A mutation in MT-TW causes a tRNA processing defect and reduced mitochondrial function in a family with Leigh syndrome

Leigh syndrome (LS) is a progressive mitochondrial neurodegenerative disorder, whose symptoms most commonly include psychomotor delay with regression, lactic acidosis and a failure to thrive. Here we describe three siblings with LS, but with additional manifestations including hypertrophic cardiomyo...

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Published inMitochondrion Vol. 25; pp. 113 - 119
Main Authors Duff, Rachael M, Shearwood, Anne-Marie J, Ermer, Judith, Rossetti, Giulia, Gooding, Rebecca, Richman, Tara R, Balasubramaniam, Shanti, Thorburn, David R, Rackham, Oliver, Lamont, Phillipa J, Filipovska, Aleksandra
Format Journal Article
LanguageEnglish
Published Netherlands 01.11.2015
Subjects
Cells, Cultured
Child
Child, Preschool
Family Health
Female
Fibroblasts - physiology
Humans
Infant
Infant, Newborn
Leigh Disease - genetics
Leigh Disease - pathology
Male
Mitochondria - genetics
Mitochondria - metabolism
Point Mutation
RNA Processing, Post-Transcriptional
RNA, Transfer, Trp - genetics
RNA, Transfer, Trp - metabolism
Siblings
Leigh syndrome
tRNA
OXPHOS
MT-TW
tRNA tryptophan
Mitochondrial disease
Multi-organ mitochondrial disease
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Summary:Leigh syndrome (LS) is a progressive mitochondrial neurodegenerative disorder, whose symptoms most commonly include psychomotor delay with regression, lactic acidosis and a failure to thrive. Here we describe three siblings with LS, but with additional manifestations including hypertrophic cardiomyopathy, hepatosplenomegaly, cholestatic hepatitis, and seizures. All three affected siblings were found to be homoplasmic for an m. 5559A>G mutation in the T stem of the mitochondrial DNA-encoded MT-TW by next generation sequencing. The m.5559A>G mutation causes a reduction in the steady state levels of tRNA(Trp) and this decrease likely affects the stability of other mitochondrial RNAs in the patient fibroblasts. We observe accumulation of an unprocessed transcript containing tRNA(Trp), decreased de novo protein synthesis and consequently lowered steady state levels of mitochondrial DNA-encoded proteins that compromise mitochondrial respiration. Our results show that the m.5559A>G mutation at homoplasmic levels causes LS in association with severe multi-organ disease (LS-plus) as a consequence of dysfunctional mitochondrial RNA metabolism.
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ISSN:1567-7249
1872-8278
DOI:10.1016/j.mito.2015.10.008