Similar Patterns of Clonally Expanded Somatic MtDNA Mutations in the Colon of Heterozygous MtDNA Mutator Mice and Ageing Humans

Overview

Journal Mech Ageing Dev

Specialty Geriatrics

Date 2014 Jun 11

PMID 24915468

Citations 19

Authors

Holly L Baines

James B Stewart

Craig Stamp

Anze Zupanic

Thomas B L Kirkwood

Nils-Goran Larsson

Douglass M Turnbull

Laura C Greaves

Affiliations

Soon will be listed here.

Abstract

Clonally expanded mitochondrial DNA (mtDNA) mutations resulting in focal respiratory chain deficiency in individual cells are proposed to contribute to the ageing of human tissues that depend on adult stem cells for self-renewal; however, the consequences of these mutations remain unclear. A good animal model is required to investigate this further; but it is unknown whether mechanisms for clonal expansion of mtDNA mutations, and the mutational spectra, are similar between species. Here we show that mice, heterozygous for a mutation disrupting the proof-reading activity of mtDNA polymerase (PolgA(+/mut)) resulting in an increased mtDNA mutation rate, accumulate clonally expanded mtDNA point mutations in their colonic crypts with age. This results in focal respiratory chain deficiency, and by 81 weeks of age these animals exhibit a similar level and pattern of respiratory chain deficiency to 70-year-old human subjects. Furthermore, like in humans, the mtDNA mutation spectrum appears random and there is an absence of selective constraints. Computer simulations show that a random genetic drift model of mtDNA clonal expansion can accurately model the data from the colonic crypts of wild-type, PolgA(+/mut) animals, and humans, providing evidence for a similar mechanism for clonal expansion of mtDNA point mutations between these mice and humans.

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