PALB2,CHEK2andATMrare variants and cancer risk: data from COGS

Southey, Melissa C.; Goldgar, David E.; Winqvist, Robert; Pylkäs, Katri; Couch, Fergus J.; Tischkowitz, Marc; Foulkes, William D.; Dennis, Joe; Michailidou, Kyriaki; Rensburg, Elizabeth J. van; Heikkinen, Tuomas; Nevanlinna, Heli; Hopper, John L.; Dörk, Thilo; Claes, Kathleen; Reis‐Filho, Jorge S.; Teo, Zhi L.; Radice, Paolo; Catucci, Irene; Peterlongo, Paolo; Tsimiklis, Helen; Odefrey, Fabrice; Dowty, James G.; Schmidt, Marjanka K.; Broeks, Annegien; Hogervorst, Frans B.L.; Verhoef, Senno; Carpenter, Jane; Clarke, Christine L.; Scott, Rodney J.; Fasching, Peter A.; Haeberle, Lothar; Ekici, Arif B.; Beckmann, Matthias W.; Peto, Julian; dos‐Santos‐Silva, Isabel; Fletcher, Olivia; Johnson, Nichola; Bolla, Manjeet K.; Sawyer, Elinor J.; Tomlinson, Ian; Kerin, Michael J.; Miller, Nicola; Marmé, Federik; Burwinkel, Barbara; Yang, Rongxi; Guénel, Pascal; Truong, Thérèse; Ménégaux, Florence; Sanchez, Marie; Bojesen, Stig E.; Nielsen, Sune F.; Flyger, Henrik; Benı́tez, Javier; Zamora, M. Pilar; Peŕez, José Ignacio Arias; Menéndez, Primitiva; Anton‐Culver, Hoda; Neuhausen, Susan L.; Ziogas, Argyrios; Clarke, Christina A.; Brenner, Hermann; Arndt, Volker; Stegmaier, Christa; Brauch, Hiltrud; Brüning, Thomas; Ko, Yon‐Dschun; Muranen, Taru; Aittomäki, Kristiina; Blomqvist, Carl; Bogdanova, Natalia; Antonenkova, Natalia; Lindblom, Annika; Margolin, Sara; Mannermaa, Arto; Kataja, Vesa; Kosma, Veli‐Matti; Hartikainen, Jaana M.; Spurdle, Amanda B.; Investigators, kConFab; Wauters, Els; Smeets, Dominiek; Beuselinck, Benoît; Floris, Giuseppe; Chang‐Claude, Jenny; Rudolph, Anja; Seibold, Petra; Flesch-Janys, Dieter; Olson, Janet E.; Vachon, Celine M.; Pankratz, V. Shane; McLean, Catriona; Haiman, Christopher A.; Henderson, Brian E.; Schumacher, Fredrick R.; Marchand, Loı̈c Le; Kristensen, Vessela N.; Alnæs, Grethe Grenaker; Wang, Zheng; Hunter, David J.; Lindström, Sara; Hankinson, Susan E.; Kraft, Peter; Andrulis, Irene L.; Knight, Julia A.; Glendon, Gord; Mulligan, Anna Marie; Jukkola-Vuorinen, Arja; Grip, Mervi; Kauppila, Saila; Devilee, Peter; Tollenaar, Robert A.E.M.; Seynaeve, Caroline; Hollestelle, Antoinette; García‐Closas, Montserrat; Figueroa, Jonine D.; Chanock, Stephen J.; Lissowska, Jolanta; Czene, Kamila; Darabi, Hatef; Eriksson, Mikael; Eccles, Diana M.; Rafiq, Sajjad; Tapper, William; Gerty, Sue; Hooning, Maartje J.; Martens, John W.M.; Collée, J. Margriet; Tilanus-Linthorst, Madeleine M.A.; Hall, Per; Li, Jingmei; Brand, Judith S.; Humphreys, Keith; Cox, Angela; Reed, Malcolm W. R.; Luccarini, Craig; Baynes, Caroline; Dunning, Alison M.; Hamann, Ute; Torres, Diana; Ulmer, Hans Ulrich; Rüdiger, Thomas; Jakubowska, Anna; Lubiński, Jan; Jaworska, Katarzyna; Durda, Katarzyna; Slager, Susan L.; Toland, Amanda E.; Ambrosone, Christine B.; Yannoukakos, Drakoulis; Swerdlow, Anthony J.; Ashworth, Alan; Orr, Nick; Jones, Michael E.; González‐Neira, Anna; Pita, Guillermo; Alonso, María R.; Álvarez, Núria; Herrero, Daniel; Tessier, Daniel C.; Denis, Vincent; Bertucci, François; Simard, Jacques; Dumont, Martine; Soucy, Penny; Eeles, Rosalind A.; Muir, Kenneth; Wiklund, Fredrik; Grönberg, Henrik; Schleutker, Johanna; Nordestgaard, Børge G.; Weischer, Maren; Travis, Ruth C.; Neal, David E.; Donovan, Jenny; Hamdy, Freddie C.; Khaw, Kay‐Tee; Stanford, Janet L.; Blot, William J.; Thibodeau, Stephen N.; Schaid, Daniel J.; Kelley, Joseph L.; Maier, Christiane; Kibel, Adam S.; Cybulski, Cezary; Cannon-Albright, Lisa; Butterbach, Katja; Park, Jong; Kaneva, Radka; Batra, Jyotsna; Teixeira, Manuel R.; Kóte-Jarai, Zsofia; Olama, Ali Amin Al; Benlloch, Sara; Renner, S.; Hartmann, Arndt; Hein, Alexander; Ruebner, Matthias; Lambrechts, Diether; Nieuwenhuysen, Els Van; Vergote, Ignace; Lambretchs, Sandrina; Doherty, Jennifer A.; Rossing, Mary Anne; Nickels, Stefan; Eilber, Ursula; Wang-Gohrke, Shan; Odunsi, Kunle; Sucheston‐Campbell, Lara E.; Friel, Grace; Lurie, Galina; Killeen, Jeffrey; Wilkens, Lynne R.; Goodman, Marc T.; Runnebaum, Ingo B.; Hillemanns, Peter; Pelttari, Liisa M.; Bützow, Ralf; Modugno, Francesmary; Edwards, Robert P.; Ness, Roberta B.; Moysich, Kirsten B.; Bois, Andreas du; Heitz, Florian; Harter, Philipp; Kommoss, Stefan; Karlan, Beth Y.; Walsh, Christine; Lester, Jenny; Jensen, Allan; Kjær, Susanne K.; Høgdall, Estrid; Peissel, Bernard; Bonanni, Bernardo; Bernard, Loris; Goode, Ellen L.; Fridley, Brooke L.; Vierkant, Robert A.; Cunningham, Julie M.; Larson, Melissa C.; Fogarty, Zachary; Kalli, Kimberly R.; Liang, Dong; Lu, Karen H.; Hildebrandt, Michelle A.T.; Wu, Xifeng; Levine, Douglas A.; Dao, Fanny; Bisogna, Maria; Berchuck, Andrew; Iversen, Edwin S.; Marks, Jeffrey R.; Akushevich, Lucy; Cramer, Daniel W.; Schildkraut, Joellen M.; Terry, Kathryn L.; Poole, Elizabeth M.; Stampfer, Meir J.; Tworoger, Shelley S.; Bandera, Elisa V.; Orlow, Irene; Olson, Sara H.; Bjørge, Line; Salvesen, Helga B.; Altena, Anne M. van; Aben, K.K.H.; Kiemeney, Lambertus A.; Massuger, Leon F.A.G.; Pejović, Tanja; Bean, Yukie T.; Brooks‐Wilson, Angela; Kelemen, Linda E.; Cook, Linda S.; Le, Nhu D.; Górski, Bohdan; Gronwald, Jacek; Menkiszak, Janusz; Høgdall, Claus; Lundvall, Lene; Nedergaard, Lotte; Engelholm, Svend Aage; Dicks, Ed; Tyrer, Jonathan P.; Campbell, Ian G.; McNeish, Iain A.; Paul, James; Siddiqui, Nadeem; Glasspool, Rosalind; Whittemore, Alice S.; Rothstein, Joseph H.; McGuire, Valerie; Sieh, Weiva; Cai, Hui; Shu, Xiao‐Ou; Teten, Rachel Threet; Sutphen, Rebecca; McLaughlin, John; Narod, Steven A.; Phelan, Catherine M.; Monteiro, Álvaro N.A.; Fenstermacher, David; Lin, Hui‐Yi; Permuth, Jennifer B.; Sellers, Thomas A.; Chen, Y Ann; Tsai, Ya-Yu; Chen, Zhihua; Gentry‐Maharaj, Aleksandra; Gayther, Simon A.; Ramus, Susan J.; Menon, Usha; Wu, Anna H.; Pearce, Celeste Leigh; Berg, David Van Den; Pike, Malcolm C.; Dansonka-Mieszkowska, Agnieszka; Plisiecka-Hałasa, Joanna; Moes-Sosnowska, Joanna; Kupryjańczyk, Jolanta; Pharoah, Paul D.P.; Song, Honglin; Winship, Ingrid; Chenevix‐Trench, Georgia; Giles, Graham G.; Tavtigian, Sean V.; Easton, Doug; Milne, Roger L.

doi:10.1136/jmedgenet-2016-103839

Cited by 179 publications

(143 citation statements)

References 35 publications

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“…These two studies [2, 3] together identified the p.Leu939Trp mutation in 10/1741 (0.57 %) women with breast cancer and 8/1534 (0.52 %) unaffected controls, suggesting that this mutation is not associated with breast cancer risk. Further, we later published a third study corroborating this null finding [4] and have subsequently reported additional evidence that the p.Leu939Trp mutation is not associated with breast cancer risk, based on genotyping of 42,671 breast cancer cases and 42,164 controls (odds ratio = 1.05, 95 % confidence interval = 0.83–1.32, p value = 0.70) [5]. Finally, we observed that the p.Leu939Trp mutation does not disrupt the HR-mediated DNA repair activity of PALB2 (Fig.…”

Section: Textmentioning

confidence: 91%

The PALB2 p.Leu939Trp mutation is not associated with breast cancer risk

et al. 2016

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Section: Textmentioning

confidence: 91%

The PALB2 p.Leu939Trp mutation is not associated with breast cancer risk

et al. 2016

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“…The risk is particularly high in women with rare high-penetrance sequence variants, such as mutations in BRCA1 or BRCA2, where the 10-year risk may approach 25% to 30% (4,5). Mutations in CHEK2 also increase the risk of CBC, albeit to a lesser degree (6,7), and rare pathogenic PALB2 mutations have also been shown to increase the risk of CBC (8,9). In some family studies and within subgroups of breast cancer patients, rare mutations in the ATM gene have also been shown to increase the risk of CBC (10,11).…”

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confidence: 99%

Association of Common Genetic Variants With Contralateral Breast Cancer Risk in the WECARE Study

Robson

Reiner

Brooks

et al. 2017

JNCI: Journal of the National Cancer Institute

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Background: Women with unilateral breast cancer (UBC) are at risk of developing a subsequent contralateral breast cancer (CBC). Common variants are associated with breast cancer risk. Whether these influence CBC risk is unknown. Methods: Participants were breast cancer cases from the population-based Women's Environmental Cancer and Radiation Epidemiology (WECARE) Study. Sixty-seven established breast cancer risk loci were genotyped directly or by imputation in 1459 case subjects with CBC and 2126 UBC control subjects. An unweighted polygenic risk score (PRS) was created by summing the number of risk alleles for each directly genotyped single nucleotide polymorphism (SNP), or for imputed loci, the imputed dosage. A weighted PRS was calculated similarly, but where each SNP's contribution was weighted by the published per-allele log odds ratio. Unweighted and weighted polygenic risk scores and CBC risk were modeled using conditional logistic regression. Cumulative CBC risk was estimated and benchmarked using Surveillance, Epidemiology, and End Results population incidence rates. Results: Both unweighted and weighted PRS were statistically significantly associated with CBC risk. The adjusted risk ratio of CBC in women in the upper quartile of unweighted PRS compared with the lowest quartile was 1.63 (95% confidence interval [CI] ¼ 1.33 to 2.00). The estimated 10-year cumulative risk for women in the upper quartile of the unweighted PRS was 7.4% (95% CI ¼ 6.0% to 9.1%). For women in the upper quartile of the weighted PRS, the risk ratio for CBC was 1.75 (95% CI ¼ 1.41 to 2.18) compared with women in the lowest quartile. There was no statistically significant heterogeneity by age, treatment (radiation therapy dose, tamoxifen, chemotherapy), estrogen receptor status of the first primary, histology of the first primary, length of at-risk period for CBC, or breast cancer family history.

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“…mutations descending from a single ancestor have been described for example in genes causing familial breast cancer. [47][48][49][50][51] Chondrocytic cell lines were not available for the predictions of the promoter and enhancer regions. Instead data from HSMM and GM12878 cell lines were used.…”

Section: Discussionmentioning

confidence: 99%

A Whole Exome Study Identifies Novel Candidate Genes for Vertebral Bone Marrow Signal Changes (Modic Changes)

Kraatari

Skarp

Niinimäki

et al. 2017

Spine

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Study Design. Family-based study Objective. To identify rare genetic factors predisposing to Modic changes (MC).Summary of Background Data. Lumbar disc degeneration (LDD) is one of the contributing factors behind low back pain (LBP). Lumbar MC visualized as bone marrow signal intensity changes on magnetic resonance imaging (MRI) represent a specific phenotype of LDD, which has stronger association with LBP than LDD without MC.Methods. The study set consisted of two Finnish families: Family I included seven affected and four unaffected individuals and Family II eight affected and seven unaffected individuals. MC were evaluated in 26 individuals using MRI. Whole exome sequencing was used to identify alleles co-segregating with MC. ANNOVAR was used to carry out functional annotation of alleles and their frequencies were evaluated using 1000Genomes, Sequencing Initiative Suomi (SISu) and the Exome Aggregation Consortium (ExAC) databases.Results. We identified predisposing genetic alleles for MC in two Finnish families. In each family only single allele co-segregated with MC. In Family I the observed allele was an insertion and deletion in the HSPG2 gene, resulting in a premature termination codon. In Family II a single nucleotide polymorphism (rs61753465) in the MAML1 gene was identified in all affected family members.Conclusions. We have identified two novel candidate genes, MAML1 and HSPG2, associating with MC. These genes are important in cartilage structure and joint cartilage maintenance. Our findings are novel among lumbar spine degenerative phenotypes.3

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PALB2,CHEK2andATMrare variants and cancer risk: data from COGS

Cited by 179 publications

References 35 publications

The PALB2 p.Leu939Trp mutation is not associated with breast cancer risk

The PALB2 p.Leu939Trp mutation is not associated with breast cancer risk

Association of Common Genetic Variants With Contralateral Breast Cancer Risk in the WECARE Study

A Whole Exome Study Identifies Novel Candidate Genes for Vertebral Bone Marrow Signal Changes (Modic Changes)

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