Literature DB >> 21062905

In silico QTL mapping of basal liver iron levels in inbred mouse strains.

Stela McLachlan1, Seung-Min Lee, Teresa M Steele, Paula L Hawthorne, Matthew A Zapala, Eleazar Eskin, Nicholas J Schork, Gregory J Anderson, Chris D Vulpe.   

Abstract

Both iron deficiency and iron excess are detrimental in many organisms, and previous studies in both mice and humans suggest that genetic variation may influence iron status in mammals. However, these genetic factors are not well defined. To address this issue, we measured basal liver iron levels in 18 inbred strains of mice of both sexes on a defined iron diet and found ∼4-fold variation in liver iron in males (lowest 153 μg/g, highest 661 μg/g) and ∼3-fold variation in females (lowest 222 μg/g, highest 658 μg/g). We carried out a genome-wide association mapping to identify haplotypes underlying differences in liver iron and three other related traits (copper and zinc liver levels, and plasma diferric transferrin levels) in a subset of 14 inbred strains for which genotype information was available. We identified two putative quantitative trait loci (QTL) that contain genes with a known role in iron metabolism: Eif2ak1 and Igf2r. We also identified four putative QTL that reside in previously identified iron-related QTL and 22 novel putative QTL. The most promising putative QTL include a 0.22 Mb region on Chromosome 7 and a 0.32 Mb region on Chromosome 11 that both contain only one candidate gene, Adam12 and Gria1, respectively. Identified putative QTL are good candidates for further refinement and subsequent functional studies.

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Year:  2010        PMID: 21062905      PMCID: PMC3055709          DOI: 10.1152/physiolgenomics.00025.2010

Source DB:  PubMed          Journal:  Physiol Genomics        ISSN: 1094-8341            Impact factor:   3.107


  67 in total

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4.  Genetic variation of basal iron status, ferritin and iron regulatory protein in mice: potential for modulation of oxidative stress.

Authors:  B Clothier; S Robinson; R A Akhtar; J E Francis; T J Peters; K Raja; A G Smith
Journal:  Biochem Pharmacol       Date:  2000-01-15       Impact factor: 5.858

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Review 6.  Balancing acts: molecular control of mammalian iron metabolism.

Authors:  Matthias W Hentze; Martina U Muckenthaler; Nancy C Andrews
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Review 7.  Haplotype association mapping in mice.

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Journal:  Methods Mol Biol       Date:  2009

8.  ADAM12 localizes with c-Src to actin-rich structures at the cell periphery and regulates Src kinase activity.

Authors:  Dorte Stautz; Archana Sanjay; Matilde Thye Hansen; Reidar Albrechtsen; Ulla M Wewer; Marie Kveiborg
Journal:  Exp Cell Res       Date:  2009-09-19       Impact factor: 3.905

9.  A novel association between a SNP in CYBRD1 and serum ferritin levels in a cohort study of HFE hereditary haemochromatosis.

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5.  Hamp1 mRNA and plasma hepcidin levels are influenced by sex and strain but do not predict tissue iron levels in inbred mice.

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6.  In silico QTL mapping of maternal nurturing ability with the mouse diversity panel.

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7.  In silico mapping of quantitative trait loci (QTL) regulating the milk ionome in mice identifies a milk iron locus on chromosome 1.

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8.  Brain iron accumulation affects myelin-related molecular systems implicated in a rare neurogenetic disease family with neuropsychiatric features.

Authors:  M Heidari; D M Johnstone; B Bassett; R M Graham; A C G Chua; M J House; J F Collingwood; C Bettencourt; H Houlden; M Ryten; J K Olynyk; D Trinder; E A Milward
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9.  Fine-mapping and genetic analysis of the loci affecting hepatic iron overload in mice.

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10.  Gene co-expression networks shed light into diseases of brain iron accumulation.

Authors:  Conceição Bettencourt; Paola Forabosco; Sarah Wiethoff; Moones Heidari; Daniel M Johnstone; Juan A Botía; Joanna F Collingwood; John Hardy; Elizabeth A Milward; Mina Ryten; Henry Houlden
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