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.

Christopher Boniface,Carol Halsey,Christopher Deig,Nima Nabavizadeh,Michael B Heskett,Paul T Spellman,Charles R Thomas,Taylor Kelley

doi:10.3390/diagnostics11010073

Christopher Boniface, Carol Halsey + Show 6 more

Open Access

https://doi.org/10.3390/diagnostics11010073

Copy DOI

Journal: Diagnostics	Publication Date: Jan 5, 2021
Citations: 10	License type: CC BY 4.0

Affiliation: Oregon Health & Science University

Abstract

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 (n = 3) and rectal cancer (n = 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.

Highlights

Elevated circulating tumor DNA (ctDNA) Levels Are Associated with Recurrence in Rectal Adenocarcinoma with
Patient 1 is a 33 year old female who presented with cT3N1M0 distal rectal adenocarcinoma and enrolled on an unrelated phase II trial evaluating the efficacy of total neoadjuvant therapy followed by non-operative management for clinical complete responders based on MRI and endoscopy (NCT02008656) [13]
CtDNA levels decreased fivefold during four months of total neoadjuvant therapy (Figure 2A). She was without clinically detectable disease for six months following total neoadjuvant therapy and proceeded with non-operative management (NOM) per the trial; ctDNA levels remained elevated

Summary

Introduction

Circulating tumor DNA (ctDNA) has been extensively investigated for its diagnostic and prognostic utility as such a biomarker [4,5,6,7,8], the longitudinal application of ctDNA monitoring throughout multi-modality therapy Circulating tumor DNA (ctDNA) has been extensively investigated for its diagnostic and prognostic utility as such a biomarker [4,5,6,7,8], the longitudinal application of ctDNA monitoring throughout multi-modality therapy (systemic therapy,and/or radiotherapy, surgery) has been less extensively studied [4].ctDNA. Improved outcomes, insetting the neoadjuvant response (pCR) and improved outcomes, in theparticularly neoadjuvant for breast cancer [9,10]; feasibility of serial ctDNA measurements inmeasurements the neoadjuvant setting for breast cancerthe [9,10]; the feasibility of serial ctDNA in setting for rectal setting and esophageal has not been previously reported.

Objectives

Methods

Results

Conclusion