Clinical Characterization of a National Cohort of Patients With Germline WT1 Variants Including Late-Onset Phenotypes

Sophie E. van Peer; Roland P. Kuiper; Janna A. Hol; Sanne Egging; Bert van der Zwaag; Marc R. Lilien; M. Paola Lombardi; Marry M. van den Heuvel-Eibrink; Marjolijn C.J. Jongmans

doi:10.1016/j.ekir.2024.09.007

Clinical Characterization of a National Cohort of Patients With Germline WT1 Variants Including Late-Onset Phenotypes

Sophie E. van Peer
, Roland P. Kuiper
, Janna A. Hol
, Sanne Egging
, Bert van der Zwaag
, Marc R. Lilien
, M. Paola Lombardi
, Marry M. van den Heuvel-Eibrink
, Marjolijn C.J. Jongmans

Onderzoeksoutput: Bijdrage aan tijdschrift › Artikel › peer review

2 Citaten (Scopus)

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INTRODUCTION: WT1 disorder is a recently introduced term for phenotypes associated with germline Wilms Tumor 1 (WT1) variants, including glomerulopathy, urogenital anomalies, and Wilms tumor. Previous studies showed a bias toward missense variants in the DNA-binding/Zinc-finger domain of WT1 (exon 8 and 9) and patients with early-onset glomerulopathy. Thorough genotype-phenotype correlations including follow-up data on late-onset glomerulopathy risk are lacking. To characterize the genotypic and phenotypic spectrum of WT1 disorder, we describe a national cohort of individuals with WT1 variants.

METHODS: We requested clinical and genetic data of all patients with germline WT1 variants at all Dutch genetic laboratories.

RESULTS: We identified 43 patients with pathogenic WT1 variants (truncating, n = 19; missense, n = 13; splice-site, n = 7; and deletions, n = 4). Wilms tumor was the only clinical manifestation in 10 patients, of whom 9 were female. Wilms tumor occurred in 18 of 19 patients with truncating variants, in 4 of 4 patients with deletions, and was rarer in patients with missense or splice-site variants. All patients with missense and 6 of 7 with splice-site variants developed chronic kidney disease (CKD) versus 5 of 19 patients with truncating variants (3 in adulthood, with kidney failure at the age of 24, 26, and 41 years) and 1 of 4 with a deletion. Urogenital malformations occurred predominantly in 46,XY individuals.

CONCLUSION: Among patients with WT1 variants, a genotype-phenotype correlation was observed for Wilms tumor risk and age of CKD onset. Although childhood-onset CKD was more common in patients with missense variants in the DNA-binding/Zinc-finger domain, other patients may develop CKD and kidney failure later in life. Therefore, life-long surveillance of kidney function is recommended. Being alert about WT1 variants is especially important for girls with Wilms tumor who often miss additional phenotypes.

Originele taal-2	Engels
Pagina's (van-tot)	3570-3579
Aantal pagina's	10
Tijdschrift	Kidney international reports
Volume	9
Nummer van het tijdschrift	12
DOI's	https://doi.org/10.1016/j.ekir.2024.09.007
Status	Gepubliceerd - dec. 2024

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10.1016/j.ekir.2024.09.007

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van Peer, S. E., Kuiper, R. P., Hol, J. A., Egging, S., van der Zwaag, B., Lilien, M. R., Lombardi, M. P., van den Heuvel-Eibrink, M. M., & Jongmans, M. C. J. (2024). Clinical Characterization of a National Cohort of Patients With Germline WT1 Variants Including Late-Onset Phenotypes. Kidney international reports, 9(12), 3570-3579. https://doi.org/10.1016/j.ekir.2024.09.007

@article{1886b0b9a4184aff8647f318ae5174bd,

title = "Clinical Characterization of a National Cohort of Patients With Germline WT1 Variants Including Late-Onset Phenotypes",

abstract = "INTRODUCTION: WT1 disorder is a recently introduced term for phenotypes associated with germline Wilms Tumor 1 (WT1) variants, including glomerulopathy, urogenital anomalies, and Wilms tumor. Previous studies showed a bias toward missense variants in the DNA-binding/Zinc-finger domain of WT1 (exon 8 and 9) and patients with early-onset glomerulopathy. Thorough genotype-phenotype correlations including follow-up data on late-onset glomerulopathy risk are lacking. To characterize the genotypic and phenotypic spectrum of WT1 disorder, we describe a national cohort of individuals with WT1 variants.METHODS: We requested clinical and genetic data of all patients with germline WT1 variants at all Dutch genetic laboratories.RESULTS: We identified 43 patients with pathogenic WT1 variants (truncating, n = 19; missense, n = 13; splice-site, n = 7; and deletions, n = 4). Wilms tumor was the only clinical manifestation in 10 patients, of whom 9 were female. Wilms tumor occurred in 18 of 19 patients with truncating variants, in 4 of 4 patients with deletions, and was rarer in patients with missense or splice-site variants. All patients with missense and 6 of 7 with splice-site variants developed chronic kidney disease (CKD) versus 5 of 19 patients with truncating variants (3 in adulthood, with kidney failure at the age of 24, 26, and 41 years) and 1 of 4 with a deletion. Urogenital malformations occurred predominantly in 46,XY individuals.CONCLUSION: Among patients with WT1 variants, a genotype-phenotype correlation was observed for Wilms tumor risk and age of CKD onset. Although childhood-onset CKD was more common in patients with missense variants in the DNA-binding/Zinc-finger domain, other patients may develop CKD and kidney failure later in life. Therefore, life-long surveillance of kidney function is recommended. Being alert about WT1 variants is especially important for girls with Wilms tumor who often miss additional phenotypes.",

keywords = "Denys-Drash, WT1, Wilms tumor",

author = "\{van Peer\}, \{Sophie E.\} and Kuiper, \{Roland P.\} and Hol, \{Janna A.\} and Sanne Egging and \{van der Zwaag\}, Bert and Lilien, \{Marc R.\} and Lombardi, \{M. Paola\} and \{van den Heuvel-Eibrink\}, \{Marry M.\} and Jongmans, \{Marjolijn C.J.\}",

note = "Publisher Copyright: {\textcopyright} 2024 International Society of Nephrology",

year = "2024",

month = dec,

doi = "10.1016/j.ekir.2024.09.007",

language = "English",

volume = "9",

pages = "3570--3579",

journal = "Kidney international reports",

issn = "2468-0249",

publisher = "Elsevier Inc.",

number = "12",

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TY - JOUR

T1 - Clinical Characterization of a National Cohort of Patients With Germline WT1 Variants Including Late-Onset Phenotypes

AU - van Peer, Sophie E.

AU - Kuiper, Roland P.

AU - Hol, Janna A.

AU - Egging, Sanne

AU - van der Zwaag, Bert

AU - Lilien, Marc R.

AU - Lombardi, M. Paola

AU - van den Heuvel-Eibrink, Marry M.

AU - Jongmans, Marjolijn C.J.

PY - 2024/12

Y1 - 2024/12

N2 - INTRODUCTION: WT1 disorder is a recently introduced term for phenotypes associated with germline Wilms Tumor 1 (WT1) variants, including glomerulopathy, urogenital anomalies, and Wilms tumor. Previous studies showed a bias toward missense variants in the DNA-binding/Zinc-finger domain of WT1 (exon 8 and 9) and patients with early-onset glomerulopathy. Thorough genotype-phenotype correlations including follow-up data on late-onset glomerulopathy risk are lacking. To characterize the genotypic and phenotypic spectrum of WT1 disorder, we describe a national cohort of individuals with WT1 variants.METHODS: We requested clinical and genetic data of all patients with germline WT1 variants at all Dutch genetic laboratories.RESULTS: We identified 43 patients with pathogenic WT1 variants (truncating, n = 19; missense, n = 13; splice-site, n = 7; and deletions, n = 4). Wilms tumor was the only clinical manifestation in 10 patients, of whom 9 were female. Wilms tumor occurred in 18 of 19 patients with truncating variants, in 4 of 4 patients with deletions, and was rarer in patients with missense or splice-site variants. All patients with missense and 6 of 7 with splice-site variants developed chronic kidney disease (CKD) versus 5 of 19 patients with truncating variants (3 in adulthood, with kidney failure at the age of 24, 26, and 41 years) and 1 of 4 with a deletion. Urogenital malformations occurred predominantly in 46,XY individuals.CONCLUSION: Among patients with WT1 variants, a genotype-phenotype correlation was observed for Wilms tumor risk and age of CKD onset. Although childhood-onset CKD was more common in patients with missense variants in the DNA-binding/Zinc-finger domain, other patients may develop CKD and kidney failure later in life. Therefore, life-long surveillance of kidney function is recommended. Being alert about WT1 variants is especially important for girls with Wilms tumor who often miss additional phenotypes.

AB - INTRODUCTION: WT1 disorder is a recently introduced term for phenotypes associated with germline Wilms Tumor 1 (WT1) variants, including glomerulopathy, urogenital anomalies, and Wilms tumor. Previous studies showed a bias toward missense variants in the DNA-binding/Zinc-finger domain of WT1 (exon 8 and 9) and patients with early-onset glomerulopathy. Thorough genotype-phenotype correlations including follow-up data on late-onset glomerulopathy risk are lacking. To characterize the genotypic and phenotypic spectrum of WT1 disorder, we describe a national cohort of individuals with WT1 variants.METHODS: We requested clinical and genetic data of all patients with germline WT1 variants at all Dutch genetic laboratories.RESULTS: We identified 43 patients with pathogenic WT1 variants (truncating, n = 19; missense, n = 13; splice-site, n = 7; and deletions, n = 4). Wilms tumor was the only clinical manifestation in 10 patients, of whom 9 were female. Wilms tumor occurred in 18 of 19 patients with truncating variants, in 4 of 4 patients with deletions, and was rarer in patients with missense or splice-site variants. All patients with missense and 6 of 7 with splice-site variants developed chronic kidney disease (CKD) versus 5 of 19 patients with truncating variants (3 in adulthood, with kidney failure at the age of 24, 26, and 41 years) and 1 of 4 with a deletion. Urogenital malformations occurred predominantly in 46,XY individuals.CONCLUSION: Among patients with WT1 variants, a genotype-phenotype correlation was observed for Wilms tumor risk and age of CKD onset. Although childhood-onset CKD was more common in patients with missense variants in the DNA-binding/Zinc-finger domain, other patients may develop CKD and kidney failure later in life. Therefore, life-long surveillance of kidney function is recommended. Being alert about WT1 variants is especially important for girls with Wilms tumor who often miss additional phenotypes.

KW - Denys-Drash

KW - WT1

KW - Wilms tumor

UR - https://www.scopus.com/pages/publications/85205910693

U2 - 10.1016/j.ekir.2024.09.007

DO - 10.1016/j.ekir.2024.09.007

M3 - Article

C2 - 39698353

AN - SCOPUS:85205910693

SN - 2468-0249

VL - 9

SP - 3570

EP - 3579

JO - Kidney international reports

JF - Kidney international reports

IS - 12

ER -

Clinical Characterization of a National Cohort of Patients With Germline WT1 Variants Including Late-Onset Phenotypes

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