| Literature DB >> 32385911 |
Yukiko Yatsuka1,2, Yoshihito Kishita1,2, Luke E Formosa3, Masaru Shimura4, Fumihito Nozaki5, Tatsuya Fujii5, Kazuhiro R Nitta1,2, Akira Ohtake6,7, Kei Murayama4, Michael T Ryan3, Yasushi Okazaki1,2,8.
Abstract
Mitochondrial complex I deficiency is caused by pathogenic variants in mitochondrial and nuclear genes associated with complex I structure and assembly. We report the case of a patient with NDUFA8-related mitochondrial disease. The patient presented with developmental delay, microcephaly, and epilepsy. His fibroblasts showed apparent biochemical defects in mitochondrial complex I. Whole-exome sequencing revealed that the patient carried a homozygous variant in NDUFA8. His fibroblasts showed a reduction in the protein expression level of not only NDUFA8, but also the other complex I subunits, consistent with assembly defects. The enzyme activity of complex I and oxygen consumption rate were restored by reintroducing wild-typeNDUFA8 cDNA into patient fibroblasts. The functional properties of the variant in NDUFA8 were also investigated using NDUFA8 knockout cells expressing wild-type or mutated NDUFA8 cDNA. These experiments further supported the pathogenicity of the variant in complex I assembly. This is the first report describing that the loss of NDUFA8, which has not previously been associated with mitochondrial disease, causes severe defect in the assembly of mitochondrial complex I, leading to progressive neurological and developmental abnormalities.Entities:
Keywords: CX9C motif; OXPHOS; complex I deficiency; disulfide relay import pathway; mitochondrial disease; mitochondrial intermembrane space
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Year: 2020 PMID: 32385911 DOI: 10.1111/cge.13773
Source DB: PubMed Journal: Clin Genet ISSN: 0009-9163 Impact factor: 4.438