Base-excision repair deficiency alone or combined with increased oxidative stress does not increase mtDNA point mutations in mice

Johanna H.K. Kauppila; Nina A. Bonekamp; Arnaud Mourier; Marita A Isokallio; Alexandra Just; Timo E.S. Kauppila; James B. Stewart; Nils-Göran Larsson

doi:https://doi.org/10.1093/nar/gky456

doi.org/10.1093/nar/gky456

Base-excision repair deficiency alone or combined with increased oxidative stress does not increase mtDNA point mutations in mice

Johanna H.K. Kauppila

8

,

Nina A. Bonekamp

8

,

..., Nils-Göran Larsson

76

Nucleic Acids Research14.90

Volume: 46, Issue: 13, Pages: 6642 - 6669

Published: May 31, 2018

Abstract

Mitochondrial DNA (mtDNA) mutations become more prevalent with age and are postulated to contribute to the ageing process. Point mutations of mtDNA have been suggested to originate from two main sources, i.e. replicative errors and oxidative damage, but the contribution of each of these processes is much discussed. To elucidate the origin of mtDNA mutations, we measured point mutation load in mice with deficient mitochondrial base-excision...

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Paper Details

Title

Base-excision repair deficiency alone or combined with increased oxidative stress does not increase mtDNA point mutations in mice

DOI

doi.org/10.1093/nar/gky456

Published Date

May 31, 2018

Journal

Nucleic Acids Research

Volume

46

Issue

13

Pages

6642 - 6669

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