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Biallelic Mutations in MRPS34 Lead to Instability of the Small Mitoribosomal Subunit and Leigh Syndrome.


ABSTRACT: The synthesis of all 13 mitochondrial DNA (mtDNA)-encoded protein subunits of the human oxidative phosphorylation (OXPHOS) system is carried out by mitochondrial ribosomes (mitoribosomes). Defects in the stability of mitoribosomal proteins or mitoribosome assembly impair mitochondrial protein translation, causing combined OXPHOS enzyme deficiency and clinical disease. Here we report four autosomal-recessive pathogenic mutations in the gene encoding the small mitoribosomal subunit protein, MRPS34, in six subjects from four unrelated families with Leigh syndrome and combined OXPHOS defects. Whole-exome sequencing was used to independently identify all variants. Two splice-site mutations were identified, including homozygous c.321+1G>T in a subject of Italian ancestry and homozygous c.322-10G>A in affected sibling pairs from two unrelated families of Puerto Rican descent. In addition, compound heterozygous MRPS34 mutations were identified in a proband of French ancestry; a missense (c.37G>A [p.Glu13Lys]) and a nonsense (c.94C>T [p.Gln32?]) variant. We demonstrated that these mutations reduce MRPS34 protein levels and the synthesis of OXPHOS subunits encoded by mtDNA. Examination of the mitoribosome profile and quantitative proteomics showed that the mitochondrial translation defect was caused by destabilization of the small mitoribosomal subunit and impaired monosome assembly. Lentiviral-mediated expression of wild-type MRPS34 rescued the defect in mitochondrial translation observed in skin fibroblasts from affected subjects, confirming the pathogenicity of MRPS34 mutations. Our data establish that MRPS34 is required for normal function of the mitoribosome in humans and furthermore demonstrate the power of quantitative proteomic analysis to identify signatures of defects in specific cellular pathways in fibroblasts from subjects with inherited disease.

SUBMITTER: Lake NJ 

PROVIDER: S-EPMC5544391 | biostudies-literature | 2017 Aug

REPOSITORIES: biostudies-literature

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Biallelic Mutations in MRPS34 Lead to Instability of the Small Mitoribosomal Subunit and Leigh Syndrome.

Lake Nicole J NJ   Webb Bryn D BD   Stroud David A DA   Richman Tara R TR   Ruzzenente Benedetta B   Compton Alison G AG   Mountford Hayley S HS   Pulman Juliette J   Zangarelli Coralie C   Rio Marlene M   Boddaert Nathalie N   Assouline Zahra Z   Sherpa Mingma D MD   Schadt Eric E EE   Houten Sander M SM   Byrnes James J   McCormick Elizabeth M EM   Zolkipli-Cunningham Zarazuela Z   Haude Katrina K   Zhang Zhancheng Z   Retterer Kyle K   Bai Renkui R   Calvo Sarah E SE   Mootha Vamsi K VK   Christodoulou John J   Rötig Agnes A   Filipovska Aleksandra A   Cristian Ingrid I   Falk Marni J MJ   Metodiev Metodi D MD   Thorburn David R DR  

American journal of human genetics 20170801 2


The synthesis of all 13 mitochondrial DNA (mtDNA)-encoded protein subunits of the human oxidative phosphorylation (OXPHOS) system is carried out by mitochondrial ribosomes (mitoribosomes). Defects in the stability of mitoribosomal proteins or mitoribosome assembly impair mitochondrial protein translation, causing combined OXPHOS enzyme deficiency and clinical disease. Here we report four autosomal-recessive pathogenic mutations in the gene encoding the small mitoribosomal subunit protein, MRPS34  ...[more]

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