Literature DB >> 9443465

Multiple mtDNA deletions features in autosomal dominant and recessive diseases suggest distinct pathogeneses.

R Carrozzo1, M Hirano, B Fromenty, C Casali, F M Santorelli, E Bonilla, S DiMauro, E A Schon, A F Miranda.   

Abstract

Multiple mitochondrial DNA (mtDNA) deletions have been described in patients with autosomal dominant progressive external ophthalmoplegia (AD-PEO) and in autosomal recessive disorders including mitochondrial neurogastrointestinal encephalomyopathy (MNGIE) and autosomal recessive cardiomyopathy ophthalmoplegia (ARCO). The pathogenic bases of these disorders are unknown. We studied three patients with AD-PEO and three patients with autosomal recessive (AR)-PEO (two patients with MNGIE and one patient with ARCO). Histochemistry and Southern blot analyses of DNA were performed in skeletal muscle from the patients. Muscle mtDNA was used to characterize the pattern and amounts of the multiple mtDNA rearrangements; PCR analysis was performed to obtain finer maps of the deleted regions in both conditions. The patients with AD-PEO had myopathic features; the patients with AR-PEO had multisystem disorders. The percentage of ragged-red and cytochrome c oxidase-negative fibers tended to be higher in muscle from the patients with AD-PEO (19% +/- 13.9, 29.7 +/- 26.3) than in muscle from the patients with AR-PEO (1.4% +/- 1.4, 3.3% +/- 3.2; p < 0.10). The sizes of the multiple mtDNA deletions ranged from approximately 4.0 to 10.0 kilobases in muscle from both groups of patients, and in both groups, we identified only deleted and no duplicated mtDNA molecules. Patients with AD-PEO harbored a greater proportion of deleted mtDNA species in muscle (31% +/- 5.3) than did patients with AR-PEO (9.7% +/- 9.1; p < 0.05). In the patients with AD-PEO, we identified a deletion that included the mtDNA heavy strand promoter (HSP) region, which had been previously described as the HSP deletion. The HSP deletion was not present in the patients with AR-PEO. Our findings show the clinical, histologic, and molecular genetic heterogeneity of these complex disorders. In particular, the proportions of multiple mtDNA deletions were higher in muscle samples from patients with AD-PEO than in those from patients with AR-PEO.

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Year:  1998        PMID: 9443465     DOI: 10.1212/wnl.50.1.99

Source DB:  PubMed          Journal:  Neurology        ISSN: 0028-3878            Impact factor:   9.910


  14 in total

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3.  Mitochondrial neuro-gastrointestinal encephalopathy syndrome.

Authors:  Anuj Walia; B R Thapa; V Kim
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4.  Multiple mtDNA deletions: clinical and molecular correlations.

Authors:  F M Santorelli; G De Joanna; C Casali; A Tessa; G Siciliano; G A Amabile; F Pierelli; L Vilarinho; L Santoro
Journal:  J Inherit Metab Dis       Date:  2000-03       Impact factor: 4.982

Review 5.  Primary Mitochondrial Disease and Secondary Mitochondrial Dysfunction: Importance of Distinction for Diagnosis and Treatment.

Authors:  Dmitriy M Niyazov; Stephan G Kahler; Richard E Frye
Journal:  Mol Syndromol       Date:  2016-06-03

6.  Clinicopathological aspects of the neuropathy of neurogastrointestinal encephalomyopathy (MNGIE) in four patients including two with a Charcot-Marie-Tooth presentation.

Authors:  Gérard Said; Catherine Lacroix; Violaine Planté-Bordeneuve; Bernard Messing; Abdelhamid Slama; Pascal Crenn; Annie Nivelon-Chevallier; Laurent Bedenne; Pierre Soichot; E Manceau; Daniel Rigaud; Anne Guiochon-Mantel; Claude Matuchansky
Journal:  J Neurol       Date:  2005-03-07       Impact factor: 4.849

7.  Two families with autosomal dominant progressive external ophthalmoplegia.

Authors:  S Kiechl; R Horváth; P Luoma; U Kiechl-Kohlendorfer; B Wallacher-Scholz; R Stucka; C Thaler; J Wanschitz; A Suomalainen; M Jaksch; J Willeit
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8.  Mitochondrial neurogastrointestinal encephalomyopathy syndrome maps to chromosome 22q13.32-qter.

Authors:  M Hirano; J Garcia-de-Yebenes; A C Jones; I Nishino; S DiMauro; J R Carlo; A N Bender; A F Hahn; L M Salberg; D E Weeks; T G Nygaard
Journal:  Am J Hum Genet       Date:  1998-08       Impact factor: 11.025

9.  Targeted deletion of both thymidine phosphorylase and uridine phosphorylase and consequent disorders in mice.

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Journal:  Mol Cell Biol       Date:  2002-07       Impact factor: 4.272

10.  Site-specific somatic mitochondrial DNA point mutations in patients with thymidine phosphorylase deficiency.

Authors:  Yutaka Nishigaki; Ramon Martí; William C Copeland; Michio Hirano
Journal:  J Clin Invest       Date:  2003-06       Impact factor: 14.808
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