Divalent metal transporter-1 (DMT1/DCT1/Nramp2) is the major Fe2 transporter mediating cellular iron uptake in mammals. Phenotypic
analyses of animals with
spontaneous mutations in DMT1 indicate that it functions at two distinct sites, transporting dietary iron across the apical membrane of intestinal absorptive cells, and transporting endosomal iron released from transferrin into the cytoplasm of erythroid precursors. DMT1 also acts as a proton-dependent
transporter for other heavy metal ions including Mn2, Co2, and Cu2, but not for Mg2 or Ca2. A unique mutation in DMT1, G185R, has occurred spontaneously on two occasions in microcytic (mk) mice and once in Belgrade (b) rats. This mutation severely impairs the iron transport capability of DMT1, leading to systemic iron deficiency and anemia. The repeated occurrence of the G185R mutation cannot readily be explained by hypermutability of the gene. Here we show that G185R mutant DMT1 exhibits a new, constitutive Ca2 permeability, suggesting a gain of function that contributes to remutation and the mk and b phenotypes.