Molecular characterization informs prognosis in patients with localized Ewing sarcoma: A report from the Children’s Oncology Group

  1. Riaz Gillani
  2. David S. Shulman
  3. Natalie J. DelRocco
  4. Kelly Klega
  5. Ruxu Han
  6. Mark D. Krailo
  7. Jonathan C. Slack
  8. Mohammad Tanhaemami
  9. Abigail Ward
  10. Victoria Bainer
  11. Cora Ricker
  12. Josee Sparks
  13. Kelly M. Bailey
  14. Damon R. Reed
  15. Steven G. DuBois
  16. Patrick Leavey
  17. Leo Mascarenhas
  18. Patrick J. Grohar
  19. Alanna J. Church
  20. Brian D. Crompton
  21. Katherine A. Janeway
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Abstract

PURPOSE

Identification of discrete sub-groups associated with treatment response and resistance in localized Ewing sarcoma (EWS) remains a challenge. The primary objective of the Children’s Oncology Group biology study AEWS18B1-Q was to perform molecular characterization of a large cohort of patients with localized Ewing sarcoma treated on prospective trials with modern standard of care therapy.

METHODS

We analyzed clinical and molecular features from patients with localized EWS enrolled on AEWS0031, AEWS1031, or INT-0154 frontline trials. All patients had available FFPE tissue, frozen tissue, or whole-genome amplified material. Sequencing was performed for identification of canonical fusions, recurrent copy number alterations (CNAs), and alterations in TP53 and STAG2 . Where available, tissue was analyzed for loss of STAG2 protein expression. Molecular features were evaluated for their association with cumulative incidence of relapse in univariate and multivariable analyses.

RESULTS

Three hundred and fifty-one cases had sufficient tissue, which in most cases was extracted from two FFPE slides. EWS canonical fusions were identified in 282 cases (80.3%). Pathogenic mutations in TP53 and STAG2 were identified in 5.1% and 7.6% of cases, respectively and 63.1% of cases were found to have recurrent CNAs. In univariate analysis, there was an increased cumulative incidence of relapse in patients with TP53 mutation (5-year cumulative incidence of relapse 43%, CI [17%, 67%] vs. 22%, CI [17%, 27%]; Gray’s test P = 0.039), STAG2 mutation (53%, CI [29%, 73%] vs. 21%, CI [16%, 26%]; P < 0.001), and recurrent CNAs (30%, CI [22%, 37%] vs. 16%, CI [9%, 24%]; P = 0.005). In a multivariable analysis, STAG2 mutation was the only molecular biomarker that remained prognostic.

CONCLUSION

This is a prospective validation of the molecular prognostic features of localized EWS receiving standard of care therapy on therapeutic clinical trials. Building on prior work, patients with STAG2 mutations were at high risk of relapse.

CONTEXT

Key Objective

To determine if molecular features can identify clinically relevant disease sub-groups applicable to frontline clinical trial design among patients with localized Ewing sarcoma.

Knowledge Generated

Among 351 patients with localized Ewing sarcoma treated on prospective trials, canonical fusions were identified in 80% of cases. In a multivariable analysis of patients with genomically defined Ewing sarcoma, the presence of STAG2 mutations identified a high-risk population.

Relevance (added by Associate Editor)

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  1. Version published to 10.1101/2025.01.20.25320840v1 on medRxiv