Analytical and Clinical Validation of a Digital Sequencing Panel for Quantitative, Highly Accurate Evaluation of Cell-Free Circulating Tumor DNA

Lanman, Richard B.; Mortimer, Stefanie; Zill, Oliver A.; Sebisanovic, Dragan; López, René; Blau, Sibel; Collisson, Eric A.; Divers, Stephen G.; Hoon, Dave S.B.; Kopetz, Scott; Lee, Jeeyun; Nikolinakos, Petros; Baca, Arthur M.; Kermani, Bahram G.; Eltoukhy, Helmy; Talasaz, Amir Ali

doi:10.1371/journal.pone.0140712

Cited by 597 publications

(585 citation statements)

References 78 publications

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“…NGS is highthroughput sequencing that involves processing millions of DNA fragments. The ctDNA platform in our study utilized massively parallel and deep digital sequencing from a blood sample [7]. In contrast, tissue NGS involved parallel DNA sequencing from formalin-fixed or paraffin-embedded specimens.…”

Section: Introductionmentioning

confidence: 99%

Is Circulating Tumor DNA (Ctdna) Use Ready For Prime Time? Applications and Challenges of Ctdna in the Era of Precision Oncology

Davis¹,

Chae²,

Fj³

2017

Chemotherapy (Los Angel)

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Section: Introductionmentioning

confidence: 99%

Is Circulating Tumor DNA (Ctdna) Use Ready For Prime Time? Applications and Challenges of Ctdna in the Era of Precision Oncology

Davis¹,

Chae²,

Fj³

2017

Chemotherapy (Los Angel)

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“…20,26,27 This testing is often referred to as a liquid biopsy. The potential applications of sequencing ctDNA include screening or diagnosis of cancer, monitoring for progression or relapse, and guiding therapy for a patient with a known cancer diagnosis.…”

mentioning

confidence: 99%

“…Most research studies have evaluated the ability of ctDNA sequencing to detect somatic mutations in patients with known cancer and the ability to monitor disease. [26][27][28][29] Monitoring a known mutation by sequencing of ctDNA has been shown in several studies to correlate with relapse/progression of disease. 29,30 Also, using detection of mutations in ctDNA to help guide therapy for a patient with a known tumor has shown utility, for example, tyrosine kinase inhibitor response with epidermal growth factor receptor (EGFR)-activating mutations in lung cancer.…”

mentioning

confidence: 99%

“…29,30 Also, using detection of mutations in ctDNA to help guide therapy for a patient with a known tumor has shown utility, for example, tyrosine kinase inhibitor response with epidermal growth factor receptor (EGFR)-activating mutations in lung cancer. 26,27,31,32 Although ctDNA may have lower sensitivity for detecting mutations than testing tumor tissue, the most common clinical applications of ctDNA appear to be for patients with metastatic cancers when there is insufficient tissue for testing and a repeated biopsy would be associated with significant morbidity and mortality, and when testing of ctDNA is a reasonable alternative. 26,27,31 Using ctDNA to screen for or diagnose early-stage cancers is more problematic.…”

mentioning

confidence: 99%

“…26,27,31,32 Although ctDNA may have lower sensitivity for detecting mutations than testing tumor tissue, the most common clinical applications of ctDNA appear to be for patients with metastatic cancers when there is insufficient tissue for testing and a repeated biopsy would be associated with significant morbidity and mortality, and when testing of ctDNA is a reasonable alternative. 26,27,31 Using ctDNA to screen for or diagnose early-stage cancers is more problematic. 33 Most studies of patients with known cancer have not contained normal controls, but a limited number of targeted sequencing studies have shown some degree of mutation detection (false positives), albeit usually at a low level, in normal controls.…”

mentioning

confidence: 99%

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Review of Clinical Next-Generation Sequencing

Yohe

Thyagarajan

2017

Archives of Pathology &Amp; Laboratory Medicine

297

195

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Context.-Next-generation sequencing (NGS) is a technology being used by many laboratories to test for inherited disorders and tumor mutations. This technology is new for many practicing pathologists, who may not be familiar with the uses, methodology, and limitations of NGS.Objective.-To familiarize pathologists with several aspects of NGS, including current and expanding uses; methodology including wet bench aspects, bioinformatics, and interpretation; validation and proficiency; limitations; and issues related to the integration of NGS data into patient care.Data Sources.-The review is based on peer-reviewed literature and personal experience using NGS in a clinical setting at a major academic center.Conclusions.-The clinical applications of NGS will increase as the technology, bioinformatics, and resources evolve to address the limitations and improve quality of results. The challenge for clinical laboratories is to ensure testing is clinically relevant, cost-effective, and can be integrated into clinical care.( As with any new technology, the use of NGS in the clinical laboratory has evolved and will continue to evolve over time. New applications for the technology continue to be developed, new bioinformatics and wet bench techniques are being developed to address current limitations and improve performance, and new knowledge regarding interpretation of rare variants is being accumulated. This article is an overview of clinical NGS, including recent trends as well as evolution that will likely occur in the near future. The review is based on peer-reviewed literature and personal experience using NGS in a clinical setting at a major academic center. The Molecular Diagnostics Laboratory at

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Comparison of 2 Commercially Available Next-Generation Sequencing Platforms in Oncology

et al. 2017

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The growing use of next generation-sequencing to identify cancer-associated alterations as well as the increasing number of targeted drugs holds promise for better matching patients with cancer with effective therapies. The FoundationOne (F1; Foundation Medicine) test sequences clinical tumor samples to characterize the exons of 315 cancer-associated genes and introns from 28 genes involved in rearrangements. The Guardant360 (G360; Guardant Health) test uses cell-free circulating DNA from blood to sequence 70 genes. Both the F1 and G360 tests have high specificities (>99%) and somewhat lower sensitivities. 1,2 However, little is known about how different next-generation sequencing tests compare when used in the same patients with cancer. We compared reports from F1 and G360 testing in 9 patients from a community oncology practice to determine the level of concordance between the platforms. Methods | This study was approved by the University of Washington Institutional Review Board. Patients consented to the study, titled "A Tumor Crowd Modeling Platform for Patients with Cancer," via an online patient information statement. Nine patients (mean [SD] age, 61 [19] years; 2 men and 7 women) underwent both F1 and G360 testing from April 14, 2015, to January 30, 2016. Patient reports from results of F1 tumor and G360 circulating tumor DNA testing were examined to generate a list of all genomic alterations detected by either assay and to assess concordance between reports. Reports from results

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Analytical and Clinical Validation of a Digital Sequencing Panel for Quantitative, Highly Accurate Evaluation of Cell-Free Circulating Tumor DNA

Cited by 597 publications

References 78 publications

Is Circulating Tumor DNA (Ctdna) Use Ready For Prime Time? Applications and Challenges of Ctdna in the Era of Precision Oncology

Is Circulating Tumor DNA (Ctdna) Use Ready For Prime Time? Applications and Challenges of Ctdna in the Era of Precision Oncology

Review of Clinical Next-Generation Sequencing

Comparison of 2 Commercially Available Next-Generation Sequencing Platforms in Oncology

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