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Interleukin-1β Induces Increased Transcriptional Activation of the Transforming Growth Factor-β-activating Integrin Subunit β8 through Altering Chromatin Architecture

The integrin αvβ8 is a cell surface receptor for the latent domain (LAP) of the multifunctional cytokine TGF-β. Through its association with LAP, TGF-β is maintained in a latent form that must be activated to function. Binding to the integrin αvβ8 with subsequent metalloproteolytic cleavage of LAP r...

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Bibliographic Details
Published in:The Journal of biological chemistry 2011-10, Vol.286 (42), p.36864-36874
Main Authors: Markovics, Jennifer A., Araya, Jun, Cambier, Stephanie, Somanath, Sangeeta, Gline, Stephanie, Jablons, David, Hill, Arthur, Wolters, Paul J., Nishimura, Stephen L.
Format: Article
Language:English
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Summary:The integrin αvβ8 is a cell surface receptor for the latent domain (LAP) of the multifunctional cytokine TGF-β. Through its association with LAP, TGF-β is maintained in a latent form that must be activated to function. Binding to the integrin αvβ8 with subsequent metalloproteolytic cleavage of LAP represents a major mechanism of TGF-β activation in vivo. Altered expression of the integrin β8 subunit (ITGB8) is found in human chronic obstructive pulmonary disease, cancers, and brain vascular malformations. We have previously shown that the proinflammatory cytokine interleukin-1β (IL-1β) increases ITGB8 expression on lung fibroblasts, which increases αvβ8-mediated TGF-β activation in fibrosis and pathologic inflammation. Here we report the mechanism of increased ITGB8 expression by IL-1β. Our data support a model where the chromatin architecture of the ITGB8 core promoter is altered by nucleosomal repositioning that enhances the interaction of an AP1 complex (containing c-Jun and ATF2). This repositioning is caused by the dissociation of HDAC2 with the ITGB8 core promoter, leading to increased histone H4 acetylation and a loosening of nucleosomal-DNA interactions allowing “opening” of the chromatin structure and increased association of c-Jun and ATF-2. These changes are mediated through NFκB- and p38-dependent pathways. Ultimately, these events culminate in increasing ITGB8 transcription, αvβ8 surface expression, and αvβ8-mediated TGFβ activation. Background: IL-1β acts on fibroblasts inducing TGF-β-dependent profibrogenic responses. Results: IL-1β increases expression of the TGF-β-activating integrin β8 subunit through altering nucleosomal positioning at the ITGB8 promoter. Conclusion: IL-1β increases accessibility of transcription factors to the ITGB8 promoter in lung fibroblasts through chromatin remodeling. Significance: This provides evidence for chromatin architectural changes mediating IL-1β profibrotic programs.
ISSN:0021-9258
1083-351X
DOI:10.1074/jbc.M111.276790