| Literature DB >> 31371824 |
Matteo Boretto1, Nina Maenhoudt2, Xinlong Luo3, Aurélie Hennes4, Bram Boeckx5,6, Bich Bui2,7, Ruben Heremans2,8,9, Lisa Perneel2, Hiroto Kobayashi2,10, Indra Van Zundert11, Hilde Brems12, Benoit Cox2, Marc Ferrante13, Hiroshi Uji-I11, Kian Peng Koh3, Thomas D'Hooghe8, Arne Vanhie4,14, Ignace Vergote8,9, Christel Meuleman4,14, Carla Tomassetti4,14, Diether Lambrechts5,6, Joris Vriens4, Dirk Timmerman8,9, Hugo Vankelecom15.
Abstract
Endometrial disorders represent a major gynaecological burden. Current research models fail to recapitulate the nature and heterogeneity of these diseases, thereby hampering scientific and clinical progress. Here we developed long-term expandable organoids from a broad spectrum of endometrial pathologies. Organoids from endometriosis show disease-associated traits and cancer-linked mutations. Endometrial cancer-derived organoids accurately capture cancer subtypes, replicate the mutational landscape of the tumours and display patient-specific drug responses. Organoids were also established from precancerous pathologies encompassing endometrial hyperplasia and Lynch syndrome, and inherited gene mutations were maintained. Endometrial disease organoids reproduced the original lesion when transplanted in vivo. In summary, we developed multiple organoid models that capture endometrial disease diversity and will provide powerful research models and drug screening and discovery tools.Entities:
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Year: 2019 PMID: 31371824 DOI: 10.1038/s41556-019-0360-z
Source DB: PubMed Journal: Nat Cell Biol ISSN: 1465-7392 Impact factor: 28.824