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Somatic mitochondrial DNA (mtDNA) mutations in papillary thyroid carcinomas and differential mtDNA sequence variants in cases with thyroid tumours

Oncogene volume 19, pages 2060–2066 (2000)Cite this article

Abstract

Somatic mutations in mtDNA have recently been identified in colorectal tumours. Studies of oncocytic tumours have led to hypotheses which propose that defects in oxidative phosphorylation may result in a compensatory increase in mitochondrial replication and/or gene expression. Mutational analysis of mtDNA in thyroid neoplasia, which is characterised by increased numbers of mitochondria and is also one of the most common sites of oncocytic tumours. has been limited to date. Using the recently developed technique of two-dimensional gene scanning, we have successfully examined 21 cases of thyroid tumours, six cases of non-neoplastic thyroid pathology, 30 population controls, nine foetal thyroid tissues and nine foetal tissues of non-thyroid origin, either kidney or liver. We have identified three different somatic mutations (23%) in papillary thyroid carcinomas. In addition, we have found significant differential distributions of mtDNA sequence variants between thyroid carcinomas and controls. Interestingly, these variants appear to be more frequent in the genes which encode complex I of the mitochondrial electron transport chain compared to normal population controls. These findings suggest first, that somatic mtDNA mutations may be involved in thyroid tumorigenesis and second, that the accumulation of certain non-somatic variants may be related to tumour progression in the thyroid.

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Acknowledgements

JJ Yeh thanks James Becker for his continued support. The authors wish to acknowledge Jennifer B Kum, Sean McGrath and Wendy M Smith for technical advice. Partially funded by P30CA16058 from the National Cancer Institute (Ohio State University Comprehensive Cancer Center), a Boston University School of Medicine Surgical Research Fellowship (to JJ Yeh), and generous gifts from the Brown and Abrams families (to C Eng). PLM Dahia is a recipient of a postdoctoral fellowship from the Susan G Komen Breast Cancer Research Foundation (to C Eng).

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Authors and Affiliations

  1. Clinical Cancer Genetics and Human Cancer Genetics Programs, Ohio State University Comprehensive Cancer Center, 690C Medical Research Facility, 420 W 12th Avenue, Columbus, 43210, Ohio, OH, USA

    Jen Jen Yeh, Patricia LM Dahia & Charis Eng

  2. Charles A Dana Human Cancer Genetics Unit, Dana-Farber Cancer Institute, Boston, 02115, Massachusetts, MA, USA

    Jen Jen Yeh & Patricia LM Dahia

  3. Department of Biostatics, Dana-Farber Cancer Institute, Boston, 02115, Massachusetts, MA, USA

    Kathryn L Lunetta

  4. Institute for Drug Development, San Antonio Cancer Institute, San-Antonio, Texas, TX, USA

    Nathalie J van Orsouw & Jan Vijg

  5. Department of Surgery, Brigham and Women's Hospital, Boston, 02115, Massachusetts, MA, USA

    Francis D Moore Jr

  6. Department of Pathology, Brigham and Women's Hospital, Boston, 02115, Massachusetts, MA, USA

    George L Mutter

  7. Department of Medicine, Harvard Medical School, Harvard School of Public Health, Boston, 02115, Massachusetts, MA, USA

    Jen Jen Yeh & Patricia LM Dahia

  8. Department of Surgery, Harvard Medical School, Boston, 02115, Massachusetts, MA, USA

    Francis D Moore Jr

  9. Department of Pathology, Harvard Medical School, Boston, 02115, Massachusetts, MA, USA

    George L Mutter

  10. Harvard School of Public Health, Boston, 02115, Massachusetts, MA, USA

    Kathryn L Lunetta

  11. Department of Surgery, Boston University School of Medicine, Boston, 02114, Massachusetts, MA, USA

    Jen Jen Yeh

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  1. Jen Jen Yeh
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Yeh, J., Lunetta, K., van Orsouw, N. et al. Somatic mitochondrial DNA (mtDNA) mutations in papillary thyroid carcinomas and differential mtDNA sequence variants in cases with thyroid tumours. Oncogene 19, 2060–2066 (2000). https://doi.org/10.1038/sj.onc.1203537

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  • DOI: https://doi.org/10.1038/sj.onc.1203537

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