Pearson syndrome and the role of deletion dimers and duplications in the mtDNA

Pearson syndrome and the role of deletion dimers and duplications in the mtDNA

Pearson syndrome is an often fatal multisystem disease associated with mitochondrial DNA rearrangements. Here we report a patient with a novel mtDNA deletion of 3.4 kb ranging from nucleotides 6097 to 9541 in combination with deletion dimers. The mutation percentage in different tissues (blood, musc...

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Veröffentlicht in:Journal of inherited metabolic disease 2004-01, Vol.27 (1), p.47-55
Hauptverfasser: Jacobs, L. J. A. M., Jongbloed, R. J. E., Wijburg, F. A., Klerk, J. B. C., Geraedts, J. P. M., Nijland, J. G., Scholte, H. R., Coo, I. F. M., Smeets, H. J. M.
Format: Artikel
Sprache:eng
Schlagworte:
Anemia - genetics
Biological and medical sciences
Bone Marrow Diseases - genetics
Child
Child, Preschool
Dimerization
DNA, Mitochondrial - genetics
Fatal Outcome
Feeding. Feeding behavior
Female
Fibrosis
Fundamental and applied biological sciences. Psychology
Gene Deletion
Gene Duplication
Gene Rearrangement
Genetics of eukaryotes. Biological and molecular evolution
Genotype
Humans
Molecular and cellular biology
Pancreatic Diseases - genetics
Pancreatic Diseases - pathology
Phenotype
Syndrome
Vertebrates: anatomy and physiology, studies on body, several organs or systems
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Beschreibung
Zusammenfassung:Pearson syndrome is an often fatal multisystem disease associated with mitochondrial DNA rearrangements. Here we report a patient with a novel mtDNA deletion of 3.4 kb ranging from nucleotides 6097 to 9541 in combination with deletion dimers. The mutation percentage in different tissues (blood, muscle and liver) varied between 64% and 95%. After a remission period of about a year, the patient suddenly died at the age of 3 years owing to a severe lactic acidosis. A second patient with a previously reported deletion of 8 kb and a milder phenotype was found to have mitochondrial duplications and died at the age of 10 years. From these data and data from previous reports, we hypothesize that duplications might be beneficial in the clinical course of the disease and in life expectancy.
ISSN:0141-8955
1573-2665
DOI:10.1023/B:BOLI.0000016601.49372.18