Association of Genomic Domains in <i>BRCA1</i> and <i>BRCA2</i> with Prostate Cancer Risk and Aggressiveness

Patel, Vivek; Busch, Evan L.; Friebel, Tara M.; Cronin, Angel M.; Leslie, Goska; McGuffog, Lesley; Adlard, Julian; Agata, Simona; Agnarsson, Bjarni A.; Ahmed, Munaza; Aittomäki, Kristiina; Alducci, Elisa; Andrulis, Irene L.; Arason, Aðalgeir; Arnold, Norbert; Artioli, Grazia; Arver, Brita; Auber, Bernd; Azzollini, Jacopo; Balmañà, Judith; Barkardóttir, Rósa B.; Barnes, Daniel R.; Barroso, Alicia; Barrowdale, Daniel; Belotti, Muriel; Benı́tez, Javier; Bertelsen, Brigitte; Blok, Marinus J.; Bodrogi, I.; Bonadona, Valérie; Bonanni, Bernardo; Bondavalli, Davide; Boonen, Susanne E.; Borde, Julika; Borg, Åke; Bradbury, Angela R.; Brady, Angela; Brewer, Carole; Brunet, Joan; Bruno, Benedetto; Buys, Saundra S.; Cabezas-Camarero, Santiago; Caldés, Trinidad; Caliebe, Almuth; Caligo, Maria A.; Calvello, Mariarosaria; Campbell, Ian G.; Carnevali, Ileana; Carrasco, Estela; Chan, Tsun Leung; Chu, Annie; Chung, Wendy K.; Claes, Kathleen; Cook, Jackie; Cortesi, Laura; Couch, Fergus J.; Daly, Mary B.; Damante, Giuseppe; Darder, Esther; Davidson, Rosemarie; Hoya, Miguel de la; Puppa, Lara Della; Dennis, Joe; Dı́ez, Orland; Ding, Yuan Chun; Ditsch, Nina; Domchek, Susan M.; Donaldson, Alan; Dworniczak, Bernd; Easton, Douglas F.; Eccles, Diana; Eeles, Rosalind; Ehrencrona, Hans; Ejlertsen, Bent; Engel, Christoph; Evans, D. Gareth; Faivre, Laurence; Faust, Ulrike; Feliubadaló, Lídia; Foretová, Lenka; Fostira, Florentia; Fountzilas, George; Frost, Debra; García-Barberán, Vanesa; Garré, Pilar; Gauthier‐Villars, Marion; Gergely, Lajos; Gehrig, Andrea; Gerdes, Anne-Marie; Gesta, Paul; Giannini, Giuseppe; Glendon, Gord; Godwin, Andrew K.; Goldgar, David E.; Greene, Mark H.; Gutierrez‐Barrera, Angelica M.; Hahnen, Eric; Hamann, Ute; Hauke, Jan; Herold, N; Hogervorst, Frans B.L.; Honisch, Ellen; Hopper, John L.; Hulick, Peter J.; Investigators, kConFab; Investigators, Hebon; Izatt, Louise; Jager, Agnes; James, Paul; Janavičius, Ramūnas; Jensen, Uffe Birk; Jensen, Thomas D.; Jóhannsson, Óskar T.; John, Esther M.; Vijai, Joseph; Kang, Eunyoung; Kast, Karin; Kiiski, Johanna I.; Kim, Sung-Won; Kim, Zisun; Ko, Kwang-Pil; Konstantopoulou, Irene; Kramer, Gero; Krogh, Lotte Nylandsted; Kruse, Torben A.; Kwong, Ava; Larsen, Mirjam; Lasset, Christine; Lautrup, Charlotte Kvist; Lázaro, Conxi; Lee, Jihyoun; Lee, Jong Won; Lee, Min Hyuk; Lemke, Johannes R.; Lesueur, Fabienne; Liljegren, Annelie; Lindblom, Annika; Llovet, Patricia; López‐Fernández, Adrià; López‐Perolio, Irene; Lorca, Víctor; Loud, Jennifer T.; Edmond, S. K.; Phuong, L.; Manoukian, Siranoush; Mari, Véronique; Martin, Lynn; Matricardi, Laura; Mebirouk, Noura; Medici, Veronica; Meijers-Heijboer, Hanne; Meindl, Alfons; Mensenkamp, Arjen R.; Miller, Clare M.; Gomes, D. Molina; Montagna, Marco; Mooij, Thea M.; Moserle, Lidia; Mouret-Fourme, Emmanuelle; Mulligan, Anna Marie; Nathanson, Katherine L.; Navrátilová, Marie; Nevanlinna, Heli; Niederacher, Dieter; Nielsen, Finn C.; Ņikitina-Zaķe, Liene; Offit, Kenneth; Olàh, Edith; Olopade, Olufunmilayo I.; Ong, Kai-Ren; Osorio, Ana; Ott, Claus‐Eric; Palli, Domenico; Park, Sue Kyung; Parsons, Michael T.; Pedersen, Inge Søkilde; Peissel, Bernard; Peixoto, Ana; Pérez‐Segura, Pedro; Peterlongo, Paolo; Petersen, Annabeth Høgh; Porteous, Mary; Pujana, Miguel Ángel; Radice, Paolo; Ramser, Juliane; Rantala, Johanna; Rashid, Muhammad Usman; Rhiem, Kerstin; Rizzolo, Piera; Robson, Mark E.; Rookus, Matti A.; Rossing, Caroline Maria; Ruddy, Kathryn J.; Santos, Catarina; Saule, Claire; Scarpitta, Rosa; Schmutzler, Rita K.; Schuster, Hélène; Senter, Leigha; Seynaeve, Caroline; Shah, Payal D.; Sharma, Priyanka; Shin, Vivian Y.; Silvestri, Valentina; Simard, Jacques; Singer, Christian F.; Skytte, Anne‐Bine; Snape, Katie; Solano, Angela; Soucy, Penny; Southey, Melissa C.; Spurdle, Amanda B.; Steele, Linda; Steinemann, Doris; Stoppa‐Lyonnet, Dominique; Stradella, Agostina; Sunde, Lone; Sutter, Christian; Tan, Yen Y.; Teixeira, Manuel R.; Teo, Soo Hwang; Thomassen, Mads; Tibiletti, Maria Grazia; Tischkowitz, Marc; Tognazzo, Silvia; Toland, Amanda E.; Tommasi, Stefania; Torres, Diana; Toss, Angela; Trainer, Alison H.; Tung, Nadine; Asperen, Christi J. van; Baan, Frederieke H. van der; Kolk, Lizet E. van der; Luijt, Rob B. van der; Hest, Liselotte P. van; Varesco, Liliana; Varon-Mateeva, Raymonda; Viel, Alessandra; Vierstraete, Jeroen; Villa, Roberta; Wachenfeldt, Anna von; Wagner, Philipp; Wang-Gohrke, Shan; Wappenschmidt, Barbara; Weitzel, Jeffrey N.; Wieme, Greet; Yadav, Siddhartha; Yannoukakos, Drakoulis; Yoon, Sook‐Yee; Zanzottera, Cristina; Zorn, Kristin K.; D’Amico, Anthony V.; Freedman, Matthew L.; Pomerantz, Mark; Chenevix-Trench, Georgia; Antoniou, Antonis C.; Neuhausen, Susan L.; Ottini, Laura; Nielsen, Henriette Roed; Rebbeck, Timothy R.

doi:10.1158/0008-5472.can-19-1840

Cited by 39 publications

(32 citation statements)

References 54 publications

(74 reference statements)

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“…This corresponds to a significantly higher PCa risk associated with PVs in the PCCR than PVs not in the PCCR (HR = 2.34, 95% CI 1.09–5.03; Table 1 ). Compared with PVs in the region c.1001 to c.7913 [8] , PCCR PVs were associated with an HR of 2.09 (95% CI 0.98–4.45). As previously reported, the SIR for carriers of PVs in the wide definition of the OCCR ( n = 178) was 2.46 (95% CI 1.07–5.64) [1] , and the risk for carriers of PCCR PVs was also significantly higher than that for OCCR PV carriers (HR = 3.41, 95% CI 1.27–9.16).…”

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confidence: 96%

“…PVs in the OCCR have consistently been shown to be associated with an increased ovarian cancer risk but a decreased breast cancer risk [2] , [3] , [5] , [6] , although the precise boundaries of the OCCR [3] , [5] and the mechanisms behind this risk variation remain uncertain. It has been proposed that the likelihood that a PV triggers nonsense-mediated mRNA decay varies by genomic region [7] , [8] so that OCCR PVs might produce a truncated or alternatively spliced protein the capability of which to suppress tumours varies by cancer type [2] , [3] , [5] , [7] , [8] , but there is currently no experimental support for this hypothesis [7] . Shortly after the publication of our manuscript, Patel and coworkers [8] proposed the existence of a prostate cancer cluster region (PCCR) at the 3′ end of BRCA2 , based on retrospective cohort data.…”

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confidence: 99%

“…It has been proposed that the likelihood that a PV triggers nonsense-mediated mRNA decay varies by genomic region [7] , [8] so that OCCR PVs might produce a truncated or alternatively spliced protein the capability of which to suppress tumours varies by cancer type [2] , [3] , [5] , [7] , [8] , but there is currently no experimental support for this hypothesis [7] . Shortly after the publication of our manuscript, Patel and coworkers [8] proposed the existence of a prostate cancer cluster region (PCCR) at the 3′ end of BRCA2 , based on retrospective cohort data. This retrospective study reported that men with BRCA2 PVs in the proposed PCCR have a higher risk of PCa (hazard ratio [HR] = 1.78, 95% confidence interval [CI] 1.25–2.52), particularly Gleason score ≥8 PCa (HR = 3.11, 95% CI 1.63–5.95), than men with PVs in the reference region c.1001 to c.7913, but did not present estimates of the absolute PCa risk for PCCR PV carriers [8] .…”

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confidence: 99%

“…Shortly after the publication of our manuscript, Patel and coworkers [8] proposed the existence of a prostate cancer cluster region (PCCR) at the 3′ end of BRCA2 , based on retrospective cohort data. This retrospective study reported that men with BRCA2 PVs in the proposed PCCR have a higher risk of PCa (hazard ratio [HR] = 1.78, 95% confidence interval [CI] 1.25–2.52), particularly Gleason score ≥8 PCa (HR = 3.11, 95% CI 1.63–5.95), than men with PVs in the reference region c.1001 to c.7913, but did not present estimates of the absolute PCa risk for PCCR PV carriers [8] . In order to substantiate or refute this association, and to provide direct estimates of the absolute risk of PCa for carriers of BRCA2 PCCR PVs, we have reanalysed our prospective data.…”

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confidence: 99%

“…Detailed information on the cohort and on inclusion criteria, data collection, follow-up, and statistical analysis approach is available in our recent publication [1] . The participants’ PVs (listed in Supplementary Table S1) were grouped on the basis of position within the BRCA2 gene, based on the proposed PCCR (c.7914 to 3′ [8] ; HGVS nomenclature [ http://varnomen.hgvs.org/ ]; using cDNA reference sequence NM_000059.3 and reference genome hg18) and the wide definition of the OCCR (c.2831 to c.6401) [1] , [2] , [3] , [4] . We additionally considered the region bounded by c.756 and c.1000 in which Patel and coworkers [8] found evidence of an increased PCa risk, but due to a small sample size ( n = 1) we could not estimate the PCa risk associated with this region.…”

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confidence: 99%

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Prostate Cancer Risk by BRCA2 Genomic Regions

et al. 2020

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A BRCA2 prostate cancer cluster region (PCCR) was recently proposed (c.7914 to 3′) wherein pathogenic variants (PVs) are associated with higher prostate cancer (PCa) risk than PVs elsewhere in the BRCA2 gene. Using a prospective cohort study of 447 male BRCA2 PV carriers recruited in the UK and Ireland from 1998 to 2016, we estimated standardised incidence ratios (SIRs) compared with population incidences and assessed variation in risk by PV location. Carriers of PVs in the PCCR had a PCa SIR of 8.33 (95% confidence interval [CI] 4.46–15.6) and were at a higher risk of PCa than carriers of other BRCA2 PVs (SIR = 3.31, 95% CI 1.97–5.57; hazard ratio = 2.34, 95% CI 1.09–5.03). PCCR PV carriers had an estimated cumulative PCa risk of 44% (95% CI 23–72%) by the age of 75 yr and 78% (95% CI 54–94%) by the age of 85 yr. Our results corroborate the existence of a PCCR in BRCA2 in a prospective cohort. Patient summary In this report, we investigated whether the risk of prostate cancer for men with a harmful mutation in the BRCA2 gene differs based on where in the gene the mutation is located. We found that men with mutations in one region of BRCA2 had a higher risk of prostate cancer than men with mutations elsewhere in the gene.

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Prostate Cancer Risk by BRCA2 Genomic Regions

et al. 2020

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Characterization of the Cancer Spectrum in Men With GermlineBRCA1andBRCA2Pathogenic Variants

Silvestri¹,

Leslie²,

Barnes³

et al. 2020

JAMA Oncol

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and the CIMBA Group IMPORTANCE The limited data on cancer phenotypes in men with germline BRCA1 and BRCA2 pathogenic variants (PVs) have hampered the development of evidence-based recommendations for early cancer detection and risk reduction in this population. OBJECTIVE To compare the cancer spectrum and frequencies between male BRCA1 and BRCA2 PV carriers. DESIGN, SETTING, AND PARTICIPANTS Retrospective cohort study of 6902 men, including 3651 BRCA1 and 3251 BRCA2 PV carriers, older than 18 years recruited from cancer genetics clinics from 1966 to 2017 by 53 study groups in 33 countries worldwide collaborating through the Consortium of Investigators of Modifiers of BRCA1/2 (CIMBA). Clinical data and pathologic characteristics were collected.MAIN OUTCOMES AND MEASURES BRCA1/2 status was the outcome in a logistic regression, and cancer diagnoses were the independent predictors. All odds ratios (ORs) were adjusted for age, country of origin, and calendar year of the first interview.RESULTS Among the 6902 men in the study (median [range] age, 51.6 [18-100] years), 1634 cancers were diagnosed in 1376 men (19.9%), the majority (922 of 1,376 [67%]) being BRCA2 PV carriers. Being affected by any cancer was associated with a higher probability of being a BRCA2, rather than a BRCA1, PV carrier (OR, 3.23; 95% CI, 2.81-3.70; P < .001), as well as developing 2 (OR, 7.97; 95% CI, 5.47-11.60; P < .001) and 3 (OR, 19.60; 95% CI, 4.64-82.89; P < .001) primary tumors. A higher frequency of breast (OR, 5.47; 95% CI, 4.06-7.37; P < .001) and prostate (OR, 1.39; 95% CI, 1.09-1.78; P = .008) cancers was associated with a higher probability of being a BRCA2 PV carrier. Among cancers other than breast and prostate, pancreatic cancer was associated with a higher probability (OR, 3.00; 95% CI, 1.55-5.81; P = .001) and colorectal cancer with a lower probability (OR, 0.47; 95% CI, 0.29-0.78; P = .003) of being a BRCA2 PV carrier.CONCLUSIONS AND RELEVANCE Significant differences in the cancer spectrum were observed in male BRCA2, compared with BRCA1, PV carriers. These data may inform future recommendations for surveillance of BRCA1/2-associated cancers and guide future prospective studies for estimating cancer risks in men with BRCA1/2 PVs.

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Identification of novel prostate cancer genes in patients stratified by Gleason classification: Role of antitumoral genes

Guardia-Bolívar

Barrios‐Rodríguez

Zwir

et al. 2022

Intl Journal of Cancer

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Prostate cancer (PCa) is a tumor with a great heterogeneity, both at a molecular and clinical level. Despite its global good prognosis, cases can vary from indolent to lethal metastatic and scientific efforts are aimed to discern those with worse outcomes. Current prognostic markers, as Gleason score, fall short when it comes to distinguishing these cases. Identification of new early biomarkers to enable a better PCa distinction and classification remains a challenge. In order to identify new genes implicated in PCa progression we conducted several differential gene expression analyses over paired samples comparing primary PCa tissue against healthy prostatic tissue of PCa patients. The results obtained show that this approach is a serious alternative to overcome patient heterogeneity. We were able to identify 250 genes whose expression varies along with tissue differentiation—healthy to tumor tissue, 161 of these genes are described here for the first time to be related to PCa. The further manual curation of these genes allowed to annotate 39 genes with antitumoral activity, 22 of them described for the first time to be related to PCa proliferation and metastasis. These findings could be replicated in different cohorts for most genes. Results obtained considering paired differential expression, functional annotation and replication results point to: CGREF1, UNC5A, C16orf74, LGR6, IGSF1, QPRT and CA14 as possible new early markers in PCa. These genes may prevent the progression of the disease and their expression should be studied in patients with different outcomes.

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Association of Genomic Domains in BRCA1 and BRCA2 with Prostate Cancer Risk and Aggressiveness

Cited by 39 publications

References 54 publications

Prostate Cancer Risk by BRCA2 Genomic Regions

Prostate Cancer Risk by BRCA2 Genomic Regions

Characterization of the Cancer Spectrum in Men With GermlineBRCA1andBRCA2Pathogenic Variants

Identification of novel prostate cancer genes in patients stratified by Gleason classification: Role of antitumoral genes

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