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Publication : Expression of the DMT1 (NRAMP2/DCT1) iron transporter in mice with genetic iron overload disorders.

First Author  Canonne-Hergaux F Year  2001
Journal  Blood Volume  97
Issue  4 Pages  1138-40
PubMed ID  11159549 Mgi Jnum  J:67402
Mgi Id  MGI:1930475 Doi  10.1182/blood.v97.4.1138
Citation  Canonne-Hergaux F, et al. (2001) Expression of the DMT1 (NRAMP2/DCT1) iron transporter in mice with genetic iron overload disorders. Blood 97(4):1138-40
abstractText  Iron overload is highly prevalent, but its molecular pathogenesis is poorly understood. Recently, DMT1 was shown to be a major apical iron transporter in absorptive cells of the duodenum. In vivo, it is the only transporter known to be important for the uptake of dietary non-heme iron from the gut lumen. The expression and subcellular localization of DMT1 protein in 3 mouse models of iron overload were examined: hypotransferrinemic (Trf(hpx)) mice, Hfe knockout mice, and B2m knockout mice. Interestingly, in Trf(hpx) homozygotes, DMT1 expression was strongly induced in the villus brush border when compared to control animals. This suggests that DMT1 expression is increased in response to iron deficiency in the erythron, even in the setting of systemic iron overload. In contrast, no increase was seen in DMT1 expression in animals with iron overload resembling human hemochromatosis. Therefore, it does not appear that changes in DMT1 levels are primarily responsible for iron loading in hemochromatosis.
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