Facile detection of mitochondrial DNA mutations in tumors and bodily fluids

Makiko S. Fliss; Henning Usadel; Otàvia L. Caballero; Li Wu; Martin R. Buta; Scott M. Eleff; Jin Jen; David Sidransky

doi:10.1126/science.287.5460.2017

Facile detection of mitochondrial DNA mutations in tumors and bodily fluids

Makiko S. Fliss, Henning Usadel, Otàvia L. Caballero, Li Wu, Martin R. Buta, Scott M. Eleff, Jin Jen, David Sidransky

School of Medicine

Research output: Contribution to journal › Article › peer-review

669 Scopus citations

Abstract

Examination of human bladder, head and neck, and lung primary tumors revealed a high frequency of mitochondrial DNA (mtDNA) mutations. The majority of these somatic mutations were homoplasmic in nature, indicating that the mutant mtDNA became dominant in tumor cells. The mutated mtDNA was readily detectable in paired bodily fluids from each type of cancer and was 19 to 220 times as abundant as mutated nuclear p53 DNA. By virtue of their clonal nature and high copy number, mitochondrial mutations may provide a powerful molecular marker for noninvasive detection of cancer.

Original language	English (US)
Pages (from-to)	2017-2019
Number of pages	3
Journal	Science
Volume	287
Issue number	5460
DOIs	https://doi.org/10.1126/science.287.5460.2017
State	Published - Mar 17 2000

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title = "Facile detection of mitochondrial DNA mutations in tumors and bodily fluids",

abstract = "Examination of human bladder, head and neck, and lung primary tumors revealed a high frequency of mitochondrial DNA (mtDNA) mutations. The majority of these somatic mutations were homoplasmic in nature, indicating that the mutant mtDNA became dominant in tumor cells. The mutated mtDNA was readily detectable in paired bodily fluids from each type of cancer and was 19 to 220 times as abundant as mutated nuclear p53 DNA. By virtue of their clonal nature and high copy number, mitochondrial mutations may provide a powerful molecular marker for noninvasive detection of cancer.",

author = "Fliss, {Makiko S.} and Henning Usadel and Caballero, {Ot{\`a}via L.} and Li Wu and Buta, {Martin R.} and Eleff, {Scott M.} and Jin Jen and David Sidransky",

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T1 - Facile detection of mitochondrial DNA mutations in tumors and bodily fluids

AU - Fliss, Makiko S.

AU - Usadel, Henning

AU - Caballero, Otàvia L.

AU - Wu, Li

AU - Buta, Martin R.

AU - Eleff, Scott M.

AU - Jen, Jin

AU - Sidransky, David

PY - 2000/3/17

Y1 - 2000/3/17

N2 - Examination of human bladder, head and neck, and lung primary tumors revealed a high frequency of mitochondrial DNA (mtDNA) mutations. The majority of these somatic mutations were homoplasmic in nature, indicating that the mutant mtDNA became dominant in tumor cells. The mutated mtDNA was readily detectable in paired bodily fluids from each type of cancer and was 19 to 220 times as abundant as mutated nuclear p53 DNA. By virtue of their clonal nature and high copy number, mitochondrial mutations may provide a powerful molecular marker for noninvasive detection of cancer.

AB - Examination of human bladder, head and neck, and lung primary tumors revealed a high frequency of mitochondrial DNA (mtDNA) mutations. The majority of these somatic mutations were homoplasmic in nature, indicating that the mutant mtDNA became dominant in tumor cells. The mutated mtDNA was readily detectable in paired bodily fluids from each type of cancer and was 19 to 220 times as abundant as mutated nuclear p53 DNA. By virtue of their clonal nature and high copy number, mitochondrial mutations may provide a powerful molecular marker for noninvasive detection of cancer.

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VL - 287

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EP - 2019

JO - Science

JF - Science

IS - 5460

ER -

Facile detection of mitochondrial DNA mutations in tumors and bodily fluids

Abstract

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