Predisposition Footprints in the Somatic Genome of Wilms Tumors

Taryn D Treger; Jenny Wegert; Anna Wenger; Tim H H Coorens; Reem Al-Saadi; Paul G Kemps; Jonathan Kennedy; Conor Parks; Nathaniel D Anderson; Angus Hodder; Aleksandra Letunovska; Hyunchul Jung; Toochi Ogbonnah; Mi K Trinh; Henry Lee-Six; Guillaume Morcrette; Marry M van den Heuvel-Eibrink; Jarno Drost; Ruben van Boxtel; Eline J M Bertrums; Bianca F Goemans; Evangelia Antoniou; Dirk Reinhardt; Heike Streitenberger; Barbara Ziegler; Jack Bartram; John C Hutchinson; Gordan M Vujanic; Christian Vokuhl; Tanzina Chowdhury; Rhoikos Furtwängler; Norbert Graf; Kathy Pritchard-Jones; Manfred Gessler; Sam Behjati

doi:10.1158/2159-8290.CD-24-0878

Predisposition Footprints in the Somatic Genome of Wilms Tumors

Taryn D Treger, Jenny Wegert, Anna Wenger, Tim H H Coorens, Reem Al-Saadi, Paul G Kemps, Jonathan Kennedy, Conor Parks, Nathaniel D Anderson, Angus Hodder, Aleksandra Letunovska, Hyunchul Jung, Toochi Ogbonnah, Mi K Trinh, Henry Lee-Six, Guillaume Morcrette, Marry M van den Heuvel-Eibrink, Jarno Drost, Ruben van Boxtel, Eline J M BertrumsBianca F Goemans, Evangelia Antoniou, Dirk Reinhardt, Heike Streitenberger, Barbara Ziegler, Jack Bartram, John C Hutchinson, Gordan M Vujanic, Christian Vokuhl, Tanzina Chowdhury, Rhoikos Furtwängler, Norbert Graf, Kathy Pritchard-Jones, Manfred Gessler, Sam Behjati

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Approximately 10% of children with cancer harbor a mutation in a predisposition gene. In children with the kidney cancer Wilms tumor, the prevalence is as high as 30%. Certain predispositions are associated with defined histological and clinical features, suggesting differences in tumorigenesis. To investigate this, we assembled a cohort of 137 children with Wilms tumor, of whom 71 had a pathogenic germline or mosaic variant. We examined 237 neoplasms (including two secondary leukemias), utilizing whole-genome sequencing, RNA sequencing, and genome-wide methylation, validating our findings in an independent cohort. Tumor development differed in children harboring a predisposition, depending on the variant gene and its developmental timing. Differences pervaded the repertoire of driver events, including high-risk mutations, the clonal architecture of normal kidneys, and the relatedness of neoplasms from the same individual. Our findings indicate that predisposition may preordain Wilms tumorigenesis, suggesting a variant-specific approach to managing children merits consideration. Significance: Tumors that arise in children with a cancer predisposition may develop through the same mutational pathways as sporadic tumors. We examined this question in the childhood kidney cancer, Wilms tumor. We found that certain predispositions dictate the genetic development of tumors, with clinical implications for these children. See related commentary by Brzezinski and Malkin, p. 258.

Originele taal-2	Engels
Pagina's (van-tot)	286-298
Aantal pagina's	13
Tijdschrift	Cancer discovery
Volume	15
Nummer van het tijdschrift	2
DOI's	https://doi.org/10.1158/2159-8290.CD-24-0878
Status	Gepubliceerd - 7 feb. 2025
Extern gepubliceerd	Ja

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10.1158/2159-8290.CD-24-0878

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Treger, T. D., Wegert, J., Wenger, A., Coorens, T. H. H., Al-Saadi, R., Kemps, P. G., Kennedy, J., Parks, C., Anderson, N. D., Hodder, A., Letunovska, A., Jung, H., Ogbonnah, T., Trinh, M. K., Lee-Six, H., Morcrette, G., van den Heuvel-Eibrink, M. M., Drost, J., van Boxtel, R., ... Behjati, S. (2025). Predisposition Footprints in the Somatic Genome of Wilms Tumors. Cancer discovery, 15(2), 286-298. https://doi.org/10.1158/2159-8290.CD-24-0878

@article{97dc1e02be474953b3e829f5d1ff2c8b,

title = "Predisposition Footprints in the Somatic Genome of Wilms Tumors",

abstract = "Approximately 10% of children with cancer harbor a mutation in a predisposition gene. In children with the kidney cancer Wilms tumor, the prevalence is as high as 30%. Certain predispositions are associated with defined histological and clinical features, suggesting differences in tumorigenesis. To investigate this, we assembled a cohort of 137 children with Wilms tumor, of whom 71 had a pathogenic germline or mosaic variant. We examined 237 neoplasms (including two secondary leukemias), utilizing whole-genome sequencing, RNA sequencing, and genome-wide methylation, validating our findings in an independent cohort. Tumor development differed in children harboring a predisposition, depending on the variant gene and its developmental timing. Differences pervaded the repertoire of driver events, including high-risk mutations, the clonal architecture of normal kidneys, and the relatedness of neoplasms from the same individual. Our findings indicate that predisposition may preordain Wilms tumorigenesis, suggesting a variant-specific approach to managing children merits consideration. Significance: Tumors that arise in children with a cancer predisposition may develop through the same mutational pathways as sporadic tumors. We examined this question in the childhood kidney cancer, Wilms tumor. We found that certain predispositions dictate the genetic development of tumors, with clinical implications for these children. See related commentary by Brzezinski and Malkin, p. 258.",

keywords = "Humans, Wilms Tumor/genetics, Genetic Predisposition to Disease, Kidney Neoplasms/genetics, Male, Female, Child, Mutation, Child, Preschool, Infant",

author = "Treger, {Taryn D} and Jenny Wegert and Anna Wenger and Coorens, {Tim H H} and Reem Al-Saadi and Kemps, {Paul G} and Jonathan Kennedy and Conor Parks and Anderson, {Nathaniel D} and Angus Hodder and Aleksandra Letunovska and Hyunchul Jung and Toochi Ogbonnah and Trinh, {Mi K} and Henry Lee-Six and Guillaume Morcrette and {van den Heuvel-Eibrink}, {Marry M} and Jarno Drost and {van Boxtel}, Ruben and Bertrums, {Eline J M} and Goemans, {Bianca F} and Evangelia Antoniou and Dirk Reinhardt and Heike Streitenberger and Barbara Ziegler and Jack Bartram and Hutchinson, {John C} and Vujanic, {Gordan M} and Christian Vokuhl and Tanzina Chowdhury and Rhoikos Furtw{\"a}ngler and Norbert Graf and Kathy Pritchard-Jones and Manfred Gessler and Sam Behjati",

note = "{\textcopyright}2025 American Association for Cancer Research.",

year = "2025",

month = feb,

day = "7",

doi = "10.1158/2159-8290.CD-24-0878",

language = "English",

volume = "15",

pages = "286--298",

journal = "Cancer discovery",

issn = "2159-8274",

publisher = "American Association for Cancer Research Inc.",

number = "2",

}

Treger, TD, Wegert, J, Wenger, A, Coorens, THH, Al-Saadi, R, Kemps, PG, Kennedy, J, Parks, C, Anderson, ND, Hodder, A, Letunovska, A, Jung, H, Ogbonnah, T, Trinh, MK, Lee-Six, H, Morcrette, G, van den Heuvel-Eibrink, MM, Drost, J, van Boxtel, R, Bertrums, EJM, Goemans, BF, Antoniou, E, Reinhardt, D, Streitenberger, H, Ziegler, B, Bartram, J, Hutchinson, JC, Vujanic, GM, Vokuhl, C, Chowdhury, T, Furtwängler, R, Graf, N, Pritchard-Jones, K, Gessler, M & Behjati, S 2025, 'Predisposition Footprints in the Somatic Genome of Wilms Tumors', Cancer discovery, vol. 15, nr. 2, blz. 286-298. https://doi.org/10.1158/2159-8290.CD-24-0878

TY - JOUR

T1 - Predisposition Footprints in the Somatic Genome of Wilms Tumors

AU - Treger, Taryn D

AU - Wegert, Jenny

AU - Wenger, Anna

AU - Coorens, Tim H H

AU - Al-Saadi, Reem

AU - Kemps, Paul G

AU - Kennedy, Jonathan

AU - Parks, Conor

AU - Anderson, Nathaniel D

AU - Hodder, Angus

AU - Letunovska, Aleksandra

AU - Jung, Hyunchul

AU - Ogbonnah, Toochi

AU - Trinh, Mi K

AU - Lee-Six, Henry

AU - Morcrette, Guillaume

AU - van den Heuvel-Eibrink, Marry M

AU - Drost, Jarno

AU - van Boxtel, Ruben

AU - Bertrums, Eline J M

AU - Goemans, Bianca F

AU - Antoniou, Evangelia

AU - Reinhardt, Dirk

AU - Streitenberger, Heike

AU - Ziegler, Barbara

AU - Bartram, Jack

AU - Hutchinson, John C

AU - Vujanic, Gordan M

AU - Vokuhl, Christian

AU - Chowdhury, Tanzina

AU - Furtwängler, Rhoikos

AU - Graf, Norbert

AU - Pritchard-Jones, Kathy

AU - Gessler, Manfred

AU - Behjati, Sam

PY - 2025/2/7

Y1 - 2025/2/7

N2 - Approximately 10% of children with cancer harbor a mutation in a predisposition gene. In children with the kidney cancer Wilms tumor, the prevalence is as high as 30%. Certain predispositions are associated with defined histological and clinical features, suggesting differences in tumorigenesis. To investigate this, we assembled a cohort of 137 children with Wilms tumor, of whom 71 had a pathogenic germline or mosaic variant. We examined 237 neoplasms (including two secondary leukemias), utilizing whole-genome sequencing, RNA sequencing, and genome-wide methylation, validating our findings in an independent cohort. Tumor development differed in children harboring a predisposition, depending on the variant gene and its developmental timing. Differences pervaded the repertoire of driver events, including high-risk mutations, the clonal architecture of normal kidneys, and the relatedness of neoplasms from the same individual. Our findings indicate that predisposition may preordain Wilms tumorigenesis, suggesting a variant-specific approach to managing children merits consideration. Significance: Tumors that arise in children with a cancer predisposition may develop through the same mutational pathways as sporadic tumors. We examined this question in the childhood kidney cancer, Wilms tumor. We found that certain predispositions dictate the genetic development of tumors, with clinical implications for these children. See related commentary by Brzezinski and Malkin, p. 258.

AB - Approximately 10% of children with cancer harbor a mutation in a predisposition gene. In children with the kidney cancer Wilms tumor, the prevalence is as high as 30%. Certain predispositions are associated with defined histological and clinical features, suggesting differences in tumorigenesis. To investigate this, we assembled a cohort of 137 children with Wilms tumor, of whom 71 had a pathogenic germline or mosaic variant. We examined 237 neoplasms (including two secondary leukemias), utilizing whole-genome sequencing, RNA sequencing, and genome-wide methylation, validating our findings in an independent cohort. Tumor development differed in children harboring a predisposition, depending on the variant gene and its developmental timing. Differences pervaded the repertoire of driver events, including high-risk mutations, the clonal architecture of normal kidneys, and the relatedness of neoplasms from the same individual. Our findings indicate that predisposition may preordain Wilms tumorigenesis, suggesting a variant-specific approach to managing children merits consideration. Significance: Tumors that arise in children with a cancer predisposition may develop through the same mutational pathways as sporadic tumors. We examined this question in the childhood kidney cancer, Wilms tumor. We found that certain predispositions dictate the genetic development of tumors, with clinical implications for these children. See related commentary by Brzezinski and Malkin, p. 258.

KW - Humans

KW - Wilms Tumor/genetics

KW - Genetic Predisposition to Disease

KW - Kidney Neoplasms/genetics

KW - Male

KW - Female

KW - Child

KW - Mutation

KW - Child, Preschool

KW - Infant

UR - https://www.mendeley.com/catalogue/f782a9e1-4c45-3d78-b64e-887ef766619d/

U2 - 10.1158/2159-8290.CD-24-0878

DO - 10.1158/2159-8290.CD-24-0878

M3 - Article

C2 - 39665570

SN - 2159-8274

VL - 15

SP - 286

EP - 298

JO - Cancer discovery

JF - Cancer discovery

IS - 2

ER -

Predisposition Footprints in the Somatic Genome of Wilms Tumors

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