Activities per year
Abstract
Aims: The group of mtDNA depletion (MIM 251880), a prevalent cause of mitochondrial disease, is a clinically and genetically heterogeneous group of autosomal recessive diseases characterized by reduced mtDNA copy number. Responsible genes are involved either in mtDNA replication or in recycling of the nucleotides in the mitochondria. The aim was to study the role of BN-PAGE in the diagnosis.
Methods: Tissue samples from 434 clinically suspected patients were analyzed using spectrophotometrical analysis and Blue Native PolyAcrylamide Gel Electrophoresis (BN-PAGE) followed by activity staining in the gel. The amount of mtDNA was measured using real-time PCR. In the patients in whom mtDNA depletion was found, DNA analysis of thymidine kinase 2 (TK2), deoxyguanosine kinase (DGUOK) and DNA polymerase gamma (POLG) was performed.
Results: In 91 patients a decreased enzyme activity in one or more OXPHOS complexes was detected using spectrophotometrical analysis. In 44 patients the presence of V subcomplexes was detected following BN-PAGE evaluation. Extensive testing of the mtDNA revealed 25 patients in whom a mtDNA defect was identified. In nine of them mtDNA depletion was found. Mutations were detected in the POLG (7), DGUOK (1) and TK2 gene (1).
Conclusions: Our study shows that mtDNA depletion is a prevalent cause of OXPHOS dysfunction. Application of BN-PAGE proves to be a powerful tool in selecting the patients for genetic evaluation of the mtDNA.
Methods: Tissue samples from 434 clinically suspected patients were analyzed using spectrophotometrical analysis and Blue Native PolyAcrylamide Gel Electrophoresis (BN-PAGE) followed by activity staining in the gel. The amount of mtDNA was measured using real-time PCR. In the patients in whom mtDNA depletion was found, DNA analysis of thymidine kinase 2 (TK2), deoxyguanosine kinase (DGUOK) and DNA polymerase gamma (POLG) was performed.
Results: In 91 patients a decreased enzyme activity in one or more OXPHOS complexes was detected using spectrophotometrical analysis. In 44 patients the presence of V subcomplexes was detected following BN-PAGE evaluation. Extensive testing of the mtDNA revealed 25 patients in whom a mtDNA defect was identified. In nine of them mtDNA depletion was found. Mutations were detected in the POLG (7), DGUOK (1) and TK2 gene (1).
Conclusions: Our study shows that mtDNA depletion is a prevalent cause of OXPHOS dysfunction. Application of BN-PAGE proves to be a powerful tool in selecting the patients for genetic evaluation of the mtDNA.
Original language | English |
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Title of host publication | Euromit7, Stockholm, Sweden |
Pages | 95-95 |
Number of pages | 1 |
Publication status | Published - 11 Jun 2008 |
Event | Finds and Results from the Swedish Cyprus Expedition: A Gender Perspective at the Medelhavsmuseet - Stockholm, Sweden Duration: 21 Sep 2009 → 25 Sep 2009 |
Conference
Conference | Finds and Results from the Swedish Cyprus Expedition: A Gender Perspective at the Medelhavsmuseet |
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Country/Territory | Sweden |
City | Stockholm |
Period | 21/09/09 → 25/09/09 |
Keywords
- BN-PAGE
- mitochondrial DNA depletion
- OXPHOS dysfunction
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Dive into the research topics of 'Role of BN-PAGE in the diagnosis of mitochondrial DNA depletion, a frequent cause of OXPHOS dysfunction.'. Together they form a unique fingerprint.Activities
- 1 Participation in conference
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Euromit 7, European meeting on mitochondrial pathology.
Sara Seneca (Participant)
11 Jun 2008 → 14 Jun 2008Activity: Participating in or organising an event › Participation in conference