npj Precision Oncology (Feb 2024)

Genomic landscape of liquid biopsy mutations in TP53 and DNA damage genes in cancer patients

  • Damien Vasseur,
  • Ahmadreza Arbab,
  • Fabiola Giudici,
  • Christophe Marzac,
  • Stefan Michiels,
  • Marco Tagliamento,
  • Arnaud Bayle,
  • Cristina Smolenschi,
  • Madona Sakkal,
  • Mihaela Aldea,
  • Hela Sassi,
  • Filippo Gustavo Dall’Olio,
  • Noémie Pata-Merci,
  • Sophie Cotteret,
  • Alice Fiévet,
  • Nathalie Auger,
  • Luc Friboulet,
  • Francesco Facchinetti,
  • Arthur Géraud,
  • Santiago Ponce,
  • Antoine Hollebecque,
  • Benjamin Besse,
  • Jean Baptiste Micol,
  • Antoine Italiano,
  • Ludovic Lacroix,
  • Etienne Rouleau

DOI
https://doi.org/10.1038/s41698-024-00544-7
Journal volume & issue
Vol. 8, no. 1
pp. 1 – 10

Abstract

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Abstract Next-generation sequencing (NGS) assays based on plasma cell-free DNA (cfDNA) are increasingly used for clinical trials inclusion. Their optimized limit of detection applied to a large number of genes leads to the identification of mutations not confirmed in tissue. It becomes essential to describe the characteristics and consequences of these liquid biopsy-only mutations. In the STING protocol (Gustave Roussy, NCT04932525), 542 patients with advanced solid cancer had cfDNA-based and tissue-based NGS analysis (performed by FoundationOne® Liquid CDx and FoundationOne CDx™, respectively). Mutations identified in the liquid biopsy but not in the paired tissue were considered as liquid biopsy-only mutations irrespective of their variant allelic frequency (VAF). Out of 542 patients, 281 (51.8%) harbored at least one liquid biopsy-only mutation. These patients were significantly older, and more heavily pretreated. Liquid biopsy-only mutations occurring in TP53, and in DDR genes (ATM, CHEK2, ATR, BRCA2, and BRCA1) accounted for 90.8% of all the mutations. The median VAF of these mutations was generally low (0.37% and 0.40% for TP53 and DDR genes respectively). The variant type repartition depended on the gene. Liquid biopsy-only mutations affected hotspot in TP53 codon 273, 125, 195, 176, 237 or 280 and ATM codon 2891 and 3008. In a subset of 37 patients, 75.0%, 53.5% and 83.3% of the liquid biopsy-only mutations occurring respectively in ATM, TP53, and CHEK2 were confirmed in the matching whole blood sample. Although liquid biopsy-only mutations makes the interpretation of liquid biopsy results more complex, they have distinct characteristics making them more easily identifiable.