<i><scp>BRCA2</scp></i> gene: a candidate for clinical testing in familial colorectal cancer type X

Garré, Pilar; Martin, Lorena; Sanz, Julián; Romero, Atocha; Tosar, Alicia; Bando, Inmaculada; Llovet, Patricia; Diaque, P.; García-Paredes, Beatriz; Dı́az-Rubio, Eduardo; Hoya, Miguel de la; Caldés, Trinidad

doi:10.1111/cge.12427

Cited by 36 publications

(35 citation statements)

References 17 publications

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“…The increased risks of breast cancer with IRRs 1.5-1.7 in the age group 30-69 years and pancreatic cancer with an IRR of 2.2 after age 70 support the suggestion of disease-predisposing variants in BRCA2, causing the observed malignancies in a small subset of FCCTX families (Garre et al, 2015).…”

Section: Discussionsupporting

confidence: 57%

“…The genetic aetiology of FCCTX is most likely heterogenous and may include rare pathogenic germline variants in e.g. heterozygous MUTYH,CHEK2,BRCA2,POLE,POLD1,SEMA4A,BMPR1A,RPS20 or OGG1 or modifying single nucleotide polymorphisms in SEMA4A, EXO1, TGFBR1, or NUDT1 (Bellido et al, 2016;Dominguez-Valentin et al, 2018;Garre et al, 2011Garre et al, , 2015Hansen et al, 2015;Nieminen et al, 2011Nieminen et al, , 2014Schulz et al, 2014;Xicola et al, 2016).…”

Section: Introductionmentioning

confidence: 99%

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Broadening Risk Profile in Familial Colorectal Cancer Type X; increased risk for five cancer types in the national Danish cohort

Therkildsen

Rasmussen

Smith-Hansen

et al. 2020

Preprint

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Section: Discussionsupporting

confidence: 57%

Section: Introductionmentioning

confidence: 99%

Broadening Risk Profile in Familial Colorectal Cancer Type X; increased risk for five cancer types in the national Danish cohort

Therkildsen

Rasmussen

Smith-Hansen

et al. 2020

Preprint

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“…Previous studies have reported early-onset CRC in women with BRCA1 mutations 26 and BRCA2 mutations in families with familial colorectal cancer type X. 27 It is possible that these 13 mutations are incidental findings; however, the cancer spectrum and penetrance for many well-established and newly discovered genes will likely be redefined now that multigene panel testing is becoming more routine.…”

Section: Discussionmentioning

confidence: 99%

Prevalence and Spectrum of Germline Cancer Susceptibility Gene Mutations Among Patients With Early-Onset Colorectal Cancer

et al. 2017

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IMPORTANCE Hereditary cancer syndromes infer high cancer risks and require intensive cancer surveillance, yet the prevalence and spectrum of these conditions among unselected patients with early-onset colorectal cancer (CRC) is largely undetermined. OBJECTIVE To determine the frequency and spectrum of cancer susceptibility gene mutations among patients with early-onset CRC. DESIGN, SETTING, AND PARTICIPANTS Overall, 450 patients diagnosed with colorectal cancer younger than 50 years were prospectively accrued from 51 hospitals into the Ohio Colorectal Cancer Prevention Initiative from January 1, 2013, to June 20, 2016. Mismatch repair (MMR) deficiency was determined by microsatellite instability and/or immunohistochemistry. Germline DNA was tested for mutations in 25 cancer susceptibility genes using next-generation sequencing. MAIN OUTCOMES AND MEASURES Mutation prevalence and spectrum in patients with early-onset CRC was determined. Clinical characteristics were assessed by mutation status. RESULTS In total 450 patients younger than 50 years were included in the study, and 75 gene mutations were found in 72 patients (16%). Forty-eight patients (10.7%) had MMR-deficient tumors, and 40 patients (83.3%) had at least 1 gene mutation: 37 had Lynch syndrome (13, MLH1 [including one with constitutional MLH1 methylation]; 16, MSH2; 1, MSH2/monoallelic MUTYH; 2, MSH6; 5, PMS2); 1 patient had the APC c.3920T>A, p.I1307K mutation and a PMS2 variant; 9 patients (18.8%) had double somatic MMR mutations (including 2 with germline biallelic MUTYH mutations); and 1 patient had somatic MLH1 methylation. Four hundred two patients (89.3%) had MMR-proficient tumors, and 32 patients (8%) had at least 1 gene mutation: 9 had mutations in high-penetrance CRC genes (5, APC; 1, APC/PMS2; 2, biallelic MUTYH; 1, SMAD4); 13 patients had mutations in high- or moderate-penetrance genes not traditionally associated with CRC (3, ATM; 1, ATM/CHEK2; 2, BRCA1; 4, BRCA2; 1, CDKN2A; 2, PALB2); 10 patients had mutations in low-penetrance CRC genes (3, APC c.3920T>A, p.I1307K; 7, monoallelic MUTYH). Importantly, 24 of 72 patients (33.3%) who were mutation positive did not meet established genetic testing criteria for the gene(s) in which they had a mutation. CONCLUSIONS AND RELEVANCE Of 450 patients with early-onset CRC, 72 (16%) had gene mutations. Given the high frequency and wide spectrum of mutations, genetic counseling and testing with a multigene panel could be considered for all patients with early-onset CRC.

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“…158,159 Because of the likely enrichment of heritable risk factors in FCCTX families, they have been the basis of extensive gene discovery efforts using wholegenome and exome sequencing approaches. To date, germline mutations in BMPR1A and breast cancer 2 (BRCA2) have been reported to underlie a small proportion of FCCTX 134,160 as have germline mutations in POLE or POLD1 (<2%) (Figure 1), 58,161 justifying the application of extended CRC susceptibility gene testing through multigene panels. A number of candidate CRC genes have been identified in FCCTX including semaphorin A4 (SEMA4), 162 FANCD2/FANCI-associated nuclease 1 (FAN1), 163 and ribosomal protein S20 (RPS20).…”

Section: Familial Crc Type Xmentioning

confidence: 99%

Update on Hereditary Colorectal Cancer: Improving the Clinical Utility of Multigene Panel Testing

Lorans

Dow

Macrae

et al. 2018

Clinical Colorectal Cancer

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Colorectal cancer (CRC), one of the most common cancers, is a major public health issue globally, especially in Westernized countries. Up to 35% of CRCs are thought to be due to heritable factors, but currently only 5% to 10% of CRCs are attributable to high-risk mutations in known CRC susceptibility genes, predominantly the mismatch repair genes (Lynch syndrome) and adenomatous polyposis coli gene (APC; familial adenomatous polyposis). In this era of precision medicine, high-risk mutation carriers, when identified, can be offered various risk management options that prevent cancers and improve survival, including risk-reducing medication, screening for early detection, and surgery. The practice of clinical genetics is currently transitioning from phenotype-directed single gene testing to multigene panels, now offered by numerous providers. For CRC, the genes included across these panels vary, ranging from well established, clinically actionable susceptibility genes with quantified magnitude of risk, to genes that lack extensive validation or have less evidence of association with CRC and, therefore, have minimal clinical utility. The current lack of consensus regarding inclusion of genes in CRC panels presents challenges in patient counseling and management, particularly when a variant in a less validated gene is identified. Furthermore, there remain considerable challenges regarding variant interpretation even for the well established CRC susceptibility genes. Ironically though, only through more widespread testing and the accumulation of large international data sets will sufficient information be generated to (i) enable well powered studies to determine if a gene is associated with CRC susceptibility, (ii) to develop better models for variant interpretation and (iii) to facilitate clinical translation.

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BRCA2 gene: a candidate for clinical testing in familial colorectal cancer type X

Cited by 36 publications

References 17 publications

Broadening Risk Profile in Familial Colorectal Cancer Type X; increased risk for five cancer types in the national Danish cohort

Broadening Risk Profile in Familial Colorectal Cancer Type X; increased risk for five cancer types in the national Danish cohort

Prevalence and Spectrum of Germline Cancer Susceptibility Gene Mutations Among Patients With Early-Onset Colorectal Cancer

Update on Hereditary Colorectal Cancer: Improving the Clinical Utility of Multigene Panel Testing

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