Therapeutic Advances in Medical Oncology (Sep 2021)

Not all 557/558 codons mutations have the same prognostic influence on recurrence-free survival: breaking the exon 11 mutations in gastrointestinal stromal tumors (GISTs)

  • Lorena Incorvaia,
  • Giuseppe Badalamenti,
  • Daniele Fanale,
  • Bruno Vincenzi,
  • Ida De Luca,
  • Laura Algeri,
  • Nadia Barraco,
  • Chiara Brando,
  • Annalisa Bonasera,
  • Marco Bono,
  • Marta Castiglia,
  • Daniela Cancelliere,
  • Massimiliano Cani,
  • Lidia Rita Corsini,
  • Alessia Fiorino,
  • Antonio Galvano,
  • Erika Pedone,
  • Alessandro Perez,
  • Alessia Pivetti,
  • Giuseppa Graceffa,
  • Gianni Pantuso,
  • Daniela Cabibi,
  • Antonio Russo,
  • Viviana Bazan

DOI
https://doi.org/10.1177/17588359211049779
Journal volume & issue
Vol. 13

Abstract

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Background: Although the gastrointestinal stromal tumor (GIST) genotype is not currently included in risk-stratification systems, a growing body of evidence shows that the pathogenic variant (PV) type and codon location hold a strong prognostic influence on recurrence-free survival (RFS). This information has particular relevance in the adjuvant setting, where an accurate prognostication could help to better identify high-risk tumors and guide clinical decision-making. Materials and Methods: Between January 2005 and December 2020, 96 patients with completely resected GISTs harboring a KIT proto-oncogene receptor tyrosine kinase ( KIT ) exon 11 PV were included in the study. We analyzed the type and codon location of the PV according to clinicopathological characteristics and clinical outcome; the metastatic sites in relapsed patients were also investigated. Results: Tumors harboring a KIT exon 11 deletion or deletion/insertion involving the 557 and/or 558 codons, showed a more aggressive clinical behavior compared with tumors carrying deletion/deletion/insertion in other codons, or tumors with duplication/insertion/single-nucleotide variant (SNV) (7-year RFS: 50% versus 73.1% versus 88.2%, respectively; p < 0.001). Notably, among 18 relapsed patients with 557 and/or 558 deletion or deletion/insertion, 14 patients (77.8%) harbored deletions simultaneously involving 557 and 558 codons, while only 4 patients (22.2%) harbored deletions involving only 1 of the 557/558 codons. Thus, when 557 or 558 deletions occurred separately, the tumor showed a prognostic behavior similar to the GIST carrying deletions outside the 557/558 position. Remarkably, patients with GISTs stratified as intermediate risk, but carrying the 557/558 deletion, showed a similar outcome to the high-risk patients with tumors harboring deletions in codons other than 557/558, or duplication/insertion/SNV. Conclusion: Our data support the inclusion of the PV type and codon location in routine risk prediction models, and suggest that intermediate-risk patients whose GISTs harbor 557/558 deletions may also need to be treated with adjuvant imatinib like the high-risk patients.