Age-related accumulation of somatic mitochondrial DNA mutations in adult-derived human ipscs

Eunju Kang; Xinjian Wang; Rebecca Tippner-Hedges; Hong Ma; Clifford D.L. Folmes; Nuria Marti Gutierrez; Yeonmi Lee; Crystal Van Dyken; Riffat Ahmed; Ying Li; Amy Koski; Tomonari Hayama; Shiyu Luo; Cary O. Harding; Paula Amato; Jeffrey Jensen; David Battaglia; David Lee; Diana Wu; Andre Terzic; Don P. Wolf; Taosheng Huang; Shoukhrat Mitalipov

doi:10.1016/j.stem.2016.02.005

Age-related accumulation of somatic mitochondrial DNA mutations in adult-derived human ipscs

Eunju Kang, Xinjian Wang, Rebecca Tippner-Hedges, Hong Ma, Clifford D.L. Folmes, Nuria Marti Gutierrez, Yeonmi Lee, Crystal Van Dyken, Riffat Ahmed, Ying Li, Amy Koski, Tomonari Hayama, Shiyu Luo, Cary O. Harding, Paula Amato, Jeffrey Jensen, David Battaglia, David Lee, Diana Wu, Andre TerzicDon P. Wolf, Taosheng Huang, Shoukhrat Mitalipov

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131 Scopus citations

Abstract

The genetic integrity of iPSCs is an important consideration for therapeutic application. In this study, we examine the accumulation of somatic mitochondrial genome (mtDNA) mutations in skin fibroblasts, blood, and iPSCs derived from young and elderly subjects (24-72 years). We found that pooled skin and blood mtDNA contained low heteroplasmic point mutations, but a panel of ten individual iPSC lines from each tissue or clonally expanded fibroblasts carried an elevated load of heteroplasmic or homoplasmic mutations, suggesting that somatic mutations randomly arise within individual cells but are not detectable in whole tissues. The frequency of mtDNA defects in iPSCs increased with age, and many mutations were non-synonymous or resided in RNA coding genes and thus can lead to respiratory defects. Our results highlight a need to monitor mtDNA mutations in iPSCs, especially those generated from older patients, and to examine the metabolic status of iPSCs destined for clinical applications.

Original language	English (US)
Pages (from-to)	625-636
Number of pages	12
Journal	Cell Stem Cell
Volume	18
Issue number	5
DOIs	https://doi.org/10.1016/j.stem.2016.02.005
State	Published - May 5 2016

ASJC Scopus subject areas

Molecular Medicine
Genetics
Cell Biology

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Kang, E., Wang, X., Tippner-Hedges, R., Ma, H., Folmes, C. D. L., Gutierrez, N. M., Lee, Y., Van Dyken, C., Ahmed, R., Li, Y., Koski, A., Hayama, T., Luo, S., Harding, C. O., Amato, P., Jensen, J., Battaglia, D., Lee, D., Wu, D., ... Mitalipov, S. (2016). Age-related accumulation of somatic mitochondrial DNA mutations in adult-derived human ipscs. Cell Stem Cell, 18(5), 625-636. https://doi.org/10.1016/j.stem.2016.02.005

Kang, E, Wang, X, Tippner-Hedges, R, Ma, H, Folmes, CDL, Gutierrez, NM, Lee, Y, Van Dyken, C, Ahmed, R, Li, Y, Koski, A, Hayama, T, Luo, S, Harding, CO, Amato, P, Jensen, J, Battaglia, D, Lee, D, Wu, D, Terzic, A, Wolf, DP, Huang, T & Mitalipov, S 2016, 'Age-related accumulation of somatic mitochondrial DNA mutations in adult-derived human ipscs', Cell Stem Cell, vol. 18, no. 5, pp. 625-636. https://doi.org/10.1016/j.stem.2016.02.005

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abstract = "The genetic integrity of iPSCs is an important consideration for therapeutic application. In this study, we examine the accumulation of somatic mitochondrial genome (mtDNA) mutations in skin fibroblasts, blood, and iPSCs derived from young and elderly subjects (24-72 years). We found that pooled skin and blood mtDNA contained low heteroplasmic point mutations, but a panel of ten individual iPSC lines from each tissue or clonally expanded fibroblasts carried an elevated load of heteroplasmic or homoplasmic mutations, suggesting that somatic mutations randomly arise within individual cells but are not detectable in whole tissues. The frequency of mtDNA defects in iPSCs increased with age, and many mutations were non-synonymous or resided in RNA coding genes and thus can lead to respiratory defects. Our results highlight a need to monitor mtDNA mutations in iPSCs, especially those generated from older patients, and to examine the metabolic status of iPSCs destined for clinical applications.",

author = "Eunju Kang and Xinjian Wang and Rebecca Tippner-Hedges and Hong Ma and Folmes, {Clifford D.L.} and Gutierrez, {Nuria Marti} and Yeonmi Lee and {Van Dyken}, Crystal and Riffat Ahmed and Ying Li and Amy Koski and Tomonari Hayama and Shiyu Luo and Harding, {Cary O.} and Paula Amato and Jeffrey Jensen and David Battaglia and David Lee and Diana Wu and Andre Terzic and Wolf, {Don P.} and Taosheng Huang and Shoukhrat Mitalipov",

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AU - Gutierrez, Nuria Marti

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AU - Ahmed, Riffat

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AU - Harding, Cary O.

AU - Amato, Paula

AU - Jensen, Jeffrey

AU - Battaglia, David

AU - Lee, David

AU - Wu, Diana

AU - Terzic, Andre

AU - Wolf, Don P.

AU - Huang, Taosheng

AU - Mitalipov, Shoukhrat

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Age-related accumulation of somatic mitochondrial DNA mutations in adult-derived human ipscs

Abstract

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