PLoS ONE (Jan 2013)

Copper deficiency leads to anemia, duodenal hypoxia, upregulation of HIF-2α and altered expression of iron absorption genes in mice.

  • Pavle Matak,
  • Sara Zumerle,
  • Maria Mastrogiannaki,
  • Souleiman El Balkhi,
  • Stephanie Delga,
  • Jacques R R Mathieu,
  • François Canonne-Hergaux,
  • Joel Poupon,
  • Paul A Sharp,
  • Sophie Vaulont,
  • Carole Peyssonnaux

DOI
https://doi.org/10.1371/journal.pone.0059538
Journal volume & issue
Vol. 8, no. 3
p. e59538

Abstract

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Iron and copper are essential trace metals, actively absorbed from the proximal gut in a regulated fashion. Depletion of either metal can lead to anemia. In the gut, copper deficiency can affect iron absorption through modulating the activity of hephaestin - a multi-copper oxidase required for optimal iron export from enterocytes. How systemic copper status regulates iron absorption is unknown. Mice were subjected to a nutritional copper deficiency-induced anemia regime from birth and injected with copper sulphate intraperitoneally to correct the anemia. Copper deficiency resulted in anemia, increased duodenal hypoxia and Hypoxia inducible factor 2α (HIF-2α) levels, a regulator of iron absorption. HIF-2α upregulation in copper deficiency appeared to be independent of duodenal iron or copper levels and correlated with the expression of iron transporters (Ferroportin - Fpn, Divalent Metal transporter - Dmt1) and ferric reductase - Dcytb. Alleviation of copper-dependent anemia with intraperitoneal copper injection resulted in down regulation of HIF-2α-regulated iron absorption genes in the gut. Our work identifies HIF-2α as an important regulator of iron transport machinery in copper deficiency.