PLoS ONE (Jan 2024)

Optimising primary molecular profiling in non-small cell lung cancer.

  • R D Schouten,
  • I Schouten,
  • M M F Schuurbiers,
  • V van der Noort,
  • R A M Damhuis,
  • E H F M van der Heijden,
  • J A Burgers,
  • N P Barlo,
  • A S R van Lindert,
  • K W Maas,
  • J J G van den Brand,
  • A A J Smit,
  • J M W van Haarst,
  • B van der Maat,
  • E Schuuring,
  • H Blaauwgeers,
  • S M Willems,
  • K Monkhorst,
  • D van den Broek,
  • M M van den Heuvel

DOI
https://doi.org/10.1371/journal.pone.0290939
Journal volume & issue
Vol. 19, no. 7
p. e0290939

Abstract

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IntroductionMolecular profiling of NSCLC is essential for optimising treatment decisions, but often incomplete. We assessed the efficacy of protocolised molecular profiling in the current standard-of-care (SoC) in a prospective observational study in the Netherlands and measured the effect of providing standardised diagnostic procedures. We also explored the potential of plasma-based molecular profiling in the primary diagnostic setting.MethodsThis multi-centre prospective study was designed to explore the performance of current clinical practice during the run-in phase using local SoC tissue profiling procedures. The subsequent phase was designed to investigate the extent to which comprehensive molecular profiling (CMP) can be maximized by protocolising tumour profiling. Successful molecular profiling was defined as completion of at least EGFR and ALK testing. Additionally, PD-L1 tumour proportions scores were explored. Lastly, the additional value of centralised plasma-based testing for EGFR and KRAS mutations using droplet digital PCR was evaluated.ResultsTotal accrual was 878 patients, 22.0% had squamous cell carcinoma and 78.0% had non-squamous NSCLC. Stage I-III was seen in 54.0%, stage IV in 46.0%. Profiling of EGFR and ALK was performed in 69.9% of 136 patients included in the run-in phase, significantly more than real-world data estimates of 55% (pConclusionThis study shows a high success rate of tissue-based molecular profiling that was significantly improved by a protocolised approach. Tissue-based profiling remains unfeasible for a substantial proportion of patients. Combined analysis of tumour tissue and circulating tumour DNA is a promising approach to allow adequate molecular profiling of more patients.