Literature DB >> 17620357

Slc11a1, formerly Nramp1, is expressed in dendritic cells and influences major histocompatibility complex class II expression and antigen-presenting cell function.

Carmel B Stober1, Sven Brode, Jacqueline K White, Jean-François Popoff, Jenefer M Blackwell.   

Abstract

Solute carrier family 11 member a1 (Slc11a1; formerly Nramp1) encodes a late endosomal/lysosomal protein/divalent cation transporter that regulates iron homeostasis in macrophages. During macrophage activation, Slc11a1 has multiple pleiotropic effects on gene regulation and function, including gamma interferon-induced class II expression and antigen-presenting cell function. The wild-type allele at Slc11a1 has been associated with a bias in Th1 cell function in vivo, which is beneficial in resistance to infection against intracellular macrophage pathogens but detrimental in contributing to development of type 1 diabetes. The extent to which this depends on macrophage versus dendritic cell (DC) function is not known. Here we show that Slc11a1 is expressed in late endosomes and/or lysosomes of CD11c(+) DCs. DCs from mutant and congenic wild-type mice upregulate interleukin-12 (IL-12) and IL-10 mRNA in response to lipopolysaccharide (LPS) stimulation, but the ratio of IL-10 to IL-12 is higher in unstimulated DCs and DCs stimulated for 15 h with LPS from mutant mice than from wild-type mice. DCs from wild-type mice upregulate major histocompatibility complex class II in response to LPS more efficiently than DCs from mutant mice. Unstimulated DCs from wild-type and mutant mice present ovalbumin (OVA) peptide with an efficiency equivalent to that of an OVA-specific CD4 T-cell line, but DCs from wild-type mice are more efficient at processing and presenting OVA or Leishmania activator of cell kinase (LACK) protein to OVA- and LACK-specific T cells. These data indicate that wild-type Slc11a1 expressed in DCs may play a role both in determining resistance to infectious disease and in susceptibility to autoimmune disease such as type 1 diabetes.

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Year:  2007        PMID: 17620357      PMCID: PMC2044529          DOI: 10.1128/IAI.00153-07

Source DB:  PubMed          Journal:  Infect Immun        ISSN: 0019-9567            Impact factor:   3.441


  51 in total

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Authors:  L Esposito; N J Hill; L E Pritchard; F Cucca; C Muxworthy; M E Merriman; A Wilson; C Julier; M Delepine; J Tuomilehto; E Tuomilehto-Wolf; C Ionesco-Tirgoviste; L Nistico'; R Buzzetti; P Pozzilli; M Ferrari; E Bosi; F Pociot; J Nerup; S C Bain; J A Todd
Journal:  Diabetes       Date:  1998-11       Impact factor: 9.461

3.  Ectopic expression of Nramp1 in COS-1 cells modulates iron accumulation.

Authors:  P G Atkinson; C H Barton
Journal:  FEBS Lett       Date:  1998-03-27       Impact factor: 4.124

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Authors:  S Searle; N A Bright; T I Roach; P G Atkinson; C H Barton; R H Meloen; J M Blackwell
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10.  Genetic control of immune response to recombinant antigens carried by an attenuated Salmonella typhimurium vaccine strain: Nramp1 influences T-helper subset responses and protection against leishmanial challenge.

Authors:  S S Soo; B Villarreal-Ramos; C M Anjam Khan; C E Hormaeche; J M Blackwell
Journal:  Infect Immun       Date:  1998-05       Impact factor: 3.441

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  25 in total

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Review 6.  Genetics-squared: combining host and pathogen genetics in the analysis of innate immunity and bacterial virulence.

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7.  Genetic interactions among Idd3, Idd5.1, Idd5.2, and Idd5.3 protective loci in the nonobese diabetic mouse model of type 1 diabetes.

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8.  Mycobacterium avium subsp. paratuberculosis as a trigger of type-1 diabetes: destination Sardinia, or beyond?

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Review 9.  Intracellular microbes and haemophagocytosis.

Authors:  Eugenia Silva-Herzog; Corrella S Detweiler
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10.  CXCR1 and SLC11A1 polymorphisms affect susceptibility to cutaneous leishmaniasis in Brazil: a case-control and family-based study.

Authors:  Léa Castellucci; Sarra E Jamieson; E Nancy Miller; Eliane Menezes; Joyce Oliveira; Andrea Magalhães; Luiz Henrique Guimarães; Marcus Lessa; Amélia Ribeiro de Jesus; Edgar M Carvalho; Jenefer M Blackwell
Journal:  BMC Med Genet       Date:  2010-01-20       Impact factor: 2.103

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