Wilms tumor primary cultures capture phenotypic heterogeneity and facilitate preclinical screening

Lisa Götz; Jenny Wegert; Alireza Paikari; Silke Appenzeller; Sabrina Bausenwein; Christian Vokuhl; Taryn D Treger; Jarno Drost; Christin Linderkamp; Dominik T Schneider; Karen Ernestus; Steven W Warman; Jörg Fuchs; Nils Welter; Norbert Graf; Sam Behjati; Rhoikos Furtwängler; Manfred Gessler

doi:10.1016/j.tranon.2024.102263

Wilms tumor primary cultures capture phenotypic heterogeneity and facilitate preclinical screening

Lisa Götz, Jenny Wegert, Alireza Paikari, Silke Appenzeller, Sabrina Bausenwein, Christian Vokuhl, Taryn D Treger, Jarno Drost, Christin Linderkamp, Dominik T Schneider, Karen Ernestus, Steven W Warman, Jörg Fuchs, Nils Welter, Norbert Graf, Sam Behjati, Rhoikos Furtwängler, Manfred Gessler

Research output: Contribution to journal › Article › peer-review

Abstract

Wilms tumors (WT) are characterized by variable contributions of blastemal, epithelial and stromal elements, reflecting their diverse cellular origins and genetic drivers. In vitro models remain rare, despite a growing need to better characterize tumor biology and evaluate new treatments. Using three approaches, we have now established a large collection of long-term cultures that represent this diversity. Adherent WT cultures are predominated by stromal cells, 3D spheroids model blastema, and patient-derived organoid cultures of both tumor and healthy kidney tissue result in the preferential growth of epithelial cells. Adherent, spheroid and organoid cultures are also clearly distinguishable by their transcriptome. Preclinical drug screening experiments revealed sensitivity to a range of inhibitors, that are highly effective in other childhood solid tumors. Sensitivity was related to MYCN status, a marker associated with adverse outcome across human cancers including WT. The combination of the three culture techniques represents a promising tool to both explore tumor heterogeneity in vitro and to facilitate characterization of candidate driver genes, in order to improve treatment regimens in the future.

Original language	English
Pages (from-to)	102263
Journal	Translational oncology
Volume	52
DOIs	https://doi.org/10.1016/j.tranon.2024.102263
Publication status	Published - Jan 2025
Externally published	Yes

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Götz, L., Wegert, J., Paikari, A., Appenzeller, S., Bausenwein, S., Vokuhl, C., Treger, T. D., Drost, J., Linderkamp, C., Schneider, D. T., Ernestus, K., Warman, S. W., Fuchs, J., Welter, N., Graf, N., Behjati, S., Furtwängler, R., & Gessler, M. (2025). Wilms tumor primary cultures capture phenotypic heterogeneity and facilitate preclinical screening. Translational oncology, 52, 102263. https://doi.org/10.1016/j.tranon.2024.102263

@article{091eaafb701341a8b512e06d192a3a09,

title = "Wilms tumor primary cultures capture phenotypic heterogeneity and facilitate preclinical screening",

abstract = "Wilms tumors (WT) are characterized by variable contributions of blastemal, epithelial and stromal elements, reflecting their diverse cellular origins and genetic drivers. In vitro models remain rare, despite a growing need to better characterize tumor biology and evaluate new treatments. Using three approaches, we have now established a large collection of long-term cultures that represent this diversity. Adherent WT cultures are predominated by stromal cells, 3D spheroids model blastema, and patient-derived organoid cultures of both tumor and healthy kidney tissue result in the preferential growth of epithelial cells. Adherent, spheroid and organoid cultures are also clearly distinguishable by their transcriptome. Preclinical drug screening experiments revealed sensitivity to a range of inhibitors, that are highly effective in other childhood solid tumors. Sensitivity was related to MYCN status, a marker associated with adverse outcome across human cancers including WT. The combination of the three culture techniques represents a promising tool to both explore tumor heterogeneity in vitro and to facilitate characterization of candidate driver genes, in order to improve treatment regimens in the future.",

keywords = "Drug screening, MYCN, Nephroblastoma, Organoid culture, Wilms tumor",

author = "Lisa G{\"o}tz and Jenny Wegert and Alireza Paikari and Silke Appenzeller and Sabrina Bausenwein and Christian Vokuhl and Treger, {Taryn D} and Jarno Drost and Christin Linderkamp and Schneider, {Dominik T} and Karen Ernestus and Warman, {Steven W} and J{\"o}rg Fuchs and Nils Welter and Norbert Graf and Sam Behjati and Rhoikos Furtw{\"a}ngler and Manfred Gessler",

note = "Copyright {\textcopyright} 2024. Published by Elsevier Inc.",

year = "2025",

month = jan,

doi = "10.1016/j.tranon.2024.102263",

language = "English",

volume = "52",

pages = "102263",

journal = "Translational oncology",

issn = "1936-5233",

publisher = "Neoplasia Press",

}

Götz, L, Wegert, J, Paikari, A, Appenzeller, S, Bausenwein, S, Vokuhl, C, Treger, TD, Drost, J, Linderkamp, C, Schneider, DT, Ernestus, K, Warman, SW, Fuchs, J, Welter, N, Graf, N, Behjati, S, Furtwängler, R & Gessler, M 2025, 'Wilms tumor primary cultures capture phenotypic heterogeneity and facilitate preclinical screening', Translational oncology, vol. 52, pp. 102263. https://doi.org/10.1016/j.tranon.2024.102263

TY - JOUR

T1 - Wilms tumor primary cultures capture phenotypic heterogeneity and facilitate preclinical screening

AU - Götz, Lisa

AU - Wegert, Jenny

AU - Paikari, Alireza

AU - Appenzeller, Silke

AU - Bausenwein, Sabrina

AU - Vokuhl, Christian

AU - Treger, Taryn D

AU - Drost, Jarno

AU - Linderkamp, Christin

AU - Schneider, Dominik T

AU - Ernestus, Karen

AU - Warman, Steven W

AU - Fuchs, Jörg

AU - Welter, Nils

AU - Graf, Norbert

AU - Behjati, Sam

AU - Furtwängler, Rhoikos

AU - Gessler, Manfred

PY - 2025/1

Y1 - 2025/1

N2 - Wilms tumors (WT) are characterized by variable contributions of blastemal, epithelial and stromal elements, reflecting their diverse cellular origins and genetic drivers. In vitro models remain rare, despite a growing need to better characterize tumor biology and evaluate new treatments. Using three approaches, we have now established a large collection of long-term cultures that represent this diversity. Adherent WT cultures are predominated by stromal cells, 3D spheroids model blastema, and patient-derived organoid cultures of both tumor and healthy kidney tissue result in the preferential growth of epithelial cells. Adherent, spheroid and organoid cultures are also clearly distinguishable by their transcriptome. Preclinical drug screening experiments revealed sensitivity to a range of inhibitors, that are highly effective in other childhood solid tumors. Sensitivity was related to MYCN status, a marker associated with adverse outcome across human cancers including WT. The combination of the three culture techniques represents a promising tool to both explore tumor heterogeneity in vitro and to facilitate characterization of candidate driver genes, in order to improve treatment regimens in the future.

AB - Wilms tumors (WT) are characterized by variable contributions of blastemal, epithelial and stromal elements, reflecting their diverse cellular origins and genetic drivers. In vitro models remain rare, despite a growing need to better characterize tumor biology and evaluate new treatments. Using three approaches, we have now established a large collection of long-term cultures that represent this diversity. Adherent WT cultures are predominated by stromal cells, 3D spheroids model blastema, and patient-derived organoid cultures of both tumor and healthy kidney tissue result in the preferential growth of epithelial cells. Adherent, spheroid and organoid cultures are also clearly distinguishable by their transcriptome. Preclinical drug screening experiments revealed sensitivity to a range of inhibitors, that are highly effective in other childhood solid tumors. Sensitivity was related to MYCN status, a marker associated with adverse outcome across human cancers including WT. The combination of the three culture techniques represents a promising tool to both explore tumor heterogeneity in vitro and to facilitate characterization of candidate driver genes, in order to improve treatment regimens in the future.

KW - Drug screening

KW - MYCN

KW - Nephroblastoma

KW - Organoid culture

KW - Wilms tumor

UR - https://www.mendeley.com/catalogue/8fd6071c-0236-3b8a-ba7e-d4b14862f542/

U2 - 10.1016/j.tranon.2024.102263

DO - 10.1016/j.tranon.2024.102263

M3 - Article

C2 - 39740515

SN - 1936-5233

VL - 52

SP - 102263

JO - Translational oncology

JF - Translational oncology

ER -

Wilms tumor primary cultures capture phenotypic heterogeneity and facilitate preclinical screening

Abstract

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