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Mitochondrial DNA mutations in human colonic crypt stem cells
Robert W. Taylor, … , Thomas B.L. Kirkwood, Douglass M. Turnbull
Robert W. Taylor, … , Thomas B.L. Kirkwood, Douglass M. Turnbull
Published November 1, 2003
Citation Information: J Clin Invest. 2003;112(9):1351-1360. https://doi.org/10.1172/JCI19435.
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Article

Mitochondrial DNA mutations in human colonic crypt stem cells

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Abstract

The mitochondrial genome encodes 13 essential subunits of the respiratory chain and has remarkable genetics based on uniparental inheritance. Within human populations, the mitochondrial genome has a high rate of sequence divergence with multiple polymorphic variants and thus has played a major role in examining the evolutionary history of our species. In recent years it has also become apparent that pathogenic mitochondrial DNA (mtDNA) mutations play an important role in neurological and other diseases. Patients harbor many different mtDNA mutations, some of which are mtDNA mutations, some of which are inherited, but others that seem to be sporadic. It has also been suggested that mtDNA mutations play a role in aging and cancer, but the evidence for a causative role in these conditions is less clear. The accumulated data would suggest, however, that mtDNA mutations occur on a frequent basis. In this article we describe a new phenomenon: the accumulation of mtDNA mutations in human colonic crypt stem cells that result in a significant biochemical defect in their progeny. These studies have important consequences not only for understanding of the finding of mtDNA mutations in aging tissues and tumors, but also for determining the frequency of mtDNA mutations within a cell.

Authors

Robert W. Taylor, Martin J. Barron, Gillian M. Borthwick, Amy Gospel, Patrick F. Chinnery, David C. Samuels, Geoffrey A. Taylor, Stefan M. Plusa, Stephanie J. Needham, Laura C. Greaves, Thomas B.L. Kirkwood, Douglass M. Turnbull

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Details of patients studied for the presence of cytochrome c oxidase–def...

Details of patients studied for the presence of cytochrome c oxidase–deficient crypts


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