Literature DB >> 14530973

SLC11 family of H+-coupled metal-ion transporters NRAMP1 and DMT1.

Bryan Mackenzie1, Matthias A Hediger.   

Abstract

NRAMP1 (natural resistance-associated macrophage protein-1) and DMT1 (divalent metal-ion transporter-1) make up the SLC11 gene family of metal-ion transporters that are energized by the H(+) electrochemical gradient. Long known to confer resistance to bacterial infection, NRAMP1 functions at the phagolysosomal membrane of macrophages and neutrophils. NRAMP1 most likely contributes to macrophage antimicrobial function by extruding essential metal ions (including Mn(2+)) from the phagolysosome via H(+)/metal-ion cotransport. An alternative hypothesis in the literature proposes that NRAMP1 concentrate Fe(2+) within the phagolysosome by means of H(+)/Fe(2+) antiport, resulting in the generation of toxic free radicals. DMT1 is expressed widely and accepts as substrates a broad range of transition metal ions, among which Fe(2+) is transported with high affinity ( K(0.5) approximately 2 microM). DMT1 accounts both for the intestinal absorption of free Fe(2+) and for transferrin-associated endosomal Fe(2+) transport in erythroid precursors and many other cell types. DMT1 is up-regulated dramatically in the intestine by dietary iron restriction and, despite high serum iron levels, is not appropriately down-regulated in hereditary hemochromatosis.

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Year:  2003        PMID: 14530973     DOI: 10.1007/s00424-003-1141-9

Source DB:  PubMed          Journal:  Pflugers Arch        ISSN: 0031-6768            Impact factor:   3.657


  81 in total

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Authors:  N Nelson; W R Harvey
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Authors:  Stephen A Harrison; Bruce R Bacon
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Authors:  X Z Chen; J B Peng; A Cohen; H Nelson; N Nelson; M A Hediger
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4.  Characterization of the iron transporter DMT1 (NRAMP2/DCT1) in red blood cells of normal and anemic mk/mk mice.

Authors:  F Canonne-Hergaux; A S Zhang; P Ponka; P Gros
Journal:  Blood       Date:  2001-12-15       Impact factor: 22.113

5.  Regulatory defects in liver and intestine implicate abnormal hepcidin and Cybrd1 expression in mouse hemochromatosis.

Authors:  Martina Muckenthaler; Cindy N Roy; Angel O Custodio; Belén Miñana; Jos deGraaf; Lynne K Montross; Nancy C Andrews; Matthias W Hentze
Journal:  Nat Genet       Date:  2003-05       Impact factor: 38.330

6.  Mechanism of increased iron absorption in murine model of hereditary hemochromatosis: increased duodenal expression of the iron transporter DMT1.

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Journal:  Proc Natl Acad Sci U S A       Date:  1999-03-16       Impact factor: 11.205

7.  Human natural resistance-associated macrophage protein 2: gene cloning and protein identification.

Authors:  F Kishi; M Tabuchi
Journal:  Biochem Biophys Res Commun       Date:  1998-10-29       Impact factor: 3.575

8.  Previously uncharacterized isoforms of divalent metal transporter (DMT)-1: implications for regulation and cellular function.

Authors:  Nadia Hubert; Matthias W Hentze
Journal:  Proc Natl Acad Sci U S A       Date:  2002-09-03       Impact factor: 11.205

9.  The human Nramp2 gene: characterization of the gene structure, alternative splicing, promoter region and polymorphisms.

Authors:  P L Lee; T Gelbart; C West; C Halloran; E Beutler
Journal:  Blood Cells Mol Dis       Date:  1998-06       Impact factor: 3.039

10.  Expression of the iron transporter DMT1 in kidney from normal and anemic mk mice.

Authors:  François Canonne-Hergaux; Philippe Gros
Journal:  Kidney Int       Date:  2002-07       Impact factor: 10.612

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  32 in total

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Review 4.  Recent advances in intestinal iron transport.

Authors:  Gregory J Anderson; David M Frazer
Journal:  Curr Gastroenterol Rep       Date:  2005-10

Review 5.  Iron metabolism in the eye: a review.

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6.  Identification of mouse SLC39A8 as the transporter responsible for cadmium-induced toxicity in the testis.

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7.  DMT1 (IRE) expression in intestinal and erythroid cells is regulated by peripheral benzodiazepine receptor-associated protein 7.

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8.  Genetic resistance of mice to Mycobacterium paratuberculosis is influenced by Slc11a1 at the early but not at the late stage of infection.

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