Diagnostics (Sep 2023)

Analytical Validation of an Immunohistochemical 7-Biomarker Prognostic Assay (immunoprint<sup>®</sup>) for Early-Stage Cutaneous Melanoma in Archival Tissue of Patients with AJCC v8 T2–T3 Disease

  • Mirjana Ziemer,
  • Beate Weidenthaler-Barth,
  • Philipp Gussek,
  • Maja Pfeiffer,
  • Johannes Kleemann,
  • Katrin Bankov,
  • Peter J. Wild,
  • Silke Seibold,
  • Priyavathi Sureshkumar,
  • Patricia Nickel,
  • Anton Strobel,
  • Markus Werner,
  • Stephan Grabbe

DOI
https://doi.org/10.3390/diagnostics13193096
Journal volume & issue
Vol. 13, no. 19
p. 3096

Abstract

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Selected patients with early-stage melanoma have a “hidden high risk” of poor oncologic outcomes. They might benefit from clinical trials, and ultimately, if warranted by trial results, judicious everyday use of adjuvant therapy. A promising tool to identify these individuals is the immunoprint® assay. This immunohistochemical 7-biomarker prognostic test was clinically validated in three independent cohorts (N = 762) to classify early-stage patients as high-risk or low-risk regarding melanoma recurrence and mortality. Using College of American Pathologists (CAP) recommendations, we analytically validated this assay in primary melanoma specimens (N = 20 patients). We assessed assay precision by determining consistency of risk classification under repeated identical conditions (repeatability) or across varying conditions (reproducibility), involving separate assay runs, operators (laboratory scientists), and/or observers (e.g., dermatopathologists). Reference classification was followed by five analytical validation phases: intra-run/intra-operator, intra-observer, inter-run, inter-operator, and inter-observer. Concordance of classifications in each phase was assessed via Fleiss’ kappa (primary endpoint) and percent agreement (secondary endpoint). Seven-marker signature classification demonstrated high consistency across validation categories (Fleiss’ kappa 0.864–1.000; overall percent agreement 95–100%), in 9/10 cases, exceeding, and in 1/10 cases, closely approaching, CAP’s recommended 0.9 level. The 7-marker assay has now been verified to provide excellent repeatability, reproducibility, and precision, besides having been clinically validated.

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