Hepcidin, a candidate modifier of the hemochromatosis phenotype in mice

Abstract

Hereditary hemochromatosis (HH) type I is a disorder of iron metabolism caused by a mutation in the HFE gene. Whereas the prevalence of the mutation is very high, its penetrance seems very low. The goal of our study was to determine whether hepcidin, a recently identified iron-regulatory peptide, could be a genetic modifier contributing to the HH phenotype. In mice, deficiency of either HFE (Hfe^-/-) or hepcidin (Usf2^-/-) is associated with the same pattern of iron overload observed in patients with HH. We intercrossed Hfe^-/- and Usf2^+/- mice and asked whether hepcidin deficiency increased the iron burden in Hfe^-/- mice. Our results showed that, indeed, liver iron accumulation was greater in the Hfe^-/-Usf2^+/- mice than in mice lacking Hfe alone. This result, in agreement with recent findings in humans, provides a genetic explanation for some variability of the HH phenotype. (Blood. 2004;103: 2841-2843)