Adenine alleviates iron overload by cAMP/PKA mediated hepatic hepcidin in mice

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TitreAdenine alleviates iron overload by cAMP/PKA mediated hepatic hepcidin in mice
Type de publicationJournal Article
Year of Publication2018
AuteursZhang Y, Wang X, Wu Q, Wang H, Zhao L, Wang X, Mu M, Xie E, He X, Shao D, Shang Y, Lai Y, Ginzburg Y, Min J, Wang F
JournalJOURNAL OF CELLULAR PHYSIOLOGY
Volume233
Pagination7268-7278
Date PublishedSEP
Type of ArticleArticle
ISSN0021-9541
Mots-clésadenine, BMP, cAMP, hemochromatosis, Hepcidin, PKA pathway, smad pathway
Résumé

Hemochromatosis is prevalent and often associated with high rates of morbidity and mortality worldwide. The safe alternative iron-reducing approaches are urgently needed in order to better control iron overload. Our unbiased vitamin screen for modulators of hepcidin, a master iron regulatory hormone, identifies adenine (vitamin B4) as a potent hepcidin agonist. Adenine significantly induced hepcidin mRNA level and promoter activity activation in human cell lines, possibly through BMP/SMAD pathway. Further studies in mice validated the effect of adenine on hepcidin upregulation. Consistently, adenine dietary supplement in mice led to an increase of hepatic hepcidin expression compared with normal diet-fed mice via BMP/SMAD pathway. Notably, adenine-rich diet significantly ameliorated iron overload accompanied by the enhanced hepcidin expression in both high iron-fed mice and in Hfe(-/-) mice, a murine model of hereditary hemochromatosis. To further validate this finding, we selected pharmacological inhibitors against BMP (LDN193189). We found LDN193189 strongly blocked the hepcidin induction by adenine. Moreover, we uncovered an essential role of cAMP/PKA-dependent axis in triggering adenine-induced hepcidin expression in primary hepatocytes by using 8br cAMP, a cAMP analog, and H89, a potent inhibitor for PKA signaling. These findings suggest a potential therapeutic role of adenine for hereditary hemochromatosis.

DOI10.1002/jcp.26559