Whole mitochondrial genome screening in maternally inherited non-syndromic hearing impairment using a microarray resequencing mitochondrial DNA chip

Lévêque, M.; Marlin, Sandrine; Jonard, Laurence; Procaccio, Vincent; Reynier, Pascal; Amati‐Bonneau, Patrizia; Baulande, Sylvain; Pierron, Denis; Lacombe, Didier; Duriez, Françoise; Francannet, Christine; Mom, T.; Journel, Hubert; Catros, Hélène; Drouin‐Garraud, Valérie; Obstoy, Marie-Françoise; Dollfus, Hélène; Eliot, Marie-Madeleine; Faivre, Laurence; Duvillard, C.; Couderc, Rémy; Garabédian, Éréa-Noël; Petit, Christine; Feldmann, Delphine; Denoyelle, Françoise

doi:10.1038/sj.ejhg.5201891

Cited by 79 publications

(59 citation statements)

References 24 publications

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“…Although these pathogenic MTTS2 mutations are associated with a variety of clinical presentations including diabetes mellitus, myopathy, neurodevelopmental delay, encephalopathy and seizures, it is interesting to note that all four are also linked to deafness, [6][7][8] and, like the vast majority of deafness-associated mt-tRNA mutations, 33 both m.12264C4T and m.12261T4C were shown here to exhibit a high threshold for pathogenicity. Two additional MTTS2 sequence variants have also been linked to auditory symptoms; m.12236G4A has been associated with hearing loss 10 and m.12224C4T, associated with haplogroup D4, has been found to modulate the penetrance of hearing loss associated with the MT-RNR1 mutation, m.1555A4G. 34 Similar to MTTS1, 35 the MTTS2 gene is emerging as an important hot spot for deafness-associated mutations.…”

Section: Discussionmentioning

confidence: 99%

“…4,5 These mutations are m.12258C4A, which can lead to progressive deafness and either diabetes mellitus 6 or retinitis pigmentosa, 7 and m.12262C4A, which has been shown to cause progressive mitochondrial myopathy, deafness and sporadic seizures. 8 A further three MTTS2 mutations have been described: m.12207G4A, which is associated with a MELAS-like phenotype, 9 m.12236G4A, which is linked to non-syndromic hearing impairment, 10 and m.12246C4A, which is associated with chronic intestinal pseudo-obstruction with myopathy and ophthalmoplegia. 11 However, due to a lack of functional investigations (eg, single-fibre analysis, trans-mitochondrial cybrid studies), their pathogenicity has not yet been unequivocally proven.…”

Section: Introductionmentioning

confidence: 99%

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Mutations in the mitochondrial tRNASer(AGY) gene are associated with deafness, retinal degeneration, myopathy and epilepsy

et al. 2012

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Although over 200 pathogenic mitochondrial DNA (mtDNA) mutations have been reported to date, determining the genetic aetiology of many cases of mitochondrial disease is still not straightforward. Here, we describe the investigations undertaken to uncover the underlying molecular defect(s) in two unrelated Caucasian patients with suspected mtDNA disease, who presented with similar symptoms of myopathy, deafness, neurodevelopmental delay, epilepsy, marked fatigue and, in one case, retinal degeneration. Histochemical and biochemical evidence of mitochondrial respiratory chain deficiency was observed in the patient muscle biopsies and both patients were discovered to harbour a novel heteroplasmic mitochondrial tRNA (mt-tRNA) Ser(AGY) (MTTS2) mutation (m.12264C4T and m.12261T4C, respectively). Clear segregation of the m.12261T4C mutation with the biochemical defect, as demonstrated by single-fibre radioactive RFLP, confirmed the pathogenicity of this novel variant in patient 2. However, unusually high levels of m.12264C4T mutation within both COX-positive (98.4 ± 1.5%) and COX-deficient (98.2 ±2.1%) fibres in patient 1 necessitated further functional investigations to prove its pathogenicity. Northern blot analysis demonstrated the detrimental effect of the m.12264C4T mutation on mt-tRNA Ser(AGY) stability, ultimately resulting in decreased steady-state levels of fully assembled complexes I and IV, as shown by blue-native polyacrylamide gel electrophoresis. Our findings expand the spectrum of pathogenic mutations associated with the MTTS2 gene and highlight MTTS2 mutations as an important cause of retinal and syndromic auditory impairment.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Mutations in the mitochondrial tRNASer(AGY) gene are associated with deafness, retinal degeneration, myopathy and epilepsy

et al. 2012

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Section: Discussionmentioning

confidence: 99%

“…56,57 The Mitochip uses hybridization for detecting mutations or polymorphisms, so that the probes mtDNA mutation screening for hereditary HL T Kato et al should be designed. 56 Although version 2.0 of Mitochip has been improved for detecting mutations, the present version has not been designed for analysis of Asian mtDNA, as it is based on the revised Cambridge reference sequence. 25,26 As it is necessary to distinguish pathological mtDNA mutations from non-pathogenic mtSNPs, this study used 11 pairs of primers for multiple PCR amplifications and multiple sequence-specific oligonucleotide probes customized for the Japanese population, which were designed to carefully detect either mutant or wild-type mtDNA, even when mtSNPs were present in the vicinity of the mutation sites.…”

Section: Discussionmentioning

confidence: 99%

Extensive and rapid screening for major mitochondrial DNA point mutations in patients with hereditary hearing loss

et al. 2010

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Sensorineural hearing loss (HL) is one of the most frequent clinical features in patients with mitochondrial diseases caused by mitochondrial DNA (mtDNA) mutations, and hearing is impaired in over half of all cases with mitochondrial disorders. This study analyzed 373 patients with suspected hereditary HL using an extensive and rapid suspension-array screening system for 29 major mtDNA mutations, including the m.1555A4G homoplasmic mutation in the MT-RNR1 gene, which causes non-syndromic sensorineural HL and aminoglycoside-induced HL, and the m.3243A4G heteroplasmic mutation in the MT-TL1 gene. This method is rapid and suitable for large-scale screening because universal 96-well plates are available for use, and because an analysis of each plate can be completed within 1 h. This system detected five different mtDNA mutations in 24 of the 373 (6.4%) patients. The m.1555A4G and m.3243A4G mutations were detected in 11 (2.9%) and 9 (2.7%) patients, respectively. In addition, three mutations, that is, m.8348A4G in the MT-TK gene, m.11778G4A in the MT-ND4 gene and 15498G4A in the MT-CYB gene were detected in one patient for each. This screening system is useful for the genetic diagnosis and epidemiological study of both syndromic and non-syndromic HL.

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“…During recent years, certain techniques, including restriction fragment length polymorphism (RFLP) genotyping, direct DNA sequence, and the resequencing Mitochip array have been described and are even commercially available for detecting mtDNA mutations [3,9,17,19], however, potential risk of contamination makes it difficult to avoid using electrophoresis detection method. Although fluorescence resonance energy transfer (FRET) by using two fluorescent dyes in close proximity is one of the most powerful and promising methods for SNP genotyping [20], the expensive costs of fluorescent modification and requirement of special equipment may limit its application widely in the clinical testing.…”

mentioning

confidence: 99%

A novel method of detecting mitochondrial m.1494C>T and m.1555A>G mutations in a single PCR reaction using base-quenched probe

Zheng

Luo

Zhang

et al. 2010

Clinica Chimica Acta

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Whole mitochondrial genome screening in maternally inherited non-syndromic hearing impairment using a microarray resequencing mitochondrial DNA chip

Cited by 79 publications

References 24 publications

Mutations in the mitochondrial tRNASer(AGY) gene are associated with deafness, retinal degeneration, myopathy and epilepsy

Mutations in the mitochondrial tRNASer(AGY) gene are associated with deafness, retinal degeneration, myopathy and epilepsy

Extensive and rapid screening for major mitochondrial DNA point mutations in patients with hereditary hearing loss

A novel method of detecting mitochondrial m.1494C>T and m.1555A>G mutations in a single PCR reaction using base-quenched probe

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