Literature DB >> 19131261

Retained features of embryonic metabolism in the adult MRL mouse.

Robert K Naviaux1, Thuy P Le, Khamilia Bedelbaeva, John Leferovich, Dmitri Gourevitch, Pawel Sachadyn, Xiang-Ming Zhang, Lise Clark, Ellen Heber-Katz.   

Abstract

The MRL mouse is an inbred laboratory strain that was derived by selective breeding in 1960 from the rapidly growing LG/J (Large) strain. MRL mice grow to nearly twice the size of other commonly used mouse strains, display uncommonly robust healing and regeneration properties, and express later onset autoimmune traits similar to Systemic Lupus Erythematosis. The regeneration trait (heal) in the MRL mouse maps to 14-20 quantitative trait loci and the autoimmune traits map to 5-8 loci. In this paper we report the metabolic and biochemical features that characterize the adult MRL mouse and distinguish it from C57BL/6 control animals. We found that adult MRL mice have retained a number of features of embryonic metabolism that are normally lost during development in other strains. These include an emphasis on aerobic glycolytic energy metabolism, increased glutamate oxidation, and a reduced capacity for fatty acid oxidation. MRL tissues, including the heart, liver, and regenerating ear hole margins, showed considerable mitochondrial genetic and physiologic reserve, decreased mitochondrial transmembrane potential (DeltaPsi(m)), decreased reactive oxygen species (ROS), and decreased oxidative phosphorylation, yet increased mitochondrial DNA and protein content. The discovery of embryonic metabolic features led us to look for cells that express markers of embryonic stem cells. We found that the adult MRL mouse has retained populations of cells that express the stem cell markers Nanog, Islet-1, and Sox2. These are present in the heart at baseline and highly induced after myocardial injury. The retention of embryonic features of metabolism in adulthood is rare in mammals. The MRL mouse provides a unique experimental window into the relationship between metabolism, stem cell biology, and regeneration.

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Year:  2009        PMID: 19131261      PMCID: PMC3646557          DOI: 10.1016/j.ymgme.2008.11.164

Source DB:  PubMed          Journal:  Mol Genet Metab        ISSN: 1096-7192            Impact factor:   4.797


  52 in total

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Review 2.  From embryonic stem cells to blastema and MRL mice.

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3.  Differences in reactive oxygen species production explain the phenotypes associated with common mouse mitochondrial DNA variants.

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4.  Evaluation of assays for the measurement of bovine neutrophil reactive oxygen species.

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5.  Heart regeneration in adult MRL mice.

Authors:  J M Leferovich; K Bedelbaeva; S Samulewicz; X M Zhang; D Zwas; E B Lankford; E Heber-Katz
Journal:  Proc Natl Acad Sci U S A       Date:  2001-08-07       Impact factor: 11.205

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9.  Autoimmune glomerulonephritis induced in congenic mouse strain carrying telomeric region of chromosome 1 derived from MRL/MpJ.

Authors:  O Ichii; A Konno; N Sasaki; D Endoh; Y Hashimoto; Y Kon
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  36 in total

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2.  Role of reactive oxygen species in hyperadrenergic hypertension: biochemical, physiological, and pharmacological evidence from targeted ablation of the chromogranin a (Chga) gene.

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5.  Drug-induced regeneration in adult mice.

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6.  Protein expression profiling in head fragments during planarian regeneration after amputation.

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Review 8.  Inflammation and Its Correlates in Regenerative Wound Healing: An Alternate Perspective.

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Review 9.  Drug delivery and epimorphic salamander-type mouse regeneration: A full parts and labor plan.

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10.  Proteomic analysis of blastema formation in regenerating axolotl limbs.

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Journal:  BMC Biol       Date:  2009-11-30       Impact factor: 7.431

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