@inproceedings{932337daa68a49f890ba67160bf0bf67,
title = "Hepcidin and Hfe in iron overload in β-thalassemia",
abstract = "Hepcidin (HAMP) negatively regulates iron absorption, degrading the iron exporter ferroportin at the level of enterocytes and macrophages. We showed that mice with β-thalassemia intermedia (th3+) have increased anemia and iron overload. However, their hepcidin expression is relatively low compared to their iron burden. We also showed that the iron metabolism gene Hfe is down-regulated in concert with hepcidin in th3+ mice. These observations suggest that low hepcidin levels are responsible for abnormal iron absorption in thalassemic mice and that down-regulation of Hfe might be involved in the pathway that controls hepcidin synthesis in β-thalassemia. Therefore, these studies suggest that increasing hepcidin andor Hfe expression could be a strategy to reduces iron overload in these animals. The goal of this paper is to review recent findings that correlate hepcidin, Hfe, and iron metabolism in β-thalassemia and to discuss potential novel therapeutic approaches based on these recent discoveries.",
keywords = "Hfe, hepcidin, iron overload, lentiviral vectors, β-thalassemia",
author = "Sara Gardenghi and Pedro Ramos and Antonia Follenzi and Niva Rao and Rachmilewitz, {Eliezer A.} and Giardina, {Patricia J.} and Grady, {Robert W.} and Stefano Rivella",
year = "2010",
month = aug,
doi = "10.1111/j.1749-6632.2010.05595.x",
language = "English",
isbn = "9781573317825",
series = "Annals of the New York Academy of Sciences",
publisher = "Blackwell Publishing Inc.",
pages = "221--225",
booktitle = "Cooley's Anemia",
}