• Title of article

    Iron responses in hepatic, intestinal and macrophage/monocyte cell lines under different culture conditions

  • Author/Authors

    Sandrine Jacolot، نويسنده , , Claude Ferec، نويسنده , , Catherine Mura، نويسنده ,

  • Issue Information
    روزنامه با شماره پیاپی سال 2008
  • Pages
    9
  • From page
    100
  • To page
    108
  • Abstract
    Iron homeostasis is mainly controlled by the liver-produced hepcidin peptide, which induces the degradation of the ferroportin iron exporter and thus regulates serum iron level. Hepcidin transcription is clearly up-regulated by the pro-inflammatory cytokine IL-6 and down-regulated, in the case of iron depletion, at least via HIF transcription factors. In addition, in vivo iron overload up-regulates hepcidin, but this cannot be reproduced in cell culture or isolated hepatocytes. Here, we investigated the steady state mRNA levels of a series of genes involved in iron metabolism in hepatic HepG2, intestinal Caco-2, and monocyte/macrophage THP-1 cell lines under different iron and culture conditions. Our results showed that iron-saturated transferrin up-regulated hepcidin mRNA synthesis from HepG2 via cross-talk with macrophages or enterocyte cytokine-producing cells, whereas non-transferrin-bound iron down-regulated hepcidin, likely due to missing TfR-iron-transferrin uptake.
  • Keywords
    quantitative RT-PCR , Iron responses , Holo-transferrin , NTBI , Cell culture conditions
  • Journal title
    Blood Cells, Molecules and Diseases
  • Serial Year
    2008
  • Journal title
    Blood Cells, Molecules and Diseases
  • Record number

    499339