The CHEK2 Variant C.349A>G Is Associated with Prostate Cancer Risk and Carriers Share a Common Ancestor

Eeles RA; Brandao A; Claessens F; Albanes D; Kogevinas M; Kaneva R; Brenner H; Cussenot O; Grindedal EM; Nielsen SF; John EM; Ingles SA; Vega A; Wiklund F; Berndt SI; Townsend PA; Pinheiro M; Tangen CM; Silva MP; Pashayan N; Logothetis CJ; Teixeira MR; Profile Study Steering Comm; PRACTICAL Consortium; Maia S; Kote-Jarai Z; Razack A; Stanford JL; Gago-Dominguez M; Penney KL; Santos C; Maier C; De Ruyck K; West CML; Cardoso M; Schleutker J; Park JY; Mucci LA; Batra J; Gronberg H; Lessel D; Travis RC; Neuhausen SL; Koutros S; Nordestgaard BG; Usmani N; Paulo P; Sorensen KD; Haiman CA; Cybulski C; Rosenstein BS; Wang Y; Neal DE; Wolk A; Kibel AS; Hamilton RJ; Newcomb LF; Southey MC; Peixoto A; Muir K; Roobol MJ

The CHEK2 Variant C.349A>G Is Associated with Prostate Cancer Risk and Carriers Share a Common Ancestor

Eeles RA; Brandao A; Claessens F; Albanes D; Kogevinas M; Kaneva R; Brenner H; Cussenot O; Grindedal EM; Nielsen SF; John EM; Ingles SA; Vega A; Wiklund F; Berndt SI; Townsend PA; Pinheiro M; Tangen CM; Silva MP; Pashayan N; Logothetis CJ; Teixeira MR; Profile Study Steering Comm; PRACTICAL Consortium; Maia S; Kote-Jarai Z; Razack A; Stanford JL; Gago-Dominguez M; Penney KL; Santos C; Maier C; De Ruyck K; West CML; Cardoso M; Schleutker J; Park JY; Mucci LA; Batra J; Gronberg H; Lessel D; Travis RC; Neuhausen SL; Koutros S; Nordestgaard BG; Usmani N; Paulo P; Sorensen KD; Haiman CA; Cybulski C; Rosenstein BS; Wang Y; Neal DE; Wolk A; Kibel AS; Hamilton RJ; Newcomb LF; Southey MC; Peixoto A; Muir K; Roobol MJ

The CHEK2 Variant C.349A>G Is Associated with Prostate Cancer Risk and Carriers Share a Common Ancestor

Eeles RA

Brandao A

Claessens F

Albanes D

Kogevinas M

Kaneva R

Brenner H

Cussenot O

Grindedal EM

Nielsen SF

John EM

Ingles SA

Vega A

Wiklund F

Berndt SI

Townsend PA

Pinheiro M

Tangen CM

Silva MP

Pashayan N

Logothetis CJ

Teixeira MR; Profile Study Steering Comm; PRACTICAL Consortium

Maia S

Kote-Jarai Z

Razack A

Stanford JL

Gago-Dominguez M

Penney KL

Santos C

Maier C

De Ruyck K

West CML

Cardoso M

Schleutker J

Park JY

Mucci LA

Batra J

Gronberg H

Lessel D

Travis RC

Neuhausen SL

Koutros S

Nordestgaard BG

Usmani N

Paulo P

Sorensen KD

Haiman CA

Cybulski C

Rosenstein BS

Wang Y

Neal DE

Wolk A

Kibel AS

Hamilton RJ

Newcomb LF

Southey MC

Peixoto A

Muir K

Roobol MJ

Katso/Avaa

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MDPI

doi:10.3390/cancers12113254

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Julkaisun pysyvä osoite on:
https://urn.fi/URN:NBN:fi-fe2021042824286

Tiivistelmä

Simple SummaryIt is well-recognised the strong contribution of genetic factors to prostate cancer (PrCa) susceptibility, thus genetic screening is critical for presymptomatic diagnosis and identification of individuals at high-risk. In this context, recurrent founder variants in cancer predisposing genes, by providing specific targets for early identification of carriers at risk of developing the disease, may be leveraged to implement cost-efficient targeted genetic screening strategies. The goal of this study was to investigate whether CHEK2 c.349A>G, the only recurrent "likely pathogenic" variant in CHEK2 gene reported in the Portuguese population, plays an important role in PrCa development, and the possibility of a founder effect behind its origin. Our results clearly demonstrate that c.349A>G in the CHEK2 tumour-suppressor gene is a founder variant significantly associated with an increased risk of PrCa, suggesting its potential usefulness for cost-effective targeted genetic screening in PrCa families.The identification of recurrent founder variants in cancer predisposing genes may have important implications for implementing cost-effective targeted genetic screening strategies. In this study, we evaluated the prevalence and relative risk of the CHEK2 recurrent variant c.349A>G in a series of 462 Portuguese patients with early-onset and/or familial/hereditary prostate cancer (PrCa), as well as in the large multicentre PRACTICAL case-control study comprising 55,162 prostate cancer cases and 36,147 controls. Additionally, we investigated the potential shared ancestry of the carriers by performing identity-by-descent, haplotype and age estimation analyses using high-density SNP data from 70 variant carriers belonging to 11 different populations included in the PRACTICAL consortium. The CHEK2 missense variant c.349A>G was found significantly associated with an increased risk for PrCa (OR 1.9; 95% CI: 1.1-3.2). A shared haplotype flanking the variant in all carriers was identified, strongly suggesting a common founder of European origin. Additionally, using two independent statistical algorithms, implemented by DMLE+2.3 and ESTIAGE, we were able to estimate the age of the variant between 2300 and 3125 years. By extending the haplotype analysis to 14 additional carrier families, a shared core haplotype was revealed among all carriers matching the conserved region previously identified in the high-density SNP analysis. These findings are consistent with CHEK2 c.349A>G being a founder variant associated with increased PrCa risk, suggesting its potential usefulness for cost-effective targeted genetic screening in PrCa families.

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