Cancers (Dec 2023)

Evaluation of the Aggressive-Variant Prostate Cancer Molecular Signature in Clinical Laboratory Improvement Amendments (CLIA) Environments

  • Paul V. Viscuse,
  • Rebecca S. Slack-Tidwell,
  • Miao Zhang,
  • Prih Rohra,
  • Keyi Zhu,
  • F. Anthony San Lucas,
  • Eric Konnick,
  • Patrick G. Pilie,
  • Bilal Siddiqui,
  • Christopher J. Logothetis,
  • Paul Corn,
  • Sumit K. Subudhi,
  • Colin C. Pritchard,
  • Rama Soundararajan,
  • Ana Aparicio

DOI
https://doi.org/10.3390/cancers15245843
Journal volume & issue
Vol. 15, no. 24
p. 5843

Abstract

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Aggressive-variant prostate cancers (AVPCs) are a subset of metastatic castrate-resistant prostate cancers (mCRPCs) characterized by defects in ≥ two of three of TP53, RB1, and PTEN (AVPCm), a profile linked to lineage plasticity, androgen indifference, and platinum sensitivity. Men with mCRPC undergoing biopsies for progression were assessed for AVPCm using immunohistochemistry (IHC), next-generation sequencing (NGS) of solid tumor DNA (stDNA), and NGS of circulating tumor DNA (ctDNA) assays in CLIA-certified labs. Biopsy characteristics, turnaround times, inter-reader concordance, and inter-assay concordance were assessed. AVPCm was detected in 13 (27%) patients via IHC, two (6%) based on stDNA, and seven (39%) based on ctDNA. The concordance of the IHC reads between pathologists was variable. IHC had a higher detection rate of AVPCm+ tumors with the shortest turnaround times. stDNA had challenges with copy number loss detection, limiting its detection rate. ctDNA detected the greatest proportion of AVPCm+ tumors but had a low tumor content in two thirds of patients. These data show the operational characteristics of AVPCm detection using various assays, and inform trial design using AVPCm as a criterion for patient selection or stratification.

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