Literature DB >> 7887888

Both nuclear and mitochondrial cytochrome c oxidase mRNA levels increase dramatically during mouse postnatal development.

K Kim1, A Lecordier, L H Bowman.   

Abstract

The steady-state levels of 13 of 16 cytochrome c oxidase (COX) mRNAs and mitochondrial DNA were measured during the postnatal development of mouse skeletal muscle, ventricle, kidney and brain as well as during the differentiation of mouse myoblasts into myofibres in cell culture. These experiments indicate that large co-ordinated increases in COX mRNA levels and isoform switching are important for the elaboration of this enzyme during postnatal development and demonstrate the importance of gene-regulatory mechanisms in controlling COX activity. On a per nucleus basis, the levels of the mitochondrial- and most nuclear-encoded COX mRNAs co-ordinately increase 3-10-fold during postnatal development, with the highest levels obtained in ventricle and skeletal muscle. However, concentrations of mitochondrial and nuclear COX mRNAs remain constant during the differentiation of myoblasts into fibres in cell culture. A gradual change from the liver to the heart isoform of COX subunit VIa mRNA occurs during postnatal development of skeletal muscle and ventricle and is nearly complete 3 days after the formation of myofibres in cell culture. Mitochondrial DNA increases proportionally with COX mRNAs during mouse postnatal development but not during myoblast differentiation in cell culture, in which mitochondrial DNA levels increase 5-fold and mitochondrial mRNA levels remain constant. This suggests that mitochondrial DNA replication may control mitochondrial RNA concentrations during postnatal development but not during myoblast differentiation in cell culture.

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Year:  1995        PMID: 7887888      PMCID: PMC1136528          DOI: 10.1042/bj3060353

Source DB:  PubMed          Journal:  Biochem J        ISSN: 0264-6021            Impact factor:   3.857


  44 in total

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5.  Cloning of mouse mitochondrial DNA in E. coli affects bacterial viability.

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Journal:  Exp Cell Res       Date:  1981-12       Impact factor: 3.905

7.  Multiple ribosomal RNA cleavage pathways in mammalian cells.

Authors:  L H Bowman; B Rabin; D Schlessinger
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8.  Coordinate reciprocal trends in glycolytic and mitochondrial transcript accumulations during the in vitro differentiation of human myoblasts.

Authors:  K A Webster; P Gunning; E Hardeman; D C Wallace; L Kedes
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9.  NRF-1: a trans-activator of nuclear-encoded respiratory genes in animal cells.

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  20 in total

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Review 5.  Mitochondrial biogenesis in the liver during development and oncogenesis.

Authors:  J M Cuezva; L K Ostronoff; J Ricart; M López de Heredia; C M Di Liegro; J M Izquierdo
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7.  Quantitative Proteomics of Presynaptic Mitochondria Reveal an Overexpression and Biological Relevance of Neuronal MitoNEET in Postnatal Brain Development.

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Review 8.  Regulation of myoglobin expression.

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9.  Induced pluripotent stem cells generated from diabetic patients with mitochondrial DNA A3243G mutation.

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10.  Alpha-actinin 4 and BAT1 interaction with the cytochrome c promoter upon skeletal muscle differentiation.

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