Non-random MtDNA Segregation Patterns Indicate a Metastable Heteroplasmic Segregation Unit in M.3243A>G Cybrid Cells

Overview

Journal PLoS One

Specialties General Medicine
Science

Date 2012 Dec 29

PMID 23272214

Citations 12

Authors

Anton K Raap

Roshan S Jahangir Tafrechi

Frans M van de Rijke

Angela Pyle

Carolina Wahlby

Karoly Szuhai

Raimond B G Ravelli

Rene F M de Coo

Harsha K Rajasimha

Mats Nilsson

Patrick F Chinnery

David C Samuels

George M C Janssen

Affiliations

Soon will be listed here.

Abstract

Many pathogenic mitochondrial DNA mutations are heteroplasmic, with a mixture of mutated and wild-type mtDNA present within individual cells. The severity and extent of the clinical phenotype is largely due to the distribution of mutated molecules between cells in different tissues, but mechanisms underpinning segregation are not fully understood. To facilitate mtDNA segregation studies we developed assays that measure m.3243A>G point mutation loads directly in hundreds of individual cells to determine the mechanisms of segregation over time. In the first study of this size, we observed a number of discrete shifts in cellular heteroplasmy between periods of stable heteroplasmy. The observed patterns could not be parsimoniously explained by random mitotic drift of individual mtDNAs. Instead, a genetically metastable, heteroplasmic mtDNA segregation unit provides the likely explanation, where stable heteroplasmy is maintained through the faithful replication of segregating units with a fixed wild-type/m.3243A>G mutant ratio, and shifts occur through the temporary disruption and re-organization of the segregation units. While the nature of the physical equivalent of the segregation unit remains uncertain, the factors regulating its organization are of major importance for the pathogenesis of mtDNA diseases.

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