• Title of article

    Novel mutation in ferroportin 1 gene is associated with autosomal dominant iron overload

  • Author/Authors

    Anne-Marie Jouanolle، نويسنده , , Véronique Douabin-Gicquel، نويسنده , , Chantal Halimi، نويسنده , , Olivier Loreal ، نويسنده , , Patricia Fergelot، نويسنده , , Thierry Delacour، نويسنده , , Anne-Sophie de Lajarte-Thirouard، نويسنده , , Bruno Turlin، نويسنده , , Jean-Yves Le Gall، نويسنده , , Estelle Cadet، نويسنده , , Jacques Rochette، نويسنده , , Veronique David، نويسنده , , Pierre Brissot، نويسنده ,

  • Issue Information
    روزنامه با شماره پیاپی سال 2003
  • Pages
    4
  • From page
    286
  • To page
    289
  • Abstract
    We report a family affected with dominant autosomal iron overload related to a new mutation in ferroportin 1, a transmembrane protein involved in the export of iron from duodenal enterocytes and likely from macrophages. The originality of this family is represented by the nature of the mutation consisting in the replacement of glycine 490 with aspartate. Clinicians should be aware of this novel iron overload entity, which corresponds to a particular phenotypic expression (high serum ferritin values contrasting with relatively low transferring saturation, and important Kupffer cell iron deposition as compared to hepatocytic iron excess) with poor tolerance of venesection therapy and a dominant pattern of inheritance. Given this dominant transmission, the mixed Causasian–Asian origin of our Asian proband leaves open the issue of the ethnic origin of the new mutation.
  • Keywords
    Ferroportin , Ferritin , Hemochromatosis , Kupffer cell , Venesection therapy , Dominant transmission , Iron overload , SLC11A3 gene
  • Journal title
    Journal of Hepatology
  • Serial Year
    2003
  • Journal title
    Journal of Hepatology
  • Record number

    585884