Cell-Free DNA Detection of Tumor Mutations in Heterogeneous, Localized Prostate Cancer Via Targeted, Multiregion Sequencing-Reference-Cited by-同舟云学术

Cell-Free DNA Detection of Tumor Mutations in Heterogeneous, Localized Prostate Cancer Via Targeted, Multiregion Sequencing

Published:2021-04 Issue:5 Volume: Page:710-725
ISSN:2473-4284
Container-title:JCO Precision Oncology
language:en
Short-container-title:JCO Precision Oncology

Author:

Chen Emmalyn¹^ORCID,Cario Clinton L.¹,Leong Lancelote¹,Lopez Karen²,Márquez César P.³⁴^ORCID,Li Patricia S.²^ORCID,Oropeza Erica²,Tenggara Imelda²,Cowan Janet²^ORCID,Simko Jeffry P.²⁵,Kageyama Robin⁶,Wells Daniel K.⁶,Chan June M.¹,Friedlander Terence³^ORCID,Aggarwal Rahul³,Paris Pamela L.²^ORCID,Feng Felix²,Carroll Peter R.²^ORCID,Witte John S.¹²^ORCID

Affiliation:

1. Department of Epidemiology and Biostatistics, University of California, San Francisco, CA

2. Department of Urology, Helen Diller Family Comprehensive Cancer Center, University of California, San Francisco, CA

3. Division of Hematology/Oncology, University of California, San Francisco, CA

4. School of Medicine, Stanford University, Stanford, CA

5. Department of Anatomic Pathology, University of California, San Francisco, CA

6. Parker Institute for Cancer Immunotherapy, San Francisco, CA

Abstract

PURPOSE Cell-free DNA (cfDNA) may allow for minimally invasive identification of biologically relevant genomic alterations and genetically distinct tumor subclones. Although existing biomarkers may detect localized prostate cancer, additional strategies interrogating genomic heterogeneity are necessary for identifying and monitoring aggressive disease. In this study, we aimed to evaluate whether circulating tumor DNA can detect genomic alterations present in multiple regions of localized prostate tumor tissue. METHODS Low-pass whole-genome and targeted sequencing with a machine-learning guided 2.5-Mb targeted panel were used to identify single nucleotide variants, small insertions and deletions (indels), and copy-number alterations in cfDNA. The majority of this study focuses on the subset of 21 patients with localized disease, although 45 total individuals were evaluated, including 15 healthy controls and nine men with metastatic castration-resistant prostate cancer. Plasma cfDNA was barcoded with duplex unique molecular identifiers. For localized cases, matched tumor tissue was collected from multiple regions (one to nine samples per patient) for comparison. RESULTS Somatic tumor variants present in heterogeneous tumor foci from patients with localized disease were detected in cfDNA, and cfDNA mutational burden was found to track with disease severity. Somatic tissue alterations were identified in cfDNA, including nonsynonymous variants in FOXA1, PTEN, MED12, and ATM. Detection of these overlapping variants was associated with seminal vesicle invasion ( P = .019) and with the number of variants initially found in the matched tumor tissue samples ( P = .0005). CONCLUSION Our findings demonstrate the potential of targeted cfDNA sequencing to detect somatic tissue alterations in heterogeneous, localized prostate cancer, especially in a setting where matched tumor tissue may be unavailable (ie, active surveillance or treatment monitoring).

Publisher

American Society of Clinical Oncology (ASCO)

Subject

Cancer Research,Oncology

Link

https://ascopubs.org/doi/pdfdirect/10.1200/PO.20.00428

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1. Re: Bernard Pope, Gahee Park, Edmund Lau, et al. Ultrasensitive Detection of Circulating Tumour DNA enriches for Patients with a Greater Risk of Recurrence of Clinically Prostate Cancer. Eur Urol 2024;85:407–10;European Urology Open Science;2024-09

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4. Early Plasma Circulating Tumor DNA as a Potential Biomarker of Disease Recurrence in Non-metastatic Prostate Cancer;Cancer Research and Treatment;2023-07-15

5. Liquid Biopsy in Diagnosis and Prognosis of Non-Metastatic Prostate Cancer;Biomedicines;2022-12-02