Novel mutations in the NDUFS1 gene cause low residual activities in human complex I deficiencies.

Authors :: Hoefs, S.J.G.
Skjeldal, O.H.
Rodenburg, R.J.T.
Nedregaard, B.
Kaauwen, E. van
Spiekerkotter, U.
Kleist-Retzow, J.C. von
Smeitink, J.A.M.
Nijtmans, L.G.J.
Heuvel, L.P.W.J. van den
Hoefs, S.J.G.
Skjeldal, O.H.
Rodenburg, R.J.T.
Nedregaard, B.
Kaauwen, E. van
Spiekerkotter, U.
Kleist-Retzow, J.C. von
Smeitink, J.A.M.
Nijtmans, L.G.J.
Heuvel, L.P.W.J. van den
Source :: Molecular Genetics and Metabolism; 251; 6; 1096-7192; 3; 100; ~Molecular Genetics and Metabolism~251~6~~~1096-7192~3~100~~
Publication Year :: 2010
Abstract: 01 juli 2010<br />Contains fulltext : 87205.pdf (publisher's version ) (Closed access)<br />Mitochondrial complex I deficiency is the most frequently encountered defect of the oxidative phosphorylation system. To identify the genetic cause of the complex I deficiency, we screened the gene encoding the NDUFS1 subunit. We report 3 patients with low residual complex I activity expressed in cultured fibroblasts, which displayed novel mutations in the NDUFS1 gene. One mutation introduces a premature stop codon, 3 mutations cause a substitution of amino acids and another mutation a deletion of one amino acid. The fibroblasts of the patients display a decreased amount and activity of complex I. In addition, a disturbed assembly pattern was observed. These results suggest that NDUFS1 is a prime candidate to screen for disease-causing mutations in patients with a very low residual complex I activity in cultured fibroblasts.

Database :: OAIster
Journal :: Molecular Genetics and Metabolism; 251; 6; 1096-7192; 3; 100; ~Molecular Genetics and Metabolism~251~6~~~1096-7192~3~100~~
Publication Type :: Electronic Resource
Accession number :: edsoai.on1367214446
Document Type :: Electronic Resource

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