期刊
JOURNAL OF CELLULAR BIOCHEMISTRY
卷 115, 期 11, 页码 1928-1936出版社
WILEY-BLACKWELL
DOI: 10.1002/jcb.24864
关键词
NFkB P65; microRNA 155; ENDOTHELIAL INFLAMMATION; TNF
资金
- National Natural Science Foundation of China
- Guangdong Provincial Project of Science and Technology [81170272, 2011A030300010]
Increasing evidences have illuminated the fundamental role of inflammation in mediating all stages of atherosclerosis. miR-155, a typical multi-functional miRNA, has recently emerged as a novel component of inflammatory signal transduction in the pathogenesis of atherosclerosis. However, little is known about whether endothelial highly expressed miR-155 can regulate endothelial inflammation-related transcription factors and the predicted role of miR-155 as a negative feedback regulator in endothelial inflammation involved in atherosclerosis. Bioinformatics analysis showed that RELA (nuclear factor-B p65) is a potential target gene of miR-155 and this was confirmed by a luciferase reporter assay. Our results show that microRNA-155 mediate endothelial inflammation and decrease NFkB p65 and adhesion molecule expression in TNF-stimulated endothelial cells. Transfection with miR-155 significantly inhibited TNF-induced monocyte adhesion to endothelium. Inhibition of miR-155 enhanced p65 level and endothelial inflammatory response which was counteracted through the depletion of P65 by Si-P65. On the other hand, knockdown of eNOS, another target of miR-155, while transfecting with miR-155 inhibitor resulted in more significant inflammatory response. miR-155 is highly expressed in TNF treated HUVECs, deprived of endogenous p65 could reverse TNF-induced upregulation of miR-155. Thus, TNF induced miR-155 may serve as a negative feedback regulator in endothelial inflammation involved in atherosclerosis by targeting nuclear transcription factor P65. These results provide a rationale for intervention of intracellular microRNA as possible anti-atherosclerotic targets. J. Cell. Biochem. 115: 1928-1936, 2014. (c) 2014 Wiley Periodicals, Inc.
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