Somatic mutations and single-cell transcriptomes reveal the root of malignant rhabdoid tumours

Custers, Lars; Khabirova, Eleonora; Coorens, Tim; Oliver, Thomas R. W.; Calandrini, Camilla; Young, Matthew D.; Braga, Felipe A. Vieira; Ellis, Peter; Mamanova, Lira; Segers, Heidi; Maat, Arie; Kool, Marcel; Hoving, Eelco W.; Heuvel‐Eibrink, Marry M. van den; Nicholson, James C.; Straathof, Karin; Hook, Liz; Krijger, Ronald R. de; Trayers, Claire; Allinson, Kieren; Behjati, Sam; Drost, Jarno

doi:10.1038/s41467-021-21675-6

Cited by 47 publications

(59 citation statements)

References 54 publications

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“…Indeed, we observed a mutation in oncogene MYC and a subclonal deletion of a part of chromosome 18 in the matching clonal iPSC cell line . Nevertheless, during fetal development and even during early embryogenesis, cells can also acquire oncogenic mutations ( Custers et al., 2021 ; Greaves, 2018 ; Williams et al., 2020 ). For example, sacrococcygeal teratomas, the most common tumor type in newborns, arise from germ cells and can recapitulate cells of all three germ layers ( Manes, 1976 ; Moore et al., 2003 ).…”

Section: Discussionmentioning

confidence: 99%

Human induced pluripotent stem cells display a similar mutation burden as embryonic pluripotent cells in vivo

et al. 2022

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Summary Induced pluripotent stem cells (iPSCs) hold great promise for regenerative medicine, but genetic instability is a major concern. Embryonic pluripotent cells also accumulate mutations during early development, but how this relates to the mutation burden in iPSCs remains unknown. Here, we directly compared the mutation burden of cultured iPSCs with their isogenic embryonic cells during human embryogenesis. We generated developmental lineage trees of human fetuses by phylogenetic inference from somatic mutations in the genomes of multiple stem cells, which were derived from different germ layers. Using this approach, we characterized the mutations acquired pre-gastrulation and found a rate of 1.65 mutations per cell division. When cultured in hypoxic conditions, iPSCs generated from fetal stem cells of the assessed fetuses displayed a similar mutation rate and spectrum. Our results show that iPSCs maintain a genomic integrity during culture at a similar degree as their pluripotent counterparts do in vivo .

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Section: Discussionmentioning

confidence: 99%

Human induced pluripotent stem cells display a similar mutation burden as embryonic pluripotent cells in vivo

et al. 2022

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“…On the other hand, RMS tumoroid models are less intricate in their propagation. Lastly, while GEMs are considered essential for cell of origin studies, recent advances have shown that by genetic editing, such studies can now also be performed in tumoroid models (Custers et al, 2021).…”

Section: Discussionmentioning

confidence: 99%

Mesenchymal tumor organoid models recapitulate rhabdomyosarcoma subtypes

Meister

Koerkamp

Souza

et al. 2022

Preprint

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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 with TP53 knockout 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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“… 74 Custers et al discovered that combined HDAC and mTOR inhibition mimics MRT differentiation. 75 Recently, a small molecule epigenetic modulator known as domatinostat (4SC-202), inhibiting both class I HDACs and Lysine Demethylase (LSD1) was investigated, and cytotoxic and cytostatic effects on malignant rhabdoid tumor cells were detected. 76 The histone deacetylase inhibitor, OBP-801 induced apoptosis in malignant rhabdoid tumor cells by epigenetically releasing the silencing of NOXA, a key mediator of MRT apoptosis.…”

Section: Potential Targeted Therapeutic Approaches To Extracranial Mrtmentioning

confidence: 99%

Current and Emerging Therapeutic Approaches for Extracranial Malignant Rhabdoid Tumors

Nemes

Johann²,

Tüchert³

et al. 2022

CMAR

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Somatic mutations and single-cell transcriptomes reveal the root of malignant rhabdoid tumours

Cited by 47 publications

References 54 publications

Human induced pluripotent stem cells display a similar mutation burden as embryonic pluripotent cells in vivo

Human induced pluripotent stem cells display a similar mutation burden as embryonic pluripotent cells in vivo

Mesenchymal tumor organoid models recapitulate rhabdomyosarcoma subtypes

Current and Emerging Therapeutic Approaches for Extracranial Malignant Rhabdoid Tumors

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