Congenital deficiency of two polypeptide subunits of the iron-protein fragment of mitochondrial complex I.

Moreadith, Randall W.; Cleeter, M. W. J.; Ragan, C I; Batshaw, Mark L.; Lehninger, Albert L.

doi:10.1172/jci112834

Cited by 43 publications

(12 citation statements)

References 20 publications

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“…Low concentrations of all immunoreactive peptides of complex I have been found in other cases of complex I deficiency (14,15). However, several cases have been reported in which one or more individual subunit could not be detected; Moreadith et al (13) demonstrated lack of the 75-kD (nuclear coded) and 1 3-kD (nuclear coded) subunits, and Schapira et al (15) found a deficiency of the 24 kD FeS-protein (nuclear coded). There are several possible explanations for the severe deficiency of complex I and the less severe deficiencies of complexes III and IV.…”

Section: Resultsmentioning

confidence: 99%

“…Investigation of complex I deficiency has concentrated on identifying the defective subunit or subunits by electron paramagnetic resonance spectroscopy (7), Western blotting (13,14,15), and analysis of the mitochondrial genome (16). There have, however, been no investigations of the secondary effects of complex I deficiency on other metabolic pathways.…”

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Impaired mitochondrial beta-oxidation in a patient with an abnormality of the respiratory chain. Studies in skeletal muscle mitochondria.

Watmough

Bindoff²,

Birch‐Machin³

et al. 1990

J. Clin. Invest.

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Defects of complex I of the mitochondrial respiratory chain are important causes of neurological disease. We report studies that demonstrate a severe deficiency of complex I activity with less severe abnormalities of complexes III and IV (< 5, 63, and 30% of control values, respectively) in a skeletal muscle mitochondrial fraction from a 22-yr-old female with weakness, lactic acidemia, and the deposition of intramuscular neutral lipid. The observation that lipid accumulates in this and other patients with complex I deficiency suggests impaired mitochondrial fatty acid oxidation. To investigate this mechanism we have shown impaired flux through ft-oxidation ([U-"Cjhexadecanoate oxidation was 66% of control rate) and accumulation of specific acyl-CoA ester intermediates. The changes in fatty acid metabolism in complex I deficiency are secondary to the reduced state within the mitochondrial matrix with low NAD+/NADH ratios. (J. Clin. Invest. 1990. 85:177-184.) ,Boxidation -complex I * mitochondria

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Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Impaired mitochondrial beta-oxidation in a patient with an abnormality of the respiratory chain. Studies in skeletal muscle mitochondria.

Watmough

Bindoff²,

Birch‐Machin³

et al. 1990

J. Clin. Invest.

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“…In 19 biochemically characterized cases which fit our definition of LIMD, the mean age of onset was 3 weeks, with death occurring on the average at 5 months and associated with overwhelming lactic acidosis Rimoldi et al, 1982;Sengers et al, 1984;Bresolin et al, 1985;DiMauro et al , 1980;Heiman-Patterson et al, 1982;Moreadith et al , 1984Moreadith et al , , 1987Boustany et al , 1983;Aprille, 1985;Van Biervliet et al, 1977;Stansbie et al, 1982;Minchom et al, 1983;Muller-Hocker et al, 1983;Trijbels et al , 1983;Robinson et al, 1985Robinson et al, , 1986Zheng et al, 1989). While the clinical course was similar in all cases, only a few patients had a multiorgan pathological or biochemical assessment which could evaluate the extent of tissue dysfunction.…”

Section: Lethal Infantile Mitochondrial Disease (Limo)mentioning

confidence: 93%

“…Case IV, DiMauro et al (1980). Case V, Moreadith et al (1984Moreadith et al ( , 1987. Case VI, Zheng et al (1989).…”

Section: Lethal Infantile Mitochondrial Disease (Limo)mentioning

confidence: 99%

Oxidative Phosphorylation Diseases

Shoffner

Wallace

1990

Advances in Human Genetics

246

157

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“…The physical mapping data for NDUFA5 exclude it as a candidate gene for WPW and DFN4, which map telomeric and centromeric of NDUFA5, respectively. Moreadith et al (1987) have described a patient with cardiomyopathy who lacks mature 75 and 13-kDa subunits of complex I according to Western blot data. Thus the results and materials reported in this study provide the necessary genetic tools to define the possible role of NDUFA5 in human disease.…”

Section: Introductionmentioning

confidence: 99%

Genomic organization of the human complex I 13-kDa subunit gene NDUFA5

Tensing

Pata²,

Wittig³

et al. 1999

Cytogenet Genome Res

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We have characterized the human gene NDUFA5 encoding a 13-kDa subunit of the mitochondrial respiratory chain complex I (NADH: ubiquinone oxidoreductase). The gene contains 5 exons and 4 introns, and spans 14 kb of genomic DNA. In the untranscribed region we observed potential transcription factor binding sites. We determined a single nucleotide variant (C/T) at –318, and its frequency in the German population. The functional gene was localised by FISH to 7q31 and by radiation hybrid panel near marker D7S648 in YAC 883_a_2.

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Congenital deficiency of two polypeptide subunits of the iron-protein fragment of mitochondrial complex I.

Cited by 43 publications

References 20 publications

Impaired mitochondrial beta-oxidation in a patient with an abnormality of the respiratory chain. Studies in skeletal muscle mitochondria.

Impaired mitochondrial beta-oxidation in a patient with an abnormality of the respiratory chain. Studies in skeletal muscle mitochondria.

Oxidative Phosphorylation Diseases

Genomic organization of the human complex I 13-kDa subunit gene NDUFA5

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