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Rare germline alterations in cancer-related genes associated with the risk of multiple primary tumor development
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Journal Article
Rare germline alterations in cancer-related genes associated with the risk of multiple primary tumor development
2017
Overview
Multiple primary tumors (MPT) have been described in carriers of inherited cancer predisposition genes. However, the genetic etiology of a large proportion of MPT cases remains unclear. We reviewed 267 patients with hereditary cancer predisposition syndromes (HCPS) that underwent genetic counseling and selected 22 patients with MPT to perform genomic analysis (CytoScan HD Array, Affymetrix) aiming to identify new alterations related to a high risk of developing MPT. Twenty patients had a positive family history of cancer and 11 met phenotypic criteria for HCPS. Genetic testing for each of the genes associated with these syndromes revealed negative results for pathogenic mutations. Seventeen rare germline copy number variations (CNVs) covering 40 genes were identified in 11 patients, including an
EPCAM
/
MSH2
deletion in one Lynch syndrome patient. An enrichment analysis revealed a significant number of genes (where the CNVs are mapped) associated with carcinogenesis and/or related to functions implicated with tumor development, such as proliferation and cell survival. An interaction network analysis highlighted the importance of
TP53
pathway in cancer emergence. A high number of germline copy-neutral loss of heterozygosity (cnLOH) was identified in nine cases, particularly in two patients. Eighteen genes were covered by both rare CNVs and cnLOH, including 14 related to tumorigenesis and seven genes (
ABCC1
,
KDM4C
,
KIAA0430
,
MYH11, NDE1
,
PIWIL2
, and
ULK2
) specifically associated with cellular growth and proliferation. Overall, we identified 14 cases with rare CNVs and/or cnLOH that may contribute to the risk of MPT development.
Key message
CNVs may explain the risk of hereditary cancer syndromes in MPT patients.
CNVs affecting genes related to cancer are candidates to be involved in MPT risk.
EPCAM
/
MSH2
deletions should be investigated in patients suspected to have LS.
Gene enrichment related to the
TP53
network is associated with MPT development.
cnLOH and CNVs contribute to the risk of MPT development.
Publisher
Springer Berlin Heidelberg,Springer Nature B.V
Subject
/ Biomedical and Life Sciences
/ Colorectal Neoplasms, Hereditary Nonpolyposis - genetics
/ DNA Copy Number Variations - genetics
/ Epithelial Cell Adhesion Molecule - genetics
/ Female
/ Genetic Predisposition to Disease - genetics
/ Humans
/ Loss of Heterozygosity - genetics
/ Male
