Clinical application of a lung cancer organoid (tumoroid) culture system
Abstract Despite high expectations for lung tumoroids, they have not been applied in the clinic due to the difficulty of their long-term culture. Here, however, using AO (airway organoid) media developed by the Clevers laboratory, we succeeded in generating 3 lung tumoroid lines for long-term cultur...
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Series: | npj Precision Oncology |
Online Access: | https://doi.org/10.1038/s41698-021-00166-3 |
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doaj-9cdaa30aa00f44b393b2013acc015cd12021-04-18T11:10:31ZengNature Publishing Groupnpj Precision Oncology2397-768X2021-04-015111210.1038/s41698-021-00166-3Clinical application of a lung cancer organoid (tumoroid) culture systemEtsuko Yokota0Miki Iwai1Takuro Yukawa2Masakazu Yoshida3Yoshio Naomoto4Minoru Haisa5Yasumasa Monobe6Nagio Takigawa7Minzhe Guo8Yutaka Maeda9Takuya Fukazawa10Tomoki Yamatsuji11Department of General Surgery, Kawasaki Medical SchoolGeneral Medical Center Research Unit, Kawasaki Medical SchoolDepartment of General Surgery, Kawasaki Medical SchoolDepartment of Thoracic Surgery, Kurashiki Central HospitalDepartment of General Surgery, Kawasaki Medical SchoolProfessor with Special Assignment, Kawasaki Medical SchoolDepartment of Pathology, Kawasaki Medical SchoolDepartment of General Internal Medicine 4, Kawasaki Medical SchoolPerinatal Institute, Division of Neonatology, Perinatal and Pulmonary Biology, Cincinnati Children’s Hospital Medical Center (CCHMC) and Department of Pediatrics, The University of Cincinnati College of Medicine (UC-COM)Perinatal Institute, Division of Neonatology, Perinatal and Pulmonary Biology, Cincinnati Children’s Hospital Medical Center (CCHMC) and Department of Pediatrics, The University of Cincinnati College of Medicine (UC-COM)Department of General Surgery, Kawasaki Medical SchoolDepartment of General Surgery, Kawasaki Medical SchoolAbstract Despite high expectations for lung tumoroids, they have not been applied in the clinic due to the difficulty of their long-term culture. Here, however, using AO (airway organoid) media developed by the Clevers laboratory, we succeeded in generating 3 lung tumoroid lines for long-term culture (>13 months) from 41 lung cancer cases (primary or metastatic). Use of nutlin-3a was key to selecting lung tumoroids that harbor mutant p53 in order to eliminate normal lung epithelial organoids. Next-generation sequencing (NGS) analysis indicated that each lung tumoroid carried BRAF G469A , TPM3-ROS1 or EGFR L858R /RB1 E737* , respectively. Targeted therapies using small molecule drugs (trametinib/erlotinib for BRAF G469A , crizotinib/entrectinib for TPM3-ROS1 and ABT-263/YM-155 for EGFR L858R /RB1 E737* ) significantly suppressed the growth of each lung tumoroid line. AO media was superior to 3 different media developed by other laboratories. Our experience indicates that long-term lung tumoroid culture is feasible, allowing us to identify NGS-based therapeutic targets and determine the responsiveness to corresponding small molecule drugs.https://doi.org/10.1038/s41698-021-00166-3 |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Etsuko Yokota Miki Iwai Takuro Yukawa Masakazu Yoshida Yoshio Naomoto Minoru Haisa Yasumasa Monobe Nagio Takigawa Minzhe Guo Yutaka Maeda Takuya Fukazawa Tomoki Yamatsuji |
spellingShingle |
Etsuko Yokota Miki Iwai Takuro Yukawa Masakazu Yoshida Yoshio Naomoto Minoru Haisa Yasumasa Monobe Nagio Takigawa Minzhe Guo Yutaka Maeda Takuya Fukazawa Tomoki Yamatsuji Clinical application of a lung cancer organoid (tumoroid) culture system npj Precision Oncology |
author_facet |
Etsuko Yokota Miki Iwai Takuro Yukawa Masakazu Yoshida Yoshio Naomoto Minoru Haisa Yasumasa Monobe Nagio Takigawa Minzhe Guo Yutaka Maeda Takuya Fukazawa Tomoki Yamatsuji |
author_sort |
Etsuko Yokota |
title |
Clinical application of a lung cancer organoid (tumoroid) culture system |
title_short |
Clinical application of a lung cancer organoid (tumoroid) culture system |
title_full |
Clinical application of a lung cancer organoid (tumoroid) culture system |
title_fullStr |
Clinical application of a lung cancer organoid (tumoroid) culture system |
title_full_unstemmed |
Clinical application of a lung cancer organoid (tumoroid) culture system |
title_sort |
clinical application of a lung cancer organoid (tumoroid) culture system |
publisher |
Nature Publishing Group |
series |
npj Precision Oncology |
issn |
2397-768X |
publishDate |
2021-04-01 |
description |
Abstract Despite high expectations for lung tumoroids, they have not been applied in the clinic due to the difficulty of their long-term culture. Here, however, using AO (airway organoid) media developed by the Clevers laboratory, we succeeded in generating 3 lung tumoroid lines for long-term culture (>13 months) from 41 lung cancer cases (primary or metastatic). Use of nutlin-3a was key to selecting lung tumoroids that harbor mutant p53 in order to eliminate normal lung epithelial organoids. Next-generation sequencing (NGS) analysis indicated that each lung tumoroid carried BRAF G469A , TPM3-ROS1 or EGFR L858R /RB1 E737* , respectively. Targeted therapies using small molecule drugs (trametinib/erlotinib for BRAF G469A , crizotinib/entrectinib for TPM3-ROS1 and ABT-263/YM-155 for EGFR L858R /RB1 E737* ) significantly suppressed the growth of each lung tumoroid line. AO media was superior to 3 different media developed by other laboratories. Our experience indicates that long-term lung tumoroid culture is feasible, allowing us to identify NGS-based therapeutic targets and determine the responsiveness to corresponding small molecule drugs. |
url |
https://doi.org/10.1038/s41698-021-00166-3 |
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