Harmonization and Standardization of Panel-Based Tumor Mutational Burden Measurement: Real-World Results and Recommendations of the Quality in Pathology Study

Research output: Contribution to journalResearch articleContributedpeer-review

Contributors

  • Albrecht Stenzinger - , Heidelberg University , Translational Lung Research Center Heidelberg (TLRC) - DZL Heidelberg (Author)
  • Volker Endris - , Heidelberg University  (Author)
  • Jan Budczies - , Heidelberg University  (Author)
  • Sabine Merkelbach-Bruse - , University of Cologne (Author)
  • Daniel Kazdal - , Heidelberg University , Translational Lung Research Center Heidelberg (TLRC) - DZL Heidelberg (Author)
  • Wolfgang Dietmaier - , University of Regensburg (Author)
  • Nicole Pfarr - , Technical University of Munich (Author)
  • Udo Siebolts - , Martin Luther University Hospital (Author)
  • Michael Hummel - , Charité – Universitätsmedizin Berlin (Author)
  • Sylvia Herold - , University Hospital Carl Gustav Carus Dresden (Author)
  • Johanna Andreas - , Institute for Hematopathology Hamburg GmbH (Author)
  • Martin Zoche - , University of Zurich (Author)
  • Lars Tögel - , Friedrich-Alexander University Erlangen-Nürnberg (Author)
  • Eugen Rempel - , Heidelberg University  (Author)
  • Jörg Maas - , Quality in Pathology (QuIP) (Author)
  • Diana Merino - , Friends of Cancer Research (Author)
  • Mark Stewart - , Friends of Cancer Research (Author)
  • Karim Zaoui - , Heidelberg University  (Author)
  • Matthias Schlesner - , German Cancer Research Center (DKFZ) (Author)
  • Hanno Glimm - , National Center for Tumor Diseases Dresden, University Hospital Carl Gustav Carus Dresden, German Cancer Research Center (DKFZ), German Cancer Consortium (DKTK) Partner Site Dresden (Author)
  • Stefan Fröhling - , German Cancer Research Center (DKFZ) (Author)
  • Jeff Allen - , Friends of Cancer Research (Author)
  • David Horst - , Charité – Universitätsmedizin Berlin (Author)
  • Gustavo Baretton - , Institute of Pathology, University Hospital Carl Gustav Carus Dresden (Author)
  • Claudia Wickenhauser - , Martin Luther University Hospital (Author)
  • Markus Tiemann - , Institute for Hematopathology Hamburg GmbH (Author)
  • Matthias Evert - , University of Regensburg (Author)
  • Holger Moch - , University of Zurich (Author)
  • Thomas Kirchner - , Ludwig Maximilian University of Munich (Author)
  • Reinhard Büttner - , University of Cologne (Author)
  • Peter Schirmacher - , Heidelberg University  (Author)
  • Andreas Jung - , Ludwig Maximilian University of Munich (Author)
  • Florian Haller - , Friedrich-Alexander University Erlangen-Nürnberg (Author)
  • Wilko Weichert - , Technical University of Munich (Author)
  • Manfred Dietel - , Quality in Pathology (QuIP) (Author)

Abstract

Introduction: Tumor mutational burden (TMB) is a quantitative assessment of the number of somatic mutations within a tumor genome. Immunotherapy benefit has been associated with TMB assessed by whole-exome sequencing (wesTMB) and gene panel sequencing (psTMB). The initiatives of Quality in Pathology (QuIP) and Friends of Cancer Research have jointly addressed the need for harmonization among TMB testing options in tissues. This QuIP study identifies critical sources of variation in psTMB assessment. Methods: A total of 20 samples from three tumor types (lung adenocarcinoma, head and neck squamous cell carcinoma, and colon adenocarcinoma) with available WES data were analyzed for psTMB using six panels across 15 testing centers. Interlaboratory and interplatform variation, including agreement on variant calling and TMB classification, were investigated. Bridging factors to transform psTMB to wesTMB values were empirically derived. The impact of germline filtering was evaluated. Results: Sixteen samples had low interlaboratory and interpanel psTMB variation, with 87.7% of pairwise comparisons revealing a Spearman's ρ greater than 0.6. A wesTMB cut point of 199 missense mutations projected to psTMB cut points between 7.8 and 12.6 mutations per megabase pair; the corresponding psTMB and wesTMB classifications agreed in 74.9% of cases. For three-tier classification with cut points of 100 and 300 mutations, agreement was observed in 76.7%, weak misclassification in 21.8%, and strong misclassification in 1.5% of cases. Confounders of psTMB estimation included fixation artifacts, DNA input, sequencing depth, genome coverage, and variant allele frequency cut points. Conclusions: This study provides real-world evidence that all evaluated panels can be used to estimate TMB in a routine diagnostic setting and identifies important parameters for reliable tissue TMB assessment that require careful control. As complex or composite biomarkers beyond TMB are likely playing an increasing role in therapy prediction, the efforts by QuIP and Friends of Cancer Research also delineate a general framework and blueprint for the evaluation of such assays.

Details

Original languageEnglish
Pages (from-to)1177-1189
Number of pages13
JournalJournal of thoracic oncology
Volume15
Issue number7
Publication statusPublished - Jul 2020
Peer-reviewedYes

External IDs

PubMed 32119917
ORCID /0009-0003-2782-8190/work/198593667

Keywords

Sustainable Development Goals

ASJC Scopus subject areas

Keywords

  • Gene panel, Immuno-oncology, Lung cancer, Quality assurance, Sequencing, TMB, Tumor mutational burden