Enhanced Risk Stratification of Smoldering Multiple Myeloma with Dynamic Biomarkers: A Multinational, Multicenter Study including 2,270 Participants (PANGEA 2.0)

  1. Floris Chabrun
  2. Daniel Schwartz
  3. Susanna Gentile
  4. Elias Mai
  5. Tulika Gupta
  6. Jacqueline Perry
  7. David Cordas Dos Santos
  8. Thomas Hielscher
  9. Annika Werly
  10. Sophia Schmidt
  11. Foteini Theodorakakou
  12. Despina Fotiou
  13. Christine Liacos
  14. Nikolaos Kanellias
  15. Noelia Gisbert
  16. Esperanza Martin-Sanchez
  17. Rosalinda Termini
  18. Johannes Waldschmidt
  19. Selina Chavda
  20. Louise Ainley
  21. Matteo Claudio Da Vià
  22. Claudio de Magistris
  23. Loredana Pettine
  24. Michael Timonian
  25. Jean-Baptiste Alberge
  26. Vidhi Patel
  27. Patrick Costello
  28. Catherine Tobia
  29. Sally Phan
  30. Jennifer Lamb
  31. Maria-Theresa Silverio
  32. Maya Davis
  33. Elizabeth O'Donnell
  34. Catherine Marinac
  35. Omar Nadeem
  36. Niccolo Bolli
  37. Kwee Yong
  38. Martin Kortüm
  39. Hermann Einsele
  40. Maria Victoria Mateos Manteca
  41. Shaji Kumar
  42. Jesus San Miguel
  43. Bruno Paiva
  44. Efstathis Kastritis
  45. Meletios Dimopoulos
  46. Marc Raab
  47. Lorenzo Trippa
  48. Irene Ghobrial
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Abstract

Accurate prediction of risk of progression from smoldering (SMM) to active multiple myeloma (MM) is paramount to individualized early therapeutic strategies with minimum risk of overtreatment. Current risk stratification models do not account for evolving biomarker trajectories. We assembled the largest cohort to date of 2,270 SMM patients from six international centers with longitudinal clinical and biological data to train and validate the PANGEA 2.0 risk models. Four evolving biomarkers were significantly associated with shorter time-to-progression: M-protein increase ≥0.2g/dL, involved:uninvolved serum free light chain ratio increase ≥20, creatinine increase >25%, and hemoglobin decrease ≥1.5g/dL. PANGEA 2.0 outperforms established models including the 20/2/20 and IMWG models by more accurately predicting progression (C-statistics=0.69–0.84), even without biomarker history (C-statistics=0.69–0.83) or recent bone marrow biopsy. PANGEA 2.0 is an easy-to-use, open-access tool (https://ghobrial.shinyapps.io/pangea_2_calculator) to improve and individualize SMM risk stratification. Validation tools are available to compare PANGEA 2.0 to established models (https://ghobrial.shinyapps.io/pangea_validation).

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