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Fragment Length of Circulating Tumor DNA
Fragment Length of Circulating Tumor DNA
by Hellwig, Sabine , Rostomily, Robert C. , Baker, Daniel N. , Welker, Noah C. , Shendure, Jay , Kitzman, Jacob O. , Gligorich, Keith M. , Underhill, Hunter R. , Bronner, Mary P. , Daza, Riza
in Alleles / Animals / Biology and life sciences / Biomarkers, Tumor - blood / Carcinoma, Hepatocellular - genetics / Carcinoma, Hepatocellular - metabolism / Cell Line, Tumor / Deoxyribonucleic acid / DNA / DNA sequencing / DNA, Neoplasm - blood / DNA, Neoplasm - genetics / Experiments / Genes / Genetic aspects / Glioblastoma - blood / Glioblastoma - genetics / Hep G2 Cells / Humans / Liver Neoplasms - genetics / Liver Neoplasms - metabolism / Lung cancer / Lung Neoplasms - genetics / Lung Neoplasms - metabolism / Magnetic Resonance Imaging / Male / Medicine and Health Sciences / Melanoma / Melanoma - genetics / Melanoma - metabolism / Metastasis / Methods / Mutation / Neoplasm Transplantation / Proto-Oncogene Proteins B-raf - genetics / Rats / Research and Analysis Methods / Studies / Tumors
2016
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Fragment Length of Circulating Tumor DNA
by Hellwig, Sabine , Rostomily, Robert C. , Baker, Daniel N. , Welker, Noah C. , Shendure, Jay , Kitzman, Jacob O. , Gligorich, Keith M. , Underhill, Hunter R. , Bronner, Mary P. , Daza, Riza
in Alleles / Animals / Biology and life sciences / Biomarkers, Tumor - blood / Carcinoma, Hepatocellular - genetics / Carcinoma, Hepatocellular - metabolism / Cell Line, Tumor / Deoxyribonucleic acid / DNA / DNA sequencing / DNA, Neoplasm - blood / DNA, Neoplasm - genetics / Experiments / Genes / Genetic aspects / Glioblastoma - blood / Glioblastoma - genetics / Hep G2 Cells / Humans / Liver Neoplasms - genetics / Liver Neoplasms - metabolism / Lung cancer / Lung Neoplasms - genetics / Lung Neoplasms - metabolism / Magnetic Resonance Imaging / Male / Medicine and Health Sciences / Melanoma / Melanoma - genetics / Melanoma - metabolism / Metastasis / Methods / Mutation / Neoplasm Transplantation / Proto-Oncogene Proteins B-raf - genetics / Rats / Research and Analysis Methods / Studies / Tumors
2016
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Fragment Length of Circulating Tumor DNA
Fragment Length of Circulating Tumor DNA
by Hellwig, Sabine , Rostomily, Robert C. , Baker, Daniel N. , Welker, Noah C. , Shendure, Jay , Kitzman, Jacob O. , Gligorich, Keith M. , Underhill, Hunter R. , Bronner, Mary P. , Daza, Riza
in Alleles / Animals / Biology and life sciences / Biomarkers, Tumor - blood / Carcinoma, Hepatocellular - genetics / Carcinoma, Hepatocellular - metabolism / Cell Line, Tumor / Deoxyribonucleic acid / DNA / DNA sequencing / DNA, Neoplasm - blood / DNA, Neoplasm - genetics / Experiments / Genes / Genetic aspects / Glioblastoma - blood / Glioblastoma - genetics / Hep G2 Cells / Humans / Liver Neoplasms - genetics / Liver Neoplasms - metabolism / Lung cancer / Lung Neoplasms - genetics / Lung Neoplasms - metabolism / Magnetic Resonance Imaging / Male / Medicine and Health Sciences / Melanoma / Melanoma - genetics / Melanoma - metabolism / Metastasis / Methods / Mutation / Neoplasm Transplantation / Proto-Oncogene Proteins B-raf - genetics / Rats / Research and Analysis Methods / Studies / Tumors
2016

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Mohammed Bin Rashid Library /
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Fragment Length of Circulating Tumor DNA
Fragment Length of Circulating Tumor DNA
Journal Article

Fragment Length of Circulating Tumor DNA

Hellwig, Sabine,
Rostomily, Robert C.,
Baker, Daniel N.,
Welker, Noah C.,
Shendure, Jay,
Kitzman, Jacob O.,
Gligorich, Keith M.,
Underhill, Hunter R.,
Bronner, Mary P.,
Daza, Riza
2016
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Overview
Malignant tumors shed DNA into the circulation. The transient half-life of circulating tumor DNA (ctDNA) may afford the opportunity to diagnose, monitor recurrence, and evaluate response to therapy solely through a non-invasive blood draw. However, detecting ctDNA against the normally occurring background of cell-free DNA derived from healthy cells has proven challenging, particularly in non-metastatic solid tumors. In this study, distinct differences in fragment length size between ctDNAs and normal cell-free DNA are defined. Human ctDNA in rat plasma derived from human glioblastoma multiforme stem-like cells in the rat brain and human hepatocellular carcinoma in the rat flank were found to have a shorter principal fragment length than the background rat cell-free DNA (134-144 bp vs. 167 bp, respectively). Subsequently, a similar shift in the fragment length of ctDNA in humans with melanoma and lung cancer was identified compared to healthy controls. Comparison of fragment lengths from cell-free DNA between a melanoma patient and healthy controls found that the BRAF V600E mutant allele occurred more commonly at a shorter fragment length than the fragment length of the wild-type allele (132-145 bp vs. 165 bp, respectively). Moreover, size-selecting for shorter cell-free DNA fragment lengths substantially increased the EGFR T790M mutant allele frequency in human lung cancer. These findings provide compelling evidence that experimental or bioinformatic isolation of a specific subset of fragment lengths from cell-free DNA may improve detection of ctDNA.
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Publisher
Public Library of Science,Public Library of Science (PLoS)
Subject

Alleles

/ Animals

/ Biology and life sciences

/ Biomarkers, Tumor - blood

/ Carcinoma, Hepatocellular - genetics

/ Carcinoma, Hepatocellular - metabolism

/ Cell Line, Tumor

/ Deoxyribonucleic acid

/ DNA

/ DNA sequencing

/ DNA, Neoplasm - blood

/ DNA, Neoplasm - genetics

/ Experiments

/ Genes

/ Genetic aspects

/ Glioblastoma - blood

/ Glioblastoma - genetics

/ Hep G2 Cells

/ Humans

/ Liver Neoplasms - genetics

/ Liver Neoplasms - metabolism

/ Lung cancer

/ Lung Neoplasms - genetics

/ Lung Neoplasms - metabolism

/ Magnetic Resonance Imaging

/ Male

/ Medicine and Health Sciences

/ Melanoma

/ Melanoma - genetics

/ Melanoma - metabolism

/ Metastasis

/ Methods

/ Mutation

/ Neoplasm Transplantation

/ Proto-Oncogene Proteins B-raf - genetics

/ Rats

/ Research and Analysis Methods

/ Studies

/ Tumors

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