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Circulating Tumor DNA Abundance and Potential Utility in De Novo Metastatic Prostate Cancer
Authors:Gillian Vandekerkhove  Werner J. Struss  Matti Annala  Heini M.L. Kallio  Daniel Khalaf  Evan W. Warner  Cameron Herberts  Elie Ritch  Kevin Beja  Yulia Loktionova  Antonio Hurtado-Coll  Ladan Fazli  Alan So  Peter C. Black  Matti Nykter  Teuvo Tammela  Kim N. Chi  Martin E. Gleave  Alexander W. Wyatt
Affiliation:1. Department of Urologic Sciences, Vancouver Prostate Centre, University of British Columbia, Vancouver, Canada;2. Prostate Cancer Research Center, Faculty of Medicine and Life Sciences and BioMediTech Institute, University of Tampere, Tampere, Finland;3. Department of Medical Oncology, British Columbia Cancer Agency, Vancouver, Canada
Abstract:

Background

Several systemic therapeutic options exist for metastatic castrate-sensitive prostate cancer (mCSPC). Circulating tumor DNA (ctDNA) can molecularly profile metastatic castration-resistant prostate cancer and can influence decision-making, but remains untested in mCSPC.

Objective

To determine ctDNA abundance at de novo mCSPC diagnosis and whether ctDNA provides complementary clinically relevant information to a prostate biopsy.

Design, setting, and participants

We collected plasma cell-free DNA (cfDNA) from 53 patients newly diagnosed with mCSPC and, where possible, during treatment. Targeted sequencing was performed on cfDNA and DNA from diagnostic prostate tissue.

Results and limitations

The median ctDNA fraction was 11% (range 0–84%) among untreated patients but was lower (1.0%, range 0-51%) among patients after short-term (median 22 d) androgen deprivation therapy (ADT). TP53 mutations and DNA repair defects were identified in 47% and 21% of the cohort, respectively. The concordance for mutation detection in matched samples was 80%. Combined ctDNA and tissue analysis identified potential driver alterations in 94% of patients, whereas ctDNA or prostate biopsy alone was insufficient in 19 cases (36%). Limitations include the use of a narrow gene panel and undersampling of primary disease by prostate biopsy.

Conclusions

ctDNA provides additional information to a prostate biopsy in men with de novo mCSPC, but ADT rapidly reduces ctDNA availability. Primary tissue and ctDNA share relevant somatic alterations, suggesting that either is suitable for molecular subtyping in de novo mCSPC. The optimal approach for biomarker development should utilize both a tissue and liquid biopsy at diagnosis, as neither captures clinically relevant somatic alterations in all patients.

Patient summary

In men with advanced prostate cancer, tumor DNA shed into the bloodstream can be measured via a blood test. The information from this test provides complementary information to a prostate needle biopsy and could be used to guide management strategies.Sequencing data were deposited in the European Genome-phenome Archive (EGA) under study identifier EGAS00001003351.
Keywords:Circulating tumor DNA  Cell-free DNA  Androgen deprivation therapy  Castration-sensitive  DNA repair  Liquid biopsy  Precision oncology  Sequencing  Tissue biopsy
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