Immortalization of Different Breast Epithelial Cell Types Results in Distinct Mitochondrial Mutagenesis

Immortalization of Different Breast Epithelial Cell Types Results in Distinct Mitochondrial Mutagenesis

Different phenotypes of normal cells might influence genetic profiles, epigenetic profiles, and tumorigenicities of their transformed derivatives. In this study, we investigate whether the whole mitochondrial genome of immortalized cells can be attributed to the different phenotypes (stem vs. non-st...

Full description

Bibliographic Details
Main Authors: Sujin Kwon, Susan S. Kim, Howard E. Nebeck, Eun Hyun Ahn
Format: Article
Language:English
Published: MDPI AG 2019-06-01
Series:International Journal of Molecular Sciences
Subjects:
mitochondrial DNA
rare mutation
stem cells
breast cancer
mitochondrial tRNA
duplex sequencing
next generation sequencing
Online Access:https://www.mdpi.com/1422-0067/20/11/2813
id doaj-8589f9d6f7df488591f4fb95cd16668c
record_format Article
spelling doaj-8589f9d6f7df488591f4fb95cd16668c2020-11-25T02:40:48ZengMDPI AGInternational Journal of Molecular Sciences1422-00672019-06-012011281310.3390/ijms20112813ijms20112813Immortalization of Different Breast Epithelial Cell Types Results in Distinct Mitochondrial MutagenesisSujin Kwon0Susan S. Kim1Howard E. Nebeck2Eun Hyun Ahn3Department of Pathology, University of Washington, Seattle, WA 98195, USADepartment of Biochemistry, University of Washington, Seattle, WA 98195, USADepartment of Pathology, University of Washington, Seattle, WA 98195, USADepartment of Pathology, University of Washington, Seattle, WA 98195, USADifferent phenotypes of normal cells might influence genetic profiles, epigenetic profiles, and tumorigenicities of their transformed derivatives. In this study, we investigate whether the whole mitochondrial genome of immortalized cells can be attributed to the different phenotypes (stem vs. non-stem) of their normal epithelial cell originators. To accurately determine mutations, we employed Duplex Sequencing, which exhibits the lowest error rates among currently-available DNA sequencing methods. Our results indicate that the vast majority of the observed mutations of the whole mitochondrial DNA occur at low-frequency (rare mutations). The most prevalent rare mutation types are C→T/G→A and A→G/T→C transitions. Frequencies and spectra of homoplasmic point mutations are virtually identical between stem cell-derived immortalized (SV1) cells and non-stem cell-derived immortalized (SV22) cells, verifying that both cell types were derived from the same woman. However, frequencies of rare point mutations are significantly lower in SV1 cells (5.79 × 10<sup>−5</sup>) than in SV22 cells (1.16 × 10<sup>−4</sup>). The significantly lower frequencies of rare mutations are aligned with a finding of longer average distances to adjacent mutations in SV1 cells than in SV22 cells. Additionally, the predicted pathogenicity for rare mutations in the mitochondrial tRNA genes tends to be lower (by 2.5-fold) in SV1 cells than in SV22 cells. While four known/confirmed pathogenic mt-tRNA mutations (m.5650 G&gt;A, m.5521 G&gt;A, m.5690 A&gt;G, m.1630 A&gt;G) were identified in SV22 cells, no such mutations were observed in SV1 cells. Our findings suggest that the immortalization of normal cells with stem cell features leads to decreased mitochondrial mutagenesis, particularly in RNA gene regions. The mutation spectra and mutations specific to stem cell-derived immortalized cells (vs. non-stem cell derived) have implications in characterizing the heterogeneity of tumors and understanding the role of mitochondrial mutations in the immortalization and transformation of human cells.https://www.mdpi.com/1422-0067/20/11/2813mitochondrial DNArare mutationstem cellsbreast cancermitochondrial tRNAduplex sequencingnext generation sequencing
collection DOAJ
language English
format Article
sources DOAJ
author Sujin Kwon
Susan S. Kim
Howard E. Nebeck
Eun Hyun Ahn
spellingShingle Sujin Kwon
Susan S. Kim
Howard E. Nebeck
Eun Hyun Ahn
Immortalization of Different Breast Epithelial Cell Types Results in Distinct Mitochondrial Mutagenesis
International Journal of Molecular Sciences
mitochondrial DNA
rare mutation
stem cells
breast cancer
mitochondrial tRNA
duplex sequencing
next generation sequencing
author_facet Sujin Kwon
Susan S. Kim
Howard E. Nebeck
Eun Hyun Ahn
author_sort Sujin Kwon
title Immortalization of Different Breast Epithelial Cell Types Results in Distinct Mitochondrial Mutagenesis
title_short Immortalization of Different Breast Epithelial Cell Types Results in Distinct Mitochondrial Mutagenesis
title_full Immortalization of Different Breast Epithelial Cell Types Results in Distinct Mitochondrial Mutagenesis
title_fullStr Immortalization of Different Breast Epithelial Cell Types Results in Distinct Mitochondrial Mutagenesis
title_full_unstemmed Immortalization of Different Breast Epithelial Cell Types Results in Distinct Mitochondrial Mutagenesis
title_sort immortalization of different breast epithelial cell types results in distinct mitochondrial mutagenesis
publisher MDPI AG
series International Journal of Molecular Sciences
issn 1422-0067
publishDate 2019-06-01
description Different phenotypes of normal cells might influence genetic profiles, epigenetic profiles, and tumorigenicities of their transformed derivatives. In this study, we investigate whether the whole mitochondrial genome of immortalized cells can be attributed to the different phenotypes (stem vs. non-stem) of their normal epithelial cell originators. To accurately determine mutations, we employed Duplex Sequencing, which exhibits the lowest error rates among currently-available DNA sequencing methods. Our results indicate that the vast majority of the observed mutations of the whole mitochondrial DNA occur at low-frequency (rare mutations). The most prevalent rare mutation types are C→T/G→A and A→G/T→C transitions. Frequencies and spectra of homoplasmic point mutations are virtually identical between stem cell-derived immortalized (SV1) cells and non-stem cell-derived immortalized (SV22) cells, verifying that both cell types were derived from the same woman. However, frequencies of rare point mutations are significantly lower in SV1 cells (5.79 × 10<sup>−5</sup>) than in SV22 cells (1.16 × 10<sup>−4</sup>). The significantly lower frequencies of rare mutations are aligned with a finding of longer average distances to adjacent mutations in SV1 cells than in SV22 cells. Additionally, the predicted pathogenicity for rare mutations in the mitochondrial tRNA genes tends to be lower (by 2.5-fold) in SV1 cells than in SV22 cells. While four known/confirmed pathogenic mt-tRNA mutations (m.5650 G&gt;A, m.5521 G&gt;A, m.5690 A&gt;G, m.1630 A&gt;G) were identified in SV22 cells, no such mutations were observed in SV1 cells. Our findings suggest that the immortalization of normal cells with stem cell features leads to decreased mitochondrial mutagenesis, particularly in RNA gene regions. The mutation spectra and mutations specific to stem cell-derived immortalized cells (vs. non-stem cell derived) have implications in characterizing the heterogeneity of tumors and understanding the role of mitochondrial mutations in the immortalization and transformation of human cells.
topic mitochondrial DNA
rare mutation
stem cells
breast cancer
mitochondrial tRNA
duplex sequencing
next generation sequencing
url https://www.mdpi.com/1422-0067/20/11/2813
work_keys_str_mv AT sujinkwon immortalizationofdifferentbreastepithelialcelltypesresultsindistinctmitochondrialmutagenesis
AT susanskim immortalizationofdifferentbreastepithelialcelltypesresultsindistinctmitochondrialmutagenesis
AT howardenebeck immortalizationofdifferentbreastepithelialcelltypesresultsindistinctmitochondrialmutagenesis
AT eunhyunahn immortalizationofdifferentbreastepithelialcelltypesresultsindistinctmitochondrialmutagenesis
_version_ 1724779768589582336

Similar Items