Journal
CIRCULATION RESEARCH
Volume 102, Issue 7, Pages 823-830Publisher
LIPPINCOTT WILLIAMS & WILKINS
DOI: 10.1161/CIRCRESAHA.107.165332
Keywords
calcineurin; complement; endothelium; histone deacetylase; inflammation; interleukin-1
Funding
- NHLBI NIH HHS [HL52297, R37 HL052297, R01 HL052297] Funding Source: Medline
- NIAID NIH HHS [R01 AI053733, AI53733] Funding Source: Medline
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Activation of complement stimulates inflammation and provides an initial vigorous defense against infection. Insertion of the membrane attack complex in cell membranes of vascular endothelial cells induces changes in cell differentiation that promote coagulation, thrombosis, inflammation, and immunity. These changes are mediated by production of interleukin (IL)-1 alpha by endothelial cells, which acts locally on endothelial cells to contain infection and promote healing of the affected site. In healthy tissues, however, promoting coagulation and inflammation would be dysphysiologic. Accordingly, endothelial cell activation by the membrane attack complex depends on both transcriptional regulation of IL-1 alpha and availability of that cytokine to broadly modify endothelial cell physiology. Here, we report that the IL-1 alpha gene contains a suppressor sequence that cooperates with histone modification to regulate production of IL-1 alpha by endothelial cells. The suppressor sequence binds C/EBP (CCAAT enhancer-binding protein) family DNA-binding proteins isolated from the nucleus of quiescent endothelial cells. These results suggest constitutive suppression of IL-1 alpha maintains quiescence of endothelium and that terminal complement complexes remove that suppression, allowing IL-1 alpha transcription and, ultimately, activation of endothelium to proceed.
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