Genetic changes associated with relapse in favorable histology Wilms tumor: A Children's Oncology Group AREN03B2 study

Samantha Gadd; Vicki Huff; Andrew D. Skol; Lindsay A. Renfro; Conrad V. Fernandez; Elizabeth A. Mullen; Corbin D. Jones; Katherine A. Hoadley; Kai Lee Yap; Nilsa C. Ramirez; Sheena Aris; Quy H. Phung; Elizabeth J. Perlman

doi:10.1016/j.xcrm.2022.100644

Genetic changes associated with relapse in favorable histology Wilms tumor: A Children's Oncology Group AREN03B2 study

Samantha Gadd, Vicki Huff, Andrew D. Skol, Lindsay A. Renfro, Conrad V. Fernandez, Elizabeth A. Mullen, Corbin D. Jones, Katherine A. Hoadley, Kai Lee Yap, Nilsa C. Ramirez, Sheena Aris, Quy H. Phung, Elizabeth J. Perlman

Genetics

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

10 Scopus citations

Abstract

Over the last decade, sequencing of primary tumors has clarified the genetic underpinnings of Wilms tumor but has not affected therapy, outcome, or toxicity. We now sharpen our focus on relapse samples from the umbrella AREN03B2 study. We show that over 40% of relapse samples contain mutations in SIX1 or genes of the MYCN network, drivers of progenitor proliferation. Not previously seen in large studies of primary Wilms tumors, DIS3 and TERT are now identified as recurrently mutated. The analysis of primary-relapse tumor pairs suggests that 11p15 loss of heterozygosity (and other copy number changes) and mutations in WT1 and MLLT1 typically occur early, but mutations in SIX1, MYCN, and WTX are late developments in some individuals. Most strikingly, 75% of relapse samples had gain of 1q, providing strong conceptual support for studying circulating tumor DNA in clinical trials to better detect 1q gain earlier and monitor response.

Original language	English (US)
Article number	100644
Journal	Cell Reports Medicine
Volume	3
Issue number	6
DOIs	https://doi.org/10.1016/j.xcrm.2022.100644
State	Published - Jun 21 2022

Keywords

1q gain
: Wilms tumor
DIS3
MYCN
relapse
SIX1
TERT

ASJC Scopus subject areas

General Biochemistry, Genetics and Molecular Biology

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Gadd, S., Huff, V., Skol, A. D., Renfro, L. A., Fernandez, C. V., Mullen, E. A., Jones, C. D., Hoadley, K. A., Yap, K. L., Ramirez, N. C., Aris, S., Phung, Q. H., & Perlman, E. J. (2022). Genetic changes associated with relapse in favorable histology Wilms tumor: A Children's Oncology Group AREN03B2 study. Cell Reports Medicine, 3(6), Article 100644. https://doi.org/10.1016/j.xcrm.2022.100644

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title = "Genetic changes associated with relapse in favorable histology Wilms tumor: A Children's Oncology Group AREN03B2 study",

abstract = "Over the last decade, sequencing of primary tumors has clarified the genetic underpinnings of Wilms tumor but has not affected therapy, outcome, or toxicity. We now sharpen our focus on relapse samples from the umbrella AREN03B2 study. We show that over 40% of relapse samples contain mutations in SIX1 or genes of the MYCN network, drivers of progenitor proliferation. Not previously seen in large studies of primary Wilms tumors, DIS3 and TERT are now identified as recurrently mutated. The analysis of primary-relapse tumor pairs suggests that 11p15 loss of heterozygosity (and other copy number changes) and mutations in WT1 and MLLT1 typically occur early, but mutations in SIX1, MYCN, and WTX are late developments in some individuals. Most strikingly, 75% of relapse samples had gain of 1q, providing strong conceptual support for studying circulating tumor DNA in clinical trials to better detect 1q gain earlier and monitor response.",

keywords = "1q gain, : Wilms tumor, DIS3, MYCN, relapse, SIX1, TERT",

author = "Samantha Gadd and Vicki Huff and Skol, {Andrew D.} and Renfro, {Lindsay A.} and Fernandez, {Conrad V.} and Mullen, {Elizabeth A.} and Jones, {Corbin D.} and Hoadley, {Katherine A.} and Yap, {Kai Lee} and Ramirez, {Nilsa C.} and Sheena Aris and Phung, {Quy H.} and Perlman, {Elizabeth J.}",

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year = "2022",

month = jun,

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doi = "10.1016/j.xcrm.2022.100644",

language = "English (US)",

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T2 - A Children's Oncology Group AREN03B2 study

AU - Gadd, Samantha

AU - Huff, Vicki

AU - Skol, Andrew D.

AU - Renfro, Lindsay A.

AU - Fernandez, Conrad V.

AU - Mullen, Elizabeth A.

AU - Jones, Corbin D.

AU - Hoadley, Katherine A.

AU - Yap, Kai Lee

AU - Ramirez, Nilsa C.

AU - Aris, Sheena

AU - Phung, Quy H.

AU - Perlman, Elizabeth J.

PY - 2022/6/21

Y1 - 2022/6/21

N2 - Over the last decade, sequencing of primary tumors has clarified the genetic underpinnings of Wilms tumor but has not affected therapy, outcome, or toxicity. We now sharpen our focus on relapse samples from the umbrella AREN03B2 study. We show that over 40% of relapse samples contain mutations in SIX1 or genes of the MYCN network, drivers of progenitor proliferation. Not previously seen in large studies of primary Wilms tumors, DIS3 and TERT are now identified as recurrently mutated. The analysis of primary-relapse tumor pairs suggests that 11p15 loss of heterozygosity (and other copy number changes) and mutations in WT1 and MLLT1 typically occur early, but mutations in SIX1, MYCN, and WTX are late developments in some individuals. Most strikingly, 75% of relapse samples had gain of 1q, providing strong conceptual support for studying circulating tumor DNA in clinical trials to better detect 1q gain earlier and monitor response.

AB - Over the last decade, sequencing of primary tumors has clarified the genetic underpinnings of Wilms tumor but has not affected therapy, outcome, or toxicity. We now sharpen our focus on relapse samples from the umbrella AREN03B2 study. We show that over 40% of relapse samples contain mutations in SIX1 or genes of the MYCN network, drivers of progenitor proliferation. Not previously seen in large studies of primary Wilms tumors, DIS3 and TERT are now identified as recurrently mutated. The analysis of primary-relapse tumor pairs suggests that 11p15 loss of heterozygosity (and other copy number changes) and mutations in WT1 and MLLT1 typically occur early, but mutations in SIX1, MYCN, and WTX are late developments in some individuals. Most strikingly, 75% of relapse samples had gain of 1q, providing strong conceptual support for studying circulating tumor DNA in clinical trials to better detect 1q gain earlier and monitor response.

KW - 1q gain

KW - : Wilms tumor

KW - DIS3

KW - MYCN

KW - relapse

KW - SIX1

KW - TERT

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Genetic changes associated with relapse in favorable histology Wilms tumor: A Children's Oncology Group AREN03B2 study

Abstract

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