Mesenchymal tumor organoid models recapitulate rhabdomyosarcoma subtypes

  1. Michael T. Meister
  2. Marian J. A. Groot Koerkamp
  3. Terezinha de Souza
  4. Willemijn B. Breunis
  5. Ewa Frazer-Mendelewska
  6. Mariël Brok
  7. Jeff DeMartino
  8. Freek Manders
  9. Camilla Calandrini
  10. Hinri H. D. Kerstens
  11. Alex Janse
  12. M. Emmy M. Dolman
  13. Selma Eising
  14. Karin P. S. Langenberg
  15. Marc van Tuil
  16. Rutger R. G. Knops
  17. Sheila Terwisscha van Scheltinga
  18. Laura S. Hiemcke-Jiwa
  19. Uta Flucke
  20. Johannes H. M. Merks
  21. Max M. van Noesel
  22. Bastiaan B. J. Tops
  23. Jayne Y. Hehir-Kwa
  24. Patrick Kemmeren
  25. Jan J. Molenaar
  26. Marc van de Wetering
  27. Ruben van Boxtel
  28. Jarno Drost
  29. Frank C. P. Holstege
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Abstract

Rhabdomyosarcomas (RMS) are mesenchyme-derived tumors and the most common childhood soft tissue sarcomas. Treatment is intense, with a nevertheless poor prognosis for high-risk patients. Discovery of new therapies would benefit from additional preclinical models. Here we describe the generation of a collection of pediatric RMS tumor organoid (tumoroid) models comprising all major subtypes. For aggressive tumors, tumoroid models can often be established within four to eight weeks, indicating the feasibility of personalized drug screening. Molecular, genetic and histological characterization show that the models closely resemble the original tumors, with genetic stability over extended culture periods of up to six months. Importantly, drug screening reflects established sensitivities and the models can be modified by CRISPR/Cas9 withTP53knockout in an embryonal RMS model resulting in replicative stress drug sensitivity. Tumors of mesenchymal origin can therefore be used to generate organoid models, relevant for a variety of preclinical and clinical research questions.

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