Patient‐ and xenograft‐derived organoids recapitulate pediatric brain tumor features and patient treatments

Author:

Lago Chiara1ORCID,Federico Aniello23,Leva Gloria1ORCID,Mack Norman L23,Schwalm Benjamin23,Ballabio Claudio1ORCID,Gianesello Matteo1ORCID,Abballe Luana4,Giovannoni Isabella5ORCID,Reddel Sofia4,Rossi Sabrina5,Leone Nicolas5ORCID,Carai Andrea6,Mastronuzzi Angela4,Bisio Alessandra78ORCID,Soldano Alessia9ORCID,Quintarelli Concetta4,Locatelli Franco410ORCID,Kool Marcel231112ORCID,Miele Evelina4ORCID,Tiberi Luca1ORCID

Affiliation:

1. Armenise‐Harvard Laboratory of Brain Disorders and Cancer, CIBIO Trento Italy

2. Hopp Children's Cancer Center (KiTZ) Heidelberg Germany

3. Division of Paediatric Neurooncology German Cancer Research Center (DKFZ) and German Cancer Consortium (DKTK) Heidelberg Germany

4. Department of Onco‐Hematology, Cell and Gene Therapy, Bambino Gesù Children's Hospital Scientific Institute for Research, Hospitalization and Healthcare (IRCCS) Rome Italy

5. Pathology Unit Bambino Gesù Children's Hospital, IRCCS Rome Italy

6. Neurosurgery Unit, Department of Neurosciences Bambino Gesù Children's Hospital, IRCCS Rome Italy

7. Laboratory of Radiobiology, CIBIO Trento Italy

8. Trento Institute for Fundamental Physics and Application, TIFPA Trento Italy

9. Department of Neuroscience Scuola Internazionale Superiore di Studi Avanzati (SISSA) Trieste Italy

10. Catholic University of the Sacred Heart Rome Italy

11. Princess Máxima Center for Pediatric Oncology Utrecht The Netherlands

12. University Medical Center Utrecht, Utrecht University Utrecht The Netherlands

Abstract

AbstractBrain tumors are the leading cause of cancer‐related death in children. Experimental in vitro models that faithfully capture the hallmarks and tumor heterogeneity of pediatric brain cancers are limited and hard to establish. We present a protocol that enables efficient generation, expansion, and biobanking of pediatric brain cancer organoids. Utilizing our protocol, we have established patient‐derived organoids (PDOs) from ependymomas, medulloblastomas, low‐grade glial tumors, and patient‐derived xenograft organoids (PDXOs) from medulloblastoma xenografts. PDOs and PDXOs recapitulate histological features, DNA methylation profiles, and intratumor heterogeneity of the tumors from which they were derived. We also showed that PDOs can be xenografted. Most interestingly, when subjected to the same routinely applied therapeutic regimens, PDOs respond similarly to the patients. Taken together, our study highlights the potential of PDOs and PDXOs for research and translational applications for personalized medicine.

Funder

Fondazione Cassa Di Risparmio Di Trento E Rovereto

European Molecular Biology Organization

Fondazione Pezcoller

Fondazione Umberto Veronesi

Publisher

Springer Science and Business Media LLC

Subject

Molecular Medicine

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