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. 2020 Nov:4:882-897.
doi: 10.1200/PO.19.00388.

Genomic Profiles of De Novo High- and Low-Volume Metastatic Prostate Cancer: Results From a 2-Stage Feasibility and Prevalence Study in the STAMPEDE Trial

Clare Gilson  1 Fiona Ingleby  1 Duncan C Gilbert  1 Marina A Parry  2 Nafisah B Atako  1 Adnan Ali  3 Alex Hoyle  3   4 Noel W Clarke  3   4 Melissa Gannon  1 Chris Wanstall  1 Christopher Brawley  1 Malcolm D Mason  5 Zafar Malik  6 Andrew Simmons  7 Andrea Loehr  7 Alison Parry-Jones  5 Rosalind Eeles  8   9 Zsofia Kote-Jarai  9 Nicholas D James  9 Claire Amos  1 Mahesh K B Parmar  1 Ruth E Langley  1 Matthew R Sydes  1 Gerhardt Attard  2 Simon Chowdhury  10 STAMPEDE Investigators
Affiliations

Genomic Profiles of De Novo High- and Low-Volume Metastatic Prostate Cancer: Results From a 2-Stage Feasibility and Prevalence Study in the STAMPEDE Trial

Clare Gilson et al. JCO Precis Oncol. 2020 Nov.

Abstract

Purpose: The STAMPEDE trial recruits men with newly diagnosed, high-risk, hormone-sensitive prostate cancer. To ascertain the feasibility of targeted next-generation sequencing (tNGS) and the prevalence of baseline genomic aberrations, we sequenced tumor and germline DNA from patients with metastatic prostate cancer (mPCa) starting long-term androgen-deprivation therapy (ADT).

Methods: In a 2-stage approach, archival, formalin-fixed, paraffin-embedded (FFPE) prostate tumor core biopsy samples were retrospectively subjected to 2 tNGS assays. Prospective enrollment enabled validation using tNGS in tumor and germline DNA.

Results: In stage 1, tNGS data were obtained from 185 tumors from 287 patients (65%); 98% had de novo mPCa. We observed PI3K pathway aberrations in 43%, due to PTEN copy-number loss (34%) and/or activating mutations in PIK3 genes or AKT (18%) and TP53 mutation or loss in 33%. No androgen receptor (AR) aberrations were detected; RB1 loss was observed in < 1%. In stage 2, 93 (92%) of 101 FFPE tumors (biopsy obtained within 8 months) were successfully sequenced prospectively. The prevalence of DNA damage repair (DDR) deficiency was 14% (somatic) and 5% (germline). BRCA2 mutations and mismatch repair gene mutations were exclusive to high-volume disease. Aberrant DDR (22% v 15%), Wnt pathway (16% v 4%), and chromatin remodeling (16% v 8%) were all more common in high-volume compared with low-volume disease, but the small numbers limited statistical comparisons.

Conclusion: Prospective genomic characterization is feasible using residual diagnostic tumor samples and reveals that the genomic landscapes of de novo high-volume mPCa and advanced metastatic prostate cancer have notable similarities (PI3K pathway, DDR, Wnt, chromatin remodeling) and differences (AR, RB1). These results will inform the design and conduct of biomarker-directed trials in men with metastatic hormone-sensitive prostate cancer.

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