Cell-Free DNA Kinetics in a Pre-Clinical Model of Head and Neck Cancer

Muhanna, Nidal; Grappa, Marco A. Di; Chan, Harley; Khan, Tahsin M.; Cheng, Jiang; Zheng, Yangqiao; Irish, Jonathan C.; Bratman, Scott V.

doi:10.1038/s41598-017-17079-6

Cited by 42 publications

(37 citation statements)

References 31 publications

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“…The estimated half-life of cfDNA in circulating blood varies from several minutes (e.g., 4 min after hemodialysis cessation) to 1-2 h. [103][104][105][106] Interestingly, clearance of fetal DNA from maternal blood occurs in a bi-phasic manner: first, a rapid phase occurs with a mean half-life of~10 min to 1 h; then, a second slow phase occurs with a mean half-life of~13 h. 107 The half-life of the ctDNA level after surgical tumor resection in a pre-clinical rabbit model of head and neck cancer was 23-52 min. 25 A serial analysis of ctDNA in patients with colorectal cancer showed a halflife of 114 min. 108 The short half-life of cfDNA is convenient for "real-time" analyses of cfDNA; it facilitates treatment response evaluations and dynamic tissue status assessments in various pathophysiological conditions; for example, tissue damage or regeneration.…”

Section: Clearance Of Cfdnamentioning

confidence: 99%

“…23,24 Some studies suggested that analyses of cfDNA outperformed instrumental methods (such as computed tomography), required a lower tumor burden, and prolonged the time window for adopting clinical decisions. 23,25 Studies of cfDNA in oncology are predominantly devoted to clinical applications of cfDNA as a tumor biomarker. An association of cfDNA level with treatment outcome, low invasiveness of an assay, implementation of high-throughput techniques make liquid biopsy using extracellular DNA an attractive candidate for a routine test in cancer management.…”

Section: Introductionmentioning

confidence: 99%

“…16,56,65,76 Longer DNA fragments (i.e., >10 kb) are considered to result from necrotic cell death; for example, from cells in necrotized parts of tumors. 25 Experiments in vitro have demonstrated that the amount of extracted DNA fragments depended on the type of necrosis-inducing agent applied. 77,78 Moreover, blood sampling can affect the type of cell death; indeed, the collection of serum stimulates a release of necrotic DNA from blood cells; this mechanism could account for the higher levels of total cfDNA found in serum compared to levels found in plasma samples.…”

Section: Introductionmentioning

confidence: 99%

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Life and death of circulating cell-free DNA

Kustanovich

Schwartz

Peretz

et al. 2019

Cancer Biology & Therapy

381

386

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Tumor-specific, circulating cell-free DNA in liquid biopsies is a promising source of biomarkers for minimally invasive serial monitoring of treatment responses in cancer management. We will review the current understanding of the origin of circulating cell-free DNA and different forms of DNA release (including various types of cell death and active secretion processes) and clearance routes. The dynamics of extracellular DNA in blood during therapy and the role of circulating DNA in pathophysiological processes (tumor-associated inflammation, NETosis, and pre-metastatic niche development) provide insights into the mechanisms that contribute to tumor development and metastases formation. Better knowledge of circulating tumor-specific cell-free DNA could facilitate the development of new therapeutic and diagnostic options for cancer management. ARTICLE HISTORY

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Section: Clearance Of Cfdnamentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Life and death of circulating cell-free DNA

Kustanovich

Schwartz

Peretz

et al. 2019

Cancer Biology & Therapy

381

386

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“…For the purpose of this study, plasma ctDNA was detected by means of a previously validated qPCR assay based on a 58-bp E6 assay derived from the E6 open reading frame (ORF). (14) From prior studies, the 58-bp E6 assay has shown to be sensitive enough to achieve robust detection of CRPV DNA sequences form as little as 3.7 pg of VX2 genomic DNA. Speci cities for this test also remain high showing no evidence in samples of rabbits that were not inoculated with VX2.…”

Section: Quanti Cation Of Ctdnamentioning

confidence: 99%

“…With our prior work in kinetics of ctDNA following surgery as well as a novel nanoparticle based detection of CTC in a preclinical model, we sought to develop a similar model to determine the kinetics of CTC and ctDNA in response to radiation therapy. (13,14) The establishment of such a preclinical model will allow for greater understanding of the kinetics of liquid biopsies in response to radiation, which may be of signi cance as a biomarker in further development of combination therapy.…”

Section: Introductionmentioning

confidence: 99%

Cell-Free DNA and Circulating Tumor Cell Kinetics in a Pre-Clinical Head and Neck Cancer Model Undergoing Radiation Therapy

Muhanna

Chan

et al. 2020

Preprint

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Background: Monitoring circulating tumor DNA (ctDNA) and circulating tumor cells (CTCs), known as liquid biopsies, continue to be developed as diagnostic and prognostic markers for a wide variety of cancer indications, mainly due to their minimally invasive nature and ability to offer a wide range of phenotypic and genetic information. While liquid biopsies maintain significant promising benefits, there is still limited information regarding the kinetics of ctDNA and CTCs following radiation therapy which remains a vital treatment modality in head and neck cancers. This study aims to describe the kinetics of ctDNA and CTCs following radiation exposure in a preclinical rabbit model with VX2 induced buccal carcinoma. Methods: Seven rabbits were inoculated with VX2 cells in the buccal mucosa and subjected to radiation. At selected time points, blood sampling was performed to monitor differing levels of ctDNA and CTC. Plasma ctDNA was measured with quantitative PCR for papillomavirus E6 while CTCs were quantified using an immunomagnetic nanoparticles within a microfluidic device. Comparisons of CTC detection with EpCAM compared to multiple surface markers (EGFR, HER2 and PSMA) was evaluated and correlated with the tumor size.Results: Plasma ctDNA reflects the overall tumor burden within the animal model. Analysis of correlations between ctDNA with tumor and lymph node volumes showed a positive correlation (R= 0.452 and R = 0.433 [p <0.05]), respectively. Over the course of treatment, ctDNA levels declined and quickly becomes undetectable following tumor eradication. While during the course of treatment, ctDNA levels were noted to rise particularly upon initiation of radiation following scheduled treatment breaks. Levels of CTCs were observed to increase 1 week following inoculation of tumor to the primary site. For CTC detection, the use of multiple surface markers showed a greater sensitivity when compared to detection using only EpCAM. Plasma CTC levels remained elevated following radiation therapy which may account for an increased shedding of CTCs following radiation.Conclusion: This study demonstrates the utility of ctDNA and CTCs detection in response to radiation treatment in a preclinical head and neck model, allowing for better understanding of liquid biopsy applications in both clinical practice and research development.

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