Simultaneous A8344G heteroplasmy and mitochondrial DNA copy number quantification in Myoclonus Epilepsy and Ragged-Red Fibers (MERRF) syndrome by a multiplex Molecular Beacon based real-time fluorescence

doi:10.1093/nar/29.3.e13

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Nucleic Acids Research, 2001, Vol. 29, No. 3 e13
© 2001 Oxford University Press

Simultaneous A8344G heteroplasmy and mitochondrial DNA copy number quantification in Myoclonus Epilepsy and Ragged-Red Fibers (MERRF) syndrome by a multiplex Molecular Beacon based real-time fluorescence PCR

Károly Szuhai, Jody M. van den Ouweland, Roeland W. Dirks, Marc Lemaître¹, Jean-Christophe Truffert¹, George M. Janssen, Hans J. Tanke, Elisabeth Holme², J. Antonie Maassen and Anton K. Raap^*

Department of Molecular Cell Biology, Leiden University Medical Center, Leiden, The Netherlands, ¹Eurogentec S.A., Department of Production, Parc Scientifique, B-4102-Seraing, Belgium and ²Department of Clinical Chemistry, Sahlgrenska University Hospital, S-413 45 Gothenburg, Sweden

The association of a particular mitochondrial DNA (mtDNA) mutationwith different clinical phenotypes is a well-known feature ofmitochondrial diseases. A simple genotype–phenotype correlationhas not been found between mutation load and disease expression.Tissue and intercellular mosaicism as well as mtDNA copy numberare thought to be responsible for the different clinical phenotypes.As disease expression of mitochondrial tRNA mutations is mostlyin postmitotic tissues, studies to elucidate disease mechanismsneed to be performed on patient material. Heteroplasmy quantitationand copy number estimation using small patient biopsy sampleshas not been reported before, mainly due to technical restrictions.In order to resolve this problem, we have developed a robustassay that utilizes Molecular Beacons to accurately quantifyheteroplasmy levels and determine mtDNA copy number in smallsamples carrying the A8344G tRNA^Lys mutation. It provides themethodological basis to investigate the role of heteroplasmyand mtDNA copy number in determining the clinical phenotypes.

^* To whom correspondence should be addressed at: Laboratory forCytochemistry and Cytometry, Department of Molecular Cell Biology,Leiden University Medical Center, Wassenaarseweg 72, 2333ALLeiden, The Netherlands. Tel: +31 71 5276187; Fax: +31 71 5276180;Email: a.k.raap{at}lumc.nl Present address:Jody M. van den Ouweland,Isala Clinics, Clinical Chemistry Laboratory, PO Box 10500,8000 GM Zwolle, The Netherlands

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