| Literature DB >> 25241290 |
Maura Poli1, Michela Asperti1, Paola Ruzzenenti1, Luca Mandelli2, Natascia Campostrini3, Giuliana Martini4, Margherita Di Somma1, Federica Maccarinelli1, Domenico Girelli3, Annamaria Naggi2, Paolo Arosio5.
Abstract
Hepcidin is a peptide hormone that controls systemic iron availability and is upregulated by iron and inflammation. Heparins have been shown to be efficient hepcidin inhibitors both in vitro and in vivo, even when their anticoagulant activity has been abolished by chemical reactions of oxidation/reduction (glycol-split). We analyzed a modified heparin type, characterized by a high, almost saturated, sulfation degree and low molecular weight. It inhibited hepcidin expression in hepatic HepG2 cells, and when used in mice, it readily suppressed liver hepcidin mRNA and serum hepcidin, with a significant decrease of spleen iron. This occurred also in inflammation-model, LPS-treated animals, and after heparin chronic 10-day treatments. The heparin had low/absent anticoagulant activity, as tested for factor-Xa and -IIA, APTT and anti Xa. It reduced triglyceride levels in the mice. This heparin acts faster and is more potent than the glycol split-heparins, probably because of its smaller molecular weight and higher sulfation degree. This modified heparin has potential applications for the treatment of diseases with high hepcidin levels.Entities:
Keywords: Anemia of chronic diseases; Hepcidin; Iron absorption and metabolism; Low-molecular-weight heparins
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Year: 2014 PMID: 25241290 DOI: 10.1016/j.bcp.2014.09.007
Source DB: PubMed Journal: Biochem Pharmacol ISSN: 0006-2952 Impact factor: 5.858