Parental age and risk of genetic syndromes predisposing to nervous system tumors: nested case-control study

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Parental age and risk of genetic syndromes predisposing to nervous system tumors : nested case-control study. / Adel Fahmideh, Maral; Tettamanti, Giorgio; Lavebratt, Catharina; Talbäck, Mats; Mathiesen, Tiit; Lannering, Birgitta; Johnson, Kimberly J; Feychting, Maria.

I: Clinical Epidemiology, Bind 10, 20.06.2018, s. 729-738.

Publikation: Bidrag til tidsskriftTidsskriftartikelForskningfagfællebedømt

Harvard

Adel Fahmideh, M, Tettamanti, G, Lavebratt, C, Talbäck, M, Mathiesen, T, Lannering, B, Johnson, KJ & Feychting, M 2018, 'Parental age and risk of genetic syndromes predisposing to nervous system tumors: nested case-control study', Clinical Epidemiology, bind 10, s. 729-738. https://doi.org/10.2147/CLEP.S159183

APA

Adel Fahmideh, M., Tettamanti, G., Lavebratt, C., Talbäck, M., Mathiesen, T., Lannering, B., Johnson, K. J., & Feychting, M. (2018). Parental age and risk of genetic syndromes predisposing to nervous system tumors: nested case-control study. Clinical Epidemiology, 10, 729-738. https://doi.org/10.2147/CLEP.S159183

Vancouver

Adel Fahmideh M, Tettamanti G, Lavebratt C, Talbäck M, Mathiesen T, Lannering B o.a. Parental age and risk of genetic syndromes predisposing to nervous system tumors: nested case-control study. Clinical Epidemiology. 2018 jun. 20;10:729-738. https://doi.org/10.2147/CLEP.S159183

Author

Adel Fahmideh, Maral ; Tettamanti, Giorgio ; Lavebratt, Catharina ; Talbäck, Mats ; Mathiesen, Tiit ; Lannering, Birgitta ; Johnson, Kimberly J ; Feychting, Maria. / Parental age and risk of genetic syndromes predisposing to nervous system tumors : nested case-control study. I: Clinical Epidemiology. 2018 ; Bind 10. s. 729-738.

Bibtex

@article{ce8627c35b724891a839e6df2423da3e,
title = "Parental age and risk of genetic syndromes predisposing to nervous system tumors: nested case-control study",
abstract = "Purpose: Phacomatoses are genetic syndromes that are associated with increased risk of developing nervous system tumors. Phacomatoses are usually inherited, but many develop de novo, with unknown etiology. In this population-based study, we investigated the effect of parental age on the risk of phacomatoses in offspring.Patients and methods: The study was a population-based nested case-control study. All individuals born and residing in Sweden between January 1960 and December 2010 were eligible for inclusion. Using the Patient Register, 4625 phacomatosis cases were identified and further classified as familial or nonfamilial. Ten matched controls per case were randomly selected from the eligible population. Data were analyzed using conditional logistic regression. Analyses were conducted for neurofibromatosis alone (n=2089) and other phacomatoses combined (n=2536).Results: Compared with offspring of fathers aged 25-29 years, increased risk estimates of nonfamilial neurofibromatosis were found for offspring of fathers aged 35-39 years (odds ratio [OR]=1.43 [95% CI 1.16-1.74]) and ≥40 years (OR =1.74 [95% CI 1.38-2.19]). For other nonfamilial phacomatoses, the risk estimate for offspring of fathers aged ≥40 years was OR =1.23 (95% CI 1.01-1.50). Paternal age was not associated with familial phacomatoses, and no consistent association was observed with maternal age.Conclusion: The findings show a consistent increase in risk of de novo occurrence of phacomatoses predisposing to nervous system tumors in offspring with increasing paternal age, most pronounced for neurofibromatosis, while maternal age did not seem to influence the risk. These findings suggest an increasing rate of new mutations in the NF1 and NF2 genes in spermatozoa of older fathers.",
author = "{Adel Fahmideh}, Maral and Giorgio Tettamanti and Catharina Lavebratt and Mats Talb{\"a}ck and Tiit Mathiesen and Birgitta Lannering and Johnson, {Kimberly J} and Maria Feychting",
year = "2018",
month = jun,
day = "20",
doi = "10.2147/CLEP.S159183",
language = "English",
volume = "10",
pages = "729--738",
journal = "Clinical Epidemiology",
issn = "1179-1349",
publisher = "Dove Medical Press Ltd",

}

RIS

TY - JOUR

T1 - Parental age and risk of genetic syndromes predisposing to nervous system tumors

T2 - nested case-control study

AU - Adel Fahmideh, Maral

AU - Tettamanti, Giorgio

AU - Lavebratt, Catharina

AU - Talbäck, Mats

AU - Mathiesen, Tiit

AU - Lannering, Birgitta

AU - Johnson, Kimberly J

AU - Feychting, Maria

PY - 2018/6/20

Y1 - 2018/6/20

N2 - Purpose: Phacomatoses are genetic syndromes that are associated with increased risk of developing nervous system tumors. Phacomatoses are usually inherited, but many develop de novo, with unknown etiology. In this population-based study, we investigated the effect of parental age on the risk of phacomatoses in offspring.Patients and methods: The study was a population-based nested case-control study. All individuals born and residing in Sweden between January 1960 and December 2010 were eligible for inclusion. Using the Patient Register, 4625 phacomatosis cases were identified and further classified as familial or nonfamilial. Ten matched controls per case were randomly selected from the eligible population. Data were analyzed using conditional logistic regression. Analyses were conducted for neurofibromatosis alone (n=2089) and other phacomatoses combined (n=2536).Results: Compared with offspring of fathers aged 25-29 years, increased risk estimates of nonfamilial neurofibromatosis were found for offspring of fathers aged 35-39 years (odds ratio [OR]=1.43 [95% CI 1.16-1.74]) and ≥40 years (OR =1.74 [95% CI 1.38-2.19]). For other nonfamilial phacomatoses, the risk estimate for offspring of fathers aged ≥40 years was OR =1.23 (95% CI 1.01-1.50). Paternal age was not associated with familial phacomatoses, and no consistent association was observed with maternal age.Conclusion: The findings show a consistent increase in risk of de novo occurrence of phacomatoses predisposing to nervous system tumors in offspring with increasing paternal age, most pronounced for neurofibromatosis, while maternal age did not seem to influence the risk. These findings suggest an increasing rate of new mutations in the NF1 and NF2 genes in spermatozoa of older fathers.

AB - Purpose: Phacomatoses are genetic syndromes that are associated with increased risk of developing nervous system tumors. Phacomatoses are usually inherited, but many develop de novo, with unknown etiology. In this population-based study, we investigated the effect of parental age on the risk of phacomatoses in offspring.Patients and methods: The study was a population-based nested case-control study. All individuals born and residing in Sweden between January 1960 and December 2010 were eligible for inclusion. Using the Patient Register, 4625 phacomatosis cases were identified and further classified as familial or nonfamilial. Ten matched controls per case were randomly selected from the eligible population. Data were analyzed using conditional logistic regression. Analyses were conducted for neurofibromatosis alone (n=2089) and other phacomatoses combined (n=2536).Results: Compared with offspring of fathers aged 25-29 years, increased risk estimates of nonfamilial neurofibromatosis were found for offspring of fathers aged 35-39 years (odds ratio [OR]=1.43 [95% CI 1.16-1.74]) and ≥40 years (OR =1.74 [95% CI 1.38-2.19]). For other nonfamilial phacomatoses, the risk estimate for offspring of fathers aged ≥40 years was OR =1.23 (95% CI 1.01-1.50). Paternal age was not associated with familial phacomatoses, and no consistent association was observed with maternal age.Conclusion: The findings show a consistent increase in risk of de novo occurrence of phacomatoses predisposing to nervous system tumors in offspring with increasing paternal age, most pronounced for neurofibromatosis, while maternal age did not seem to influence the risk. These findings suggest an increasing rate of new mutations in the NF1 and NF2 genes in spermatozoa of older fathers.

U2 - 10.2147/CLEP.S159183

DO - 10.2147/CLEP.S159183

M3 - Journal article

C2 - 29950902

VL - 10

SP - 729

EP - 738

JO - Clinical Epidemiology

JF - Clinical Epidemiology

SN - 1179-1349

ER -

ID: 218400025