The Feasibility of Patient-Specific Circulating Tumor DNA Monitoring throughout Multi-Modality Therapy for Locally Advanced Esophageal and Rectal Cancer: A Potential Biomarker for Early Detection of Subclinical Disease

The Feasibility of Patient-Specific Circulating Tumor DNA Monitoring throughout Multi-Modality Therapy for Locally Advanced Esophageal and Rectal Cancer: A Potential Biomarker for Early Detection of Subclinical Disease

As non-operative management (NOM) of esophageal and rectal cancer is becoming more prevalent, blood-biomarkers such as circulating tumor DNA (ctDNA) may provide clinical information in addition to endoscopy and imaging to aid in treatment decisions following chemotherapy and radiation therapy. In th...

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Main Authors: Christopher Boniface, Christopher Deig, Carol Halsey, Taylor Kelley, Michael B. Heskett, Charles R. Thomas, Paul T. Spellman, Nima Nabavizadeh
Format: Article
Language:English
Published: MDPI AG 2021-01-01
Series:Diagnostics
Subjects:
liquid biopsy
ctDNA
cell free DNA
non-operative management
neoadjuvant therapy
Online Access:https://www.mdpi.com/2075-4418/11/1/73
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spelling doaj-d6974b3f09344d7eb288b6b717e9695e2021-01-06T00:02:17ZengMDPI AGDiagnostics2075-44182021-01-0111737310.3390/diagnostics11010073The Feasibility of Patient-Specific Circulating Tumor DNA Monitoring throughout Multi-Modality Therapy for Locally Advanced Esophageal and Rectal Cancer: A Potential Biomarker for Early Detection of Subclinical DiseaseChristopher Boniface0Christopher Deig1Carol Halsey2Taylor Kelley3Michael B. Heskett4Charles R. Thomas5Paul T. Spellman6Nima Nabavizadeh7Cancer Early Detection Advanced Research (CEDAR) Center, Division of Oncological Sciences, Knight Cancer Institute, Oregon Health & Science University (OHSU), 2720 SW Moody Ave., Portland, OR 97201, USADepartment of Radiation Medicine, Oregon Health & Science University (OHSU), 3181 SW Sam Jackson Park Rd, KPV4, Portland, OR 97239, USADepartment of Molecular and Medical Genetics, Oregon Health & Science University (OHSU) School of Medicine, 3181 SW Sam Jackson Park Rd, Portland, OR 97239, USADepartment of Molecular and Medical Genetics, Oregon Health & Science University (OHSU) School of Medicine, 3181 SW Sam Jackson Park Rd, Portland, OR 97239, USADepartment of Molecular and Medical Genetics, Oregon Health & Science University (OHSU) School of Medicine, 3181 SW Sam Jackson Park Rd, Portland, OR 97239, USADepartment of Radiation Medicine, Oregon Health & Science University (OHSU), 3181 SW Sam Jackson Park Rd, KPV4, Portland, OR 97239, USACancer Early Detection Advanced Research (CEDAR) Center, Division of Oncological Sciences, Knight Cancer Institute, Oregon Health & Science University (OHSU), 2720 SW Moody Ave., Portland, OR 97201, USADepartment of Radiation Medicine, Oregon Health & Science University (OHSU), 3181 SW Sam Jackson Park Rd, KPV4, Portland, OR 97239, USAAs non-operative management (NOM) of esophageal and rectal cancer is becoming more prevalent, blood-biomarkers such as circulating tumor DNA (ctDNA) may provide clinical information in addition to endoscopy and imaging to aid in treatment decisions following chemotherapy and radiation therapy. In this feasibility study, we prospectively collected plasma samples from locally advanced esophageal (<i>n</i> = 3) and rectal cancer (<i>n</i> = 2) patients undergoing multimodal neoadjuvant therapy to assess the feasibility of serial ctDNA monitoring throughout neoadjuvant therapy. Using the Dual-Index Degenerate Adaptor-Sequencing (DIDA-Seq) error-correction method, we serially interrogated plasma cell-free DNA at 28–41 tumor-specific genomic loci throughout therapy and in surveillance with an average limit of detection of 0.016% mutant allele frequency. In both rectal cancer patients, ctDNA levels were persistently elevated following total neoadjuvant therapy with eventual detection of clinical recurrence prior to salvage surgery. Among the esophageal cancer patients, ctDNA levels closely correlated with tumor burden throughout and following neoadjuvant therapy, which was associated with a pathologic complete response in one patient. In this feasibility study, patient- and tumor-specific ctDNA levels correlated with clinical outcomes throughout multi-modality therapy suggesting that serial monitoring of patient ctDNA has the potential to serve as a highly sensitive and specific biomarker to risk-stratify esophageal and rectal cancer patients eligible for NOM. Further prospective investigation is warranted.https://www.mdpi.com/2075-4418/11/1/73liquid biopsyctDNAcell free DNAnon-operative managementneoadjuvant therapy
collection DOAJ
language English
format Article
sources DOAJ
author Christopher Boniface
Christopher Deig
Carol Halsey
Taylor Kelley
Michael B. Heskett
Charles R. Thomas
Paul T. Spellman
Nima Nabavizadeh
spellingShingle Christopher Boniface
Christopher Deig
Carol Halsey
Taylor Kelley
Michael B. Heskett
Charles R. Thomas
Paul T. Spellman
Nima Nabavizadeh
The Feasibility of Patient-Specific Circulating Tumor DNA Monitoring throughout Multi-Modality Therapy for Locally Advanced Esophageal and Rectal Cancer: A Potential Biomarker for Early Detection of Subclinical Disease
Diagnostics
liquid biopsy
ctDNA
cell free DNA
non-operative management
neoadjuvant therapy
author_facet Christopher Boniface
Christopher Deig
Carol Halsey
Taylor Kelley
Michael B. Heskett
Charles R. Thomas
Paul T. Spellman
Nima Nabavizadeh
author_sort Christopher Boniface
title The Feasibility of Patient-Specific Circulating Tumor DNA Monitoring throughout Multi-Modality Therapy for Locally Advanced Esophageal and Rectal Cancer: A Potential Biomarker for Early Detection of Subclinical Disease
title_short The Feasibility of Patient-Specific Circulating Tumor DNA Monitoring throughout Multi-Modality Therapy for Locally Advanced Esophageal and Rectal Cancer: A Potential Biomarker for Early Detection of Subclinical Disease
title_full The Feasibility of Patient-Specific Circulating Tumor DNA Monitoring throughout Multi-Modality Therapy for Locally Advanced Esophageal and Rectal Cancer: A Potential Biomarker for Early Detection of Subclinical Disease
title_fullStr The Feasibility of Patient-Specific Circulating Tumor DNA Monitoring throughout Multi-Modality Therapy for Locally Advanced Esophageal and Rectal Cancer: A Potential Biomarker for Early Detection of Subclinical Disease
title_full_unstemmed The Feasibility of Patient-Specific Circulating Tumor DNA Monitoring throughout Multi-Modality Therapy for Locally Advanced Esophageal and Rectal Cancer: A Potential Biomarker for Early Detection of Subclinical Disease
title_sort feasibility of patient-specific circulating tumor dna monitoring throughout multi-modality therapy for locally advanced esophageal and rectal cancer: a potential biomarker for early detection of subclinical disease
publisher MDPI AG
series Diagnostics
issn 2075-4418
publishDate 2021-01-01
description As non-operative management (NOM) of esophageal and rectal cancer is becoming more prevalent, blood-biomarkers such as circulating tumor DNA (ctDNA) may provide clinical information in addition to endoscopy and imaging to aid in treatment decisions following chemotherapy and radiation therapy. In this feasibility study, we prospectively collected plasma samples from locally advanced esophageal (<i>n</i> = 3) and rectal cancer (<i>n</i> = 2) patients undergoing multimodal neoadjuvant therapy to assess the feasibility of serial ctDNA monitoring throughout neoadjuvant therapy. Using the Dual-Index Degenerate Adaptor-Sequencing (DIDA-Seq) error-correction method, we serially interrogated plasma cell-free DNA at 28–41 tumor-specific genomic loci throughout therapy and in surveillance with an average limit of detection of 0.016% mutant allele frequency. In both rectal cancer patients, ctDNA levels were persistently elevated following total neoadjuvant therapy with eventual detection of clinical recurrence prior to salvage surgery. Among the esophageal cancer patients, ctDNA levels closely correlated with tumor burden throughout and following neoadjuvant therapy, which was associated with a pathologic complete response in one patient. In this feasibility study, patient- and tumor-specific ctDNA levels correlated with clinical outcomes throughout multi-modality therapy suggesting that serial monitoring of patient ctDNA has the potential to serve as a highly sensitive and specific biomarker to risk-stratify esophageal and rectal cancer patients eligible for NOM. Further prospective investigation is warranted.
topic liquid biopsy
ctDNA
cell free DNA
non-operative management
neoadjuvant therapy
url https://www.mdpi.com/2075-4418/11/1/73
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