (EGFR) and in activating ERK and p38 MAPK. The p38 and ERK pathway inhibitors SB203580 and U0126 reversed the repressive effect of IL-17 on CXCL10 mRNA abundance and promoter activity and also reversed the inductive effect of IL-17 on CXCL8 mRNA, indicating that MAPK signaling mediates both the transcriptional repression of CXCL10 and the stabilization of CXCL8 mRNA by IL-17. The EGFR kinase inhibitor AG1478 partially reversed the effects of IL-17 on CXCL8 and CXCL10 mRNA, demonstrating a role for EGFR in downstream IL-17 signaling. The overall results indicate a positive effect of IL-17 on chemokines that recruit neutrophils (CXCL8 and CXCL1), and Th17 cells (CCL20). In contrast, IL-17 represses expression of CXCL10, CXCL11, and CCR5, three chemokines that selectively recruit Th1 but not other effector T cells.
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