Under normal conditions, iron is taken up by the cells through the transferrin-mediated pathway. However, in hereditary hemochromatosis, a common iron-overloading disorder associated with mutations in the HFE gene, iron in plasma exceeds transferrin-binding capacity, and non-transferrin-bound iron (NTBI) appears in the circulation of patients with iron overload. NTBI can be taken up by hepatocytes through a transferrin-independent pathway. Lipocalin 2 (Lcn2), a secreted protein of the lipocalin family, has emerged as the mediator of an alternative, transferrin-independent pathway for cellular iron delivery. To evaluate the importance of Lcn2 in the pathogenesis of hepatic iron loading in Hfe knockout mice, we generated HfeLcn2 double-deficient mice. Our studies revealed that deletion of Lcn2 in Hfe-knockout mice does not influence hepatic iron accumulation in Hfe(-/-) mice, or their response to iron loading, as the phenotype of HfeLcn2(-/-) mice remained indistinguishable from that of Hfe(-/-) mice.Lcn2 is not essential for iron delivery to hepatocytes in hemochromatosis.
Manfred Nairz, Igor Theurl, Andrea Schroll, Milan Theurl, Gernot Fritsche, Ewald Lindner, Markus Seifert, Marie-Laure Crouch, Klaus Hantke, Akira Shizuo, Ferric C. Fang, Günter Weiß
Øyvind Halaas, Magnus Steigedal, Markus Haug, Jane Atesoh Awuh, Liv Ryan, Andreas Brech, Shintaro Sato, Harald Husebye, Gerard A. Cangelosi, Akira Shizuo, Roland K. Strong, Terje Espevik, Trude H. Flo
Andreas Geier, Michael Josef Reugels, Ralf Weiskirchen, Hermann E. Wasmuth, Christoph G. Dietrich, Elmar Siewert, Carsten Gartung, Johann Lorenzen, Anja‐Katrin Bosserhoff, M. Brügmann, Axel M. Gressner, Siegfried Matern, Frank Lammert
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