Literature DB >> 9989781

Non-transferrin-bound iron uptake in Belgrade and normal rat erythroid cells.

L M Garrick1, K G Dolan, M A Romano, M D Garrick.   

Abstract

Belgrade (b) rats have an autosomal recessive, microcytic, hypochromic anemia. Transferrin (Tf)-dependent iron uptake is defective because of a mutation in DMT1 (Nramp2), blocking endosomal iron efflux. This experiment of nature permits the present study to address whether the mutation also affects non-Tf-bound iron (NTBI) uptake and to use NTBI uptake compared to Tf-Fe utilization to increase understanding of the phenotype of the b mutation. The distribution of 59Fe2+ into intact erythroid cells and cytosolic, stromal, heme, and nonheme fractions was different after NTBI uptake vs. Tf-Fe uptake, with the former exhibiting less iron into heme but more into stromal and nonheme fractions. Both reticulocytes and erythrocytes exhibit NTBI uptake. Only reticulocytes had heme incorporation after NTBI uptake. Properly normalized, incorporation into b/b heme was approximately 20% of +/b, a decrease similar to that for Tf-Fe utilization. NTBI uptake into heme was inhibited by bafilomycin A1, concanamycin, NH4Cl, or chloroquine, consistent with the endosomal location of the transporter; cellular uptake was uninhibited. NTBI uptake was unaffected after removal of Tf receptors by Pronase or depletion of endogenous Tf. Concentration dependence revealed that NTBI uptake into cells, cytosol, stroma, and the nonheme fraction had an apparent low affinity for iron; heme incorporation behaved like a high-affinity process, as did an expression assay for DMT1. DMT1 serves in both apparent high-affinity NTBI membrane transport and the exit of iron from the endosome during Tf delivery of iron in rat reticulocytes; the low-affinity membrane transporter, however, exhibits little dependence on DMT1.

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Year:  1999        PMID: 9989781     DOI: 10.1002/(SICI)1097-4652(199903)178:3<349::AID-JCP9>3.0.CO;2-R

Source DB:  PubMed          Journal:  J Cell Physiol        ISSN: 0021-9541            Impact factor:   6.384


  21 in total

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Journal:  Biochim Biophys Acta       Date:  2011-08-09

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Authors:  Michael D Garrick; Hung-Chieh Kuo; Farida Vargas; Steven Singleton; Lin Zhao; Jaime J Smith; Prasad Paradkar; Jerome A Roth; Laura M Garrick
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Review 4.  Influence of iron metabolism on manganese transport and toxicity.

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5.  Divalent metal-ion transporter DMT1 mediates both H+ -coupled Fe2+ transport and uncoupled fluxes.

Authors:  Bryan Mackenzie; M L Ujwal; Min-Hwang Chang; Michael F Romero; Matthias A Hediger
Journal:  Pflugers Arch       Date:  2005-08-10       Impact factor: 3.657

6.  Soluble nickel interferes with cellular iron homeostasis.

Authors:  Todd Davidson; Haobin Chen; Michael D Garrick; Gisela D'Angelo; Max Costa
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Review 7.  Manganese flux across the blood-brain barrier.

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8.  Abnormal iron metabolism in fibroblasts from a patient with the neurodegenerative disease hereditary ferritinopathy.

Authors:  Ana G Barbeito; Thierry Levade; Marie B Delisle; Bernardino Ghetti; Ruben Vidal
Journal:  Mol Neurodegener       Date:  2010-11-10       Impact factor: 14.195

9.  Glucose metabolism in the Belgrade rat, a model of iron-loading anemia.

Authors:  Xuming Jia; Jonghan Kim; Tania Veuthey; Chih-Hao Lee; Marianne Wessling-Resnick
Journal:  Am J Physiol Gastrointest Liver Physiol       Date:  2013-04-18       Impact factor: 4.052

Review 10.  Liver iron transport.

Authors:  Ross-M Graham; Anita-C-G Chua; Carly-E Herbison; John-K Olynyk; Debbie Trinder
Journal:  World J Gastroenterol       Date:  2007-09-21       Impact factor: 5.742

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