Differences in cancer prevalence among CHEK2 carriers identified via multi-gene panel testing

支票2 杂合子优势 错义突变 癌症 前列腺癌 基因型 遗传学 生物 表型 内科学 肿瘤科 医学 基因 突变 种系突变
作者
Erin G. Sutcliffe,Amy Stettner,Stacey A. Miller,Sheila Solomon,Megan L. Marshall,Maegan E. Roberts,Lisa R. Susswein,Kevin J. Arvai,Rachel T. Klein,Patricia D. Murphy,Kathleen S. Hruska
出处
期刊:Cancer genetics [Elsevier BV]
卷期号:246-247: 12-17 被引量:30
标识
DOI:10.1016/j.cancergen.2020.07.001
摘要

Abstract

Purpose

Although CHEK2 is a well-established cancer gene, questions remain including whether risks vary substantially between different variants and whether biallelic carriers have higher risks than heterozygotes. We report on a cohort of individuals with CHEK2 pathogenic and likely pathogenic variants (collectively, PV) in order to better characterize this gene.

Methods

We retrospectively queried samples submitted for multi-gene hereditary cancer testing to identify individuals with CHEK2 PVs and assessed differences in phenotypes among various genotypes.

Results

CHEK2 PVs were identified in 2508 individuals, including 32 individuals with biallelic CHEK2 PVs. Breast (female, 59.9% and male, 11.8%), prostate (20.1%), and colorectal (3.5%), were among the most frequently reported cancers. Select missense PVs showed similar cancer prevalence to truncating PVs while some others showed lower prevalence. No significant differences were observed between biallelic carriers and heterozygotes.

Conclusions

Our data support that some, but not all, CHEK2 missense PVs demonstrate lower cancer prevalence; further studies are needed to continue characterizing possible variant specific risks. In addition, biallelic CHEK2 PVs do not appear to be associated with a more severe phenotype than single CHEK2 PVs. Furthermore, co-occurrences with PVs in other cancer risk genes are common among CHEK2 heterozygotes and often warrant additional management.
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