Prevalence of germline pathogenic variants in 22 cancer susceptibility genes in Swedish pediatric cancer patients

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作者
Kristoffer von Stedingk
Karl-Johan Stjernfelt
Anders Kvist
Cecilia Wahlström
Ulf Kristoffersson
Marie Stenmark-Askmalm
Thomas Wiebe
Lars Hjorth
Jan Koster
Håkan Olsson
Ingrid Øra
机构
[1] Lund University,Department of Pediatrics, Clinical Sciences
[2] Children’s Hospital,Pediatric Oncology and Hematology
[3] Skåne University Hospital,Department of Oncogenomics
[4] University Medical Center,Department of Oncology and Pathology, Clinical Sciences
[5] AMC,Department of Laboratory Medicine, Division of Clinical Genetics
[6] University of Amsterdam,Department of Oncology, Clinical Sciences
[7] Lund University,Department of Cancer Epidemiology, Clinical Sciences
[8] Lund University,undefined
[9] Lund University,undefined
[10] Lund,undefined
[11] University,undefined
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Up to 10% of pediatric cancer patients harbor pathogenic germline variants in one or more cancer susceptibility genes. A recent study from the US reported pathogenic variants in 22 out of 60 analyzed autosomal dominant cancer susceptibility genes, implicating 8.5% of pediatric cancer patients. Here we aimed to assess the prevalence of germline pathogenic variants in these 22 genes in a population-based Swedish cohort and to compare the results to those described in other populations. We found pathogenic variants in 10 of the 22 genes covering 3.8% of these patients. The prevalence of TP53 mutations was significantly lower than described in previous studies, which can largely be attributed to differences in tumor diagnosis distributions across the three cohorts. Matched family history for relatives allowed assessment of familial cancer incidence, however, no significant difference in cancer incidence was found in families of children carrying pathogenic variants compared to those who did not.
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