Melbourne School of Population and Global Health - Research Publications

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Author: Southey, Melissa × End date: 2016 × Type: Journal Article ×

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    Identification of new breast cancer predisposition genes via whole exome sequencing
    Southey, MC ; Park, DJ ; Lesueur, F ; Odefrey, F ; Nguyen-Dumont, T ; Hammet, F ; Neuhausen, SL ; John, EM ; Andrulis, IL ; Chenevix-Trench, G ; Baglietto, L ; Le Calvez-Kelm, F ; Pertesi, M ; Lonie, A ; Pope, B ; Sinilnikova, O ; Tsimiklis, H ; Giles, GG ; Hopper, JL ; Tavtigian, SV ; Goldgar, DE (Springer Science and Business Media LLC, 2012-01)
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    Mould-sensitized adults have lower Th2 cytokines and a higher prevalence of asthma than those sensitized to other aeroallergens
    Matheson, MC ; Reece, JC ; Kandane-Rathnayake, RK ; Tang, MLK ; Simpson, JA ; Feather, IH ; Southey, MC ; Tsimiklis, H ; Hopper, JL ; Morrison, SC ; Giles, GG ; Walters, EH ; Dharmage, SC (WILEY, 2016-12)
    BACKGROUND: Evidence suggests that specific allergen sensitizations are associated with different allergic diseases which may reflect different underlying immune profiles. We aimed to examine the cytokine profiles of individuals sensitized to eight common aeroallergens. METHODS: We used data from the Tasmanian Longitudinal Health Study a population-based cohort study of 45-year-olds. Serum cytokines (IL-4, IL-5, IL-6, IL-8, IL-10, TNF-α) were measured in 1157 subjects using the LINCOplex assays. Participants underwent skin prick testing for house dust mite, cat, grasses and moulds. Multivariable linear regression was used to compare serum cytokine levels between sensitized and nonatopic subjects. RESULTS: The prevalence of allergic sensitization to any aeroallergen was 51% (95% CI 47-54). Being sensitized to any aeroallergen was strongly associated with current asthma (OR = 3.7, 95% CI 2.6-5.3), and being sensitized to any moulds was associated with a very high risk of current asthma (OR = 6.40, 95% CI 4.06-10.1). The geometric mean (GM) levels of Th2 cytokines (IL-4, IL-5 and IL-6) for adults sensitized to Cladosporium were significantly lower than the levels for nonatopic individuals (IL-4 ratio of GMs = 0.25, 95% CI 0.10-0.62, P = 0.003; IL-5 GM = 0.55, 95% CI 0.30-0.99, P = 0.05; and IL-6 GM = 0.50, 95% CI 0.24-1.07, P = 0.07). Individuals sensitized to other aeroallergens all showed elevated Th2 cytokine levels. CONCLUSION: Our study is the first large population-based study to demonstrate reduced Th2 cytokines levels in people sensitized to mould. Underlying biological mechanisms driving allergic inflammatory responses in adults sensitized to moulds may differ from those sensitized to other aeroallergens. These findings suggest that it may be necessary to tailor treatments in individuals sensitized to moulds compared with other aeroallergens in order to optimize outcomes.
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    Fine-scale mapping of 8q24 locus identifies multiple independent risk variants for breast cancer
    Shi, J ; Zhang, Y ; Zheng, W ; Michailidou, K ; Ghoussaini, M ; Bolla, MK ; Wang, Q ; Dennis, J ; Lush, M ; Milne, RL ; Shu, X-O ; Beesley, J ; Kar, S ; Andrulis, IL ; Anton-Culver, H ; Arndt, V ; Beckmann, MW ; Zhao, Z ; Guo, X ; Benitez, J ; Beeghly-Fadiel, A ; Blot, W ; Bogdanova, NV ; Bojesen, SE ; Brauch, H ; Brenner, H ; Brinton, L ; Broeks, A ; Bruening, T ; Burwinkel, B ; Cai, H ; Canisius, S ; Chang-Claude, J ; Choi, J-Y ; Couch, FJ ; Cox, A ; Cross, SS ; Czene, K ; Darabi, H ; Devilee, P ; Droit, A ; Dork, T ; Fasching, PA ; Fletcher, O ; Flyger, H ; Fostira, F ; Gaborieau, V ; Garcia-Closas, M ; Giles, GG ; Grip, M ; Guenel, P ; Haiman, CA ; Hamann, U ; Hartman, M ; Miao, H ; Hollestelle, A ; Hopper, JL ; Hsiung, C-N ; Investigators, K ; Ito, H ; Jakubowska, A ; Johnson, N ; Torres, D ; Kabisch, M ; Kang, D ; Khan, S ; Knight, JA ; Kosma, V-M ; Lambrechts, D ; Li, J ; Lindblom, A ; Lophatananon, A ; Lubinski, J ; Mannermaa, A ; Manoukian, S ; Le Marchand, L ; Margolin, S ; Marme, F ; Matsuo, K ; McLean, C ; Meindl, A ; Muir, K ; Neuhausen, SL ; Nevanlinna, H ; Nord, S ; Borresen-Dale, A-L ; Olson, JE ; Orr, N ; van den Ouweland, AMW ; Peterlongo, P ; Putti, TC ; Rudolph, A ; Sangrajrang, S ; Sawyer, EJ ; Schmidt, MK ; Schmutzler, RK ; Shen, C-Y ; Hou, M-F ; Shrubsole, MJ ; Southey, MC ; Swerdlow, A ; Teo, SH ; Thienpont, B ; Toland, AE ; Tollenaar, RAEM ; Tomlinson, I ; Truong, T ; Tseng, C-C ; Wen, W ; Winqvist, R ; Wu, AH ; Yip, CH ; Zamora, PM ; Zheng, Y ; Floris, G ; Cheng, C-Y ; Hooning, MJ ; Martens, JWM ; Seynaeve, C ; Kristensen, VN ; Hall, P ; Pharoah, PDP ; Simard, J ; Chenevix-Trench, G ; Dunning, AM ; Antoniou, AC ; Easton, DF ; Cai, Q ; Long, J (WILEY, 2016-09-15)
    Previous genome-wide association studies among women of European ancestry identified two independent breast cancer susceptibility loci represented by single nucleotide polymorphisms (SNPs) rs13281615 and rs11780156 at 8q24. A fine-mapping study across 2.06 Mb (chr8:127,561,724-129,624,067, hg19) in 55,540 breast cancer cases and 51,168 controls within the Breast Cancer Association Consortium was conducted. Three additional independent association signals in women of European ancestry, represented by rs35961416 (OR = 0.95, 95% CI = 0.93-0.97, conditional p = 5.8 × 10(-6) ), rs7815245 (OR = 0.94, 95% CI = 0.91-0.96, conditional p = 1.1 × 10(-6) ) and rs2033101 (OR = 1.05, 95% CI = 1.02-1.07, conditional p = 1.1 × 10(-4) ) were found. Integrative analysis using functional genomic data from the Roadmap Epigenomics, the Encyclopedia of DNA Elements project, the Cancer Genome Atlas and other public resources implied that SNPs rs7815245 in Signal 3, and rs1121948 in Signal 5 (in linkage disequilibrium with rs11780156, r(2)  = 0.77), were putatively functional variants for two of the five independent association signals. The results highlighted multiple 8q24 variants associated with breast cancer susceptibility in women of European ancestry.
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    Identification of a novel prostate cancer susceptibility variant in the KLK3 gene transcript
    Kote-Jarai, Z ; Al Olama, AA ; Leongamornlert, D ; Tymrakiewicz, M ; Saunders, E ; Guy, M ; Giles, GG ; Severi, G ; Southey, M ; Hopper, JL ; Sit, KC ; Harris, JM ; Batra, J ; Spurdle, AB ; Clements, JA ; Hamdy, F ; Neal, D ; Donovan, J ; Muir, K ; Pharoah, PDP ; Chanock, SJ ; Brown, N ; Benlloch, S ; Castro, E ; Mahmud, N ; O'Brien, L ; Hall, A ; Sawyer, E ; Wilkinson, R ; Easton, DF ; Eeles, RA (SPRINGER, 2011-06)
    Genome-wide association studies (GWAS) have identified more than 30 prostate cancer (PrCa) susceptibility loci. One of these (rs2735839) is located close to a plausible candidate susceptibility gene, KLK3, which encodes prostate-specific antigen (PSA). PSA is widely used as a biomarker for PrCa detection and disease monitoring. To refine the association between PrCa and variants in this region, we used genotyping data from a two-stage GWAS using samples from the UK and Australia, and the Cancer Genetic Markers of Susceptibility (CGEMS) study. Genotypes were imputed for 197 and 312 single nucleotide polymorphisms (SNPs) from HapMap2 and the 1000 Genome Project, respectively. The most significant association with PrCa was with a previously unidentified SNP, rs17632542 (combined P = 3.9 × 10(-22)). This association was confirmed by direct genotyping in three stages of the UK/Australian GWAS, involving 10,405 cases and 10,681 controls (combined P = 1.9 × 10(-34)). rs17632542 is also shown to be associated with PSA levels and it is a non-synonymous coding SNP (Ile179Thr) in KLK3. Using molecular dynamic simulation, we showed evidence that this variant has the potential to introduce alterations in the protein or affect RNA splicing. We propose that rs17632542 may directly influence PrCa risk.
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    Large-scale genomic analyses link reproductive aging to hypothalamic signaling, breast cancer susceptibility and BRCA1-mediated DNA repair
    Day, FR ; Ruth, KS ; Thompson, DJ ; Lunetta, KL ; Pervjakova, N ; Chasman, DI ; Stolk, L ; Finucane, HK ; Sulem, P ; Bulik-Sullivan, B ; Esko, T ; Johnson, AD ; Elks, CE ; Franceschini, N ; He, C ; Altmaier, E ; Brody, JA ; Franke, LL ; Huffman, JE ; Keller, MF ; McArdle, PF ; Nutile, T ; Porcu, E ; Robino, A ; Rose, LM ; Schick, UM ; Smith, JA ; Teumer, A ; Traglia, M ; Vuckovic, D ; Yao, J ; Zhao, W ; Albrecht, E ; Amin, N ; Corre, T ; Hottenga, J-J ; Mangino, M ; Smith, AV ; Tanaka, T ; Abecasis, GR ; Andrulis, IL ; Anton-Culver, H ; Antoniou, AC ; Arndt, V ; Arnold, AM ; Barbieri, C ; Beckmann, MW ; Beeghly-Fadiel, A ; Benitez, J ; Bernstein, L ; Bielinski, SJ ; Blomqvist, C ; Boerwinkle, E ; Bogdanova, NV ; Bojesen, SE ; Bolla, MK ; Borresen-Dale, A-L ; Boutin, TS ; Brauch, H ; Brenner, H ; Bruening, T ; Burwinkel, B ; Campbell, A ; Campbell, H ; Chanock, SJ ; Chapman, JR ; Chen, Y-DI ; Chenevix-Trench, G ; Couch, FJ ; Coviello, AD ; Cox, A ; Czene, K ; Darabi, H ; De Vivo, I ; Demerath, EW ; Dennis, J ; Devilee, P ; Doerk, T ; dos-Santos-Silva, I ; Dunning, AM ; Eicher, JD ; Fasching, PA ; Faul, JD ; Figueroa, J ; Flesch-Janys, D ; Gandin, I ; Garcia, ME ; Garcia-Closas, M ; Giles, GG ; Girotto, GG ; Goldberg, MS ; Gonzalez-Neira, A ; Goodarzi, MO ; Grove, ML ; Gudbjartsson, DF ; Guenel, P ; Guo, X ; Haiman, CA ; Hall, P ; Hamann, U ; Henderson, BE ; Hocking, LJ ; Hofman, A ; Homuth, G ; Hooning, MJ ; Hopper, JL ; Hu, FB ; Huang, J ; Humphreys, K ; Hunter, DJ ; Jakubowska, A ; Jones, SE ; Kabisch, M ; Karasik, D ; Knight, JA ; Kolcic, I ; Kooperberg, C ; Kosma, V-M ; Kriebel, J ; Kristensen, V ; Lambrechts, D ; Langenberg, C ; Li, J ; Li, X ; Lindstroem, S ; Liu, Y ; Luan, J ; Lubinski, J ; Maegi, R ; Mannermaa, A ; Manz, J ; Margolin, S ; Marten, J ; Martin, NG ; Masciullo, C ; Meindl, A ; Michailidou, K ; Mihailov, E ; Milani, L ; Milne, RL ; Mueller-Nurasyid, M ; Nalls, M ; Neale, BM ; Nevanlinna, H ; Neven, P ; Newman, AB ; Nordestgaard, BG ; Olson, JE ; Padmanabhan, S ; Peterlongo, P ; Peters, U ; Petersmann, A ; Peto, J ; Pharoah, PDP ; Pirastu, NN ; Pirie, A ; Pistis, G ; Polasek, O ; Porteous, D ; Psaty, BM ; Pylkas, K ; Radice, P ; Raffel, LJ ; Rivadeneira, F ; Rudan, I ; Rudolph, A ; Ruggiero, D ; Sala, CF ; Sanna, S ; Sawyer, EJ ; Schlessinger, D ; Schmidt, MK ; Schmidt, F ; Schmutzler, RK ; Schoemaker, MJ ; Scott, RA ; Seynaeve, CM ; Simard, J ; Sorice, R ; Southey, MC ; Stoeckl, D ; Strauch, K ; Swerdlow, A ; Taylor, KD ; Thorsteinsdottir, U ; Toland, AE ; Tomlinson, I ; Truong, T ; Tryggvadottir, L ; Turner, ST ; Vozzi, D ; Wang, Q ; Wellons, M ; Willemsen, G ; Wilson, JF ; Winqvist, R ; Wolffenbuttel, BBHR ; Wright, AF ; Yannoukakos, D ; Zemunik, T ; Zheng, W ; Zygmunt, M ; Bergmann, S ; Boomsma, DI ; Buring, JE ; Ferrucci, L ; Montgomery, GW ; Gudnason, V ; Spector, TD ; van Duijn, CM ; Alizadeh, BZ ; Ciullo, M ; Crisponi, L ; Easton, DF ; Gasparini, PP ; Gieger, C ; Harris, TB ; Hayward, C ; Kardia, SLR ; Kraft, P ; McKnight, B ; Metspalu, A ; Morrison, AC ; Reiner, AP ; Ridker, PM ; Rotter, JI ; Toniolo, D ; Uitterlinden, AG ; Ulivi, S ; Voelzke, H ; Wareham, NJ ; Weir, DR ; Yerges-Armstrong, LM ; Price, AL ; Stefansson, K ; Visser, JA ; Ong, KK ; Chang-Claude, J ; Murabito, JM ; Perry, JRB ; Murray, A (NATURE PORTFOLIO, 2015-11)
    Menopause timing has a substantial impact on infertility and risk of disease, including breast cancer, but the underlying mechanisms are poorly understood. We report a dual strategy in ∼70,000 women to identify common and low-frequency protein-coding variation associated with age at natural menopause (ANM). We identified 44 regions with common variants, including two regions harboring additional rare missense alleles of large effect. We found enrichment of signals in or near genes involved in delayed puberty, highlighting the first molecular links between the onset and end of reproductive lifespan. Pathway analyses identified major association with DNA damage response (DDR) genes, including the first common coding variant in BRCA1 associated with any complex trait. Mendelian randomization analyses supported a causal effect of later ANM on breast cancer risk (∼6% increase in risk per year; P = 3 × 10(-14)), likely mediated by prolonged sex hormone exposure rather than DDR mechanisms.
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    Genome-wide significant risk associations for mucinous ovarian carcinoma
    Kelemen, LE ; Lawrenson, K ; Tyrer, J ; Li, Q ; Lee, JM ; Seo, J-H ; Phelan, CM ; Beesley, J ; Chen, X ; Spindler, TJ ; Aben, KKH ; Anton-Culver, H ; Antonenkova, N ; Baker, H ; Bandera, EV ; Bean, Y ; Beckmann, MW ; Bisogna, M ; Bjorge, L ; Bogdanova, N ; Brinton, LA ; Brooks-Wilson, A ; Bruinsma, F ; Butzow, R ; Campbell, IG ; Carty, K ; Chang-Claude, J ; Chen, YA ; Chen, Z ; Cook, LS ; Cramer, DW ; Cunningham, JM ; Cybulski, C ; Dansonka-Mieszkowska, A ; Dennis, J ; Dicks, E ; Doherty, JA ; Dicks, E ; Doherty, JA ; Doerk, T ; du Bois, A ; Duerst, M ; Eccles, D ; Easton, DT ; Edwards, RP ; Eilber, U ; Ekici, AB ; Engelholm, SA ; Fasching, PA ; Fridley, BL ; Gao, Y-T ; Gentry-Maharaj, A ; Giles, GG ; Glasspool, R ; Goode, EL ; Goodman, MT ; Grownwald, J ; Harrington, P ; Harter, P ; Hasmad, HN ; Hein, A ; Heitz, F ; Hildebrandt, MAT ; Hillemanns, P ; Hogdall, E ; Hogdall, C ; Hosono, S ; Iversen, ES ; Jakubowska, A ; Jensen, A ; Ji, B-T ; Karlan, BY ; Kellar, M ; Kelley, JL ; Kiemeney, LA ; Krakstad, C ; Kjaer, SK ; Kupryjanczyk, J ; Lambrechts, D ; Lambrechts, S ; Le, ND ; Lee, AW ; Lele, S ; Leminen, A ; Lester, J ; Levine, DA ; Liang, D ; Lissowska, J ; Lu, K ; Lubinski, J ; Lundvall, L ; Massuger, LFAG ; Matsuo, K ; McGuire, V ; McLaughlin, JR ; McNeish, I ; Menon, U ; Modugno, F ; Moes-Sosnowska, J ; Moysich, KB ; Narod, SA ; Nedergaard, L ; Ness, RB ; Nevanlinna, H ; Adenan, NAM ; Odunsi, K ; Olson, SH ; Orlow, I ; Orsulic, S ; Weber, RP ; Paul, J ; Pearce, CL ; Pejovic, T ; Pelttari, LM ; Permuth-Wey, J ; Pike, MC ; Poole, EM ; Ramus, SJ ; Risch, HA ; Rosen, B ; Rossing, MA ; Rothstein, JH ; Rudolph, A ; Runnebaum, IB ; Rzepecka, IK ; Salvesen, HB ; Schildkraut, JM ; Schwaab, I ; Shu, X-O ; Shvetsov, YB ; Siddiqui, N ; Sieh, W ; Song, H ; Southey, MC ; Sucheston, L ; Tangen, IL ; Teo, S-H ; Terry, KL ; Thompson, PJ ; Tworoger, SS ; van Altena, AM ; Van Nieuwenhuysen, E ; Vergote, I ; Vierkant, RA ; Wang-Gohrke, S ; Walsh, C ; Wentzensen, N ; Whittemore, AS ; Wicklund, KG ; Wilkens, LR ; Sawicki, W ; Woo, Y-L ; Wu, X ; Wu, AH ; Yang, H ; Zheng, W ; Ziogas, A ; Sellers, TA ; Freedman, ML ; Chenevix-Trench, G ; Pharoah, PDP ; Gayther, SA ; Berchuck, A (NATURE PUBLISHING GROUP, 2015-08)
    Genome-wide association studies have identified several risk associations for ovarian carcinomas but not for mucinous ovarian carcinomas (MOCs). Our analysis of 1,644 MOC cases and 21,693 controls with imputation identified 3 new risk associations: rs752590 at 2q13 (P = 3.3 × 10(-8)), rs711830 at 2q31.1 (P = 7.5 × 10(-12)) and rs688187 at 19q13.2 (P = 6.8 × 10(-13)). We identified significant expression quantitative trait locus (eQTL) associations for HOXD9 at 2q31.1 in ovarian (P = 4.95 × 10(-4), false discovery rate (FDR) = 0.003) and colorectal (P = 0.01, FDR = 0.09) tumors and for PAX8 at 2q13 in colorectal tumors (P = 0.03, FDR = 0.09). Chromosome conformation capture analysis identified interactions between the HOXD9 promoter and risk-associated SNPs at 2q31.1. Overexpressing HOXD9 in MOC cells augmented the neoplastic phenotype. These findings provide the first evidence for MOC susceptibility variants and insights into the underlying biology of the disease.
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    Identification of six new susceptibility loci for invasive epithelial ovarian cancer
    Kuchenbaecker, KB ; Ramus, SJ ; Tyrer, J ; Lee, A ; Shen, HC ; Beesley, J ; Lawrenson, K ; McGuffog, L ; Healey, S ; Lee, JM ; Spindler, TJ ; Lin, YG ; Pejovic, T ; Bean, Y ; Li, Q ; Coetzee, S ; Hazelett, D ; Miron, A ; Southey, M ; Terry, MB ; Goldgar, DE ; Buys, SS ; Janavicius, R ; Dorfling, CM ; van Rensburg, EJ ; Neuhausen, SL ; Ding, YC ; Hansen, TVO ; Jonson, L ; Gerdes, A-M ; Ejlertsen, B ; Barrowdale, D ; Dennis, J ; Benitez, J ; Osorio, A ; Garcia, MJ ; Komenaka, I ; Weitzel, JN ; Ganschow, P ; Peterlongo, P ; Bernard, L ; Viel, A ; Bonanni, B ; Peissel, B ; Manoukian, S ; Radice, P ; Papi, L ; Ottini, L ; Fostira, F ; Konstantopoulou, I ; Garber, J ; Frost, D ; Perkins, J ; Platte, R ; Ellis, S ; Godwin, AK ; Schmutzler, RK ; Meindl, A ; Engel, C ; Sutter, C ; Sinilnikova, OM ; Damiola, F ; Mazoyer, S ; Stoppa-Lyonnet, D ; Claes, K ; De Leeneer, K ; Kirk, J ; Rodriguez, GC ; Piedmonte, M ; O'Malley, DM ; de la Hoya, M ; Caldes, T ; Aittomaeki, K ; Nevanlinna, H ; Collee, JM ; Rookus, MA ; Oosterwijk, JC ; Tihomirova, L ; Tung, N ; Hamann, U ; Isaccs, C ; Tischkowitz, M ; Imyanitov, EN ; Caligo, MA ; Campbell, IG ; Hogervorst, FBL ; Olah, E ; Diez, O ; Blanco, I ; Brunet, J ; Lazaroso, C ; Angel Pujana, M ; Jakubowska, A ; Gronwald, J ; Lubinski, J ; Sukiennicki, G ; Barkardottir, RB ; Plante, M ; Simard, J ; Soucy, P ; Montagna, M ; Tognazzo, S ; Teixeira, MR ; Pankratz, VS ; Wang, X ; Lindor, N ; Szabo, CI ; Kauff, N ; Vijai, J ; Aghajanian, CA ; Pfeiler, G ; Berger, A ; Singer, CF ; Tea, M-K ; Phelan, CM ; Greene, MH ; Mai, PL ; Rennert, G ; Mulligan, AM ; Tchatchou, S ; Andrulis, IL ; Glendon, G ; Toland, AE ; Jensen, UB ; Kruse, TA ; Thomassen, M ; Bojesen, A ; Zidan, J ; Friedman, E ; Laitman, Y ; Soller, M ; Liljegren, A ; Arver, B ; Einbeigi, Z ; Stenmark-Askmalm, M ; Olopade, OI ; Nussbaum, RL ; Rebbeck, TR ; Nathanson, KL ; Domchek, SM ; Lu, KH ; Karlan, BY ; Walsh, C ; Lester, J ; Hein, A ; Ekici, AB ; Beckmann, MW ; Fasching, PA ; Lambrechts, D ; Van Nieuwenhuysen, E ; Vergote, I ; Lambrechts, S ; Dicks, E ; Doherty, JA ; Wicklund, KG ; Rossing, MA ; Rudolph, A ; Chang-Claude, J ; Wang-Gohrke, S ; Eilber, U ; Moysich, KB ; Odunsi, K ; Sucheston, L ; Lele, S ; Wilkens, LR ; Goodman, MT ; Thompson, PJ ; Shvetsov, YB ; Runnebaum, IB ; Duerst, M ; Hillemanns, P ; Doerk, T ; Antonenkova, N ; Bogdanova, N ; Leminen, A ; Pelttari, LM ; Butzow, R ; Modugno, F ; Kelley, JL ; Edwards, RP ; Ness, RB ; du Bois, A ; Heitz, F ; Schwaab, I ; Harter, P ; Matsuo, K ; Hosono, S ; Orsulic, S ; Jensen, A ; Kjaer, SK ; Hogdall, E ; Hasmad, HN ; Azmi, MAN ; Teo, S-H ; Woo, Y-L ; Fridley, BL ; Goode, EL ; Cunningham, JM ; Vierkant, RA ; Bruinsma, F ; Giles, GG ; Liang, D ; Hildebrandt, MAT ; Wu, X ; Levine, DA ; Bisogna, M ; Berchuck, A ; Iversen, ES ; Schildkraut, JM ; Concannon, P ; Weber, RP ; Cramer, DW ; Terry, KL ; Poole, EM ; Tworoger, SS ; Bandera, EV ; Orlow, I ; Olson, SH ; Krakstad, C ; Salvesen, HB ; Tangen, IL ; Bjorge, L ; van Altena, AM ; Aben, KKH ; Kiemeney, LA ; Massuger, LFAG ; Kellar, M ; Brooks-Wilson, A ; Kelemen, LE ; Cook, LS ; Le, ND ; Cybulski, C ; Yang, H ; Lissowska, J ; Brinton, LA ; Wentzensen, N ; Hogdall, C ; Lundvall, L ; Nedergaard, L ; Baker, H ; Song, H ; Eccles, D ; McNeish, I ; Paul, J ; Carty, K ; Siddiqui, N ; Glasspool, R ; Whittemore, AS ; Rothstein, JH ; McGuire, V ; Sieh, W ; Ji, B-T ; Zheng, W ; Shu, X-O ; Gao, Y-T ; Rosen, B ; Risch, HA ; McLaughlin, JR ; Narod, SA ; Monteiro, AN ; Chen, A ; Lin, H-Y ; Permuth-Wey, J ; Sellers, TA ; Tsai, Y-Y ; Chen, Z ; Ziogas, A ; Anton-Culver, H ; Gentry-Maharaj, A ; Menon, U ; Harrington, P ; Lee, AW ; Wu, AH ; Pearce, CL ; Coetzee, G ; Pike, MC ; Dansonka-Mieszkowska, A ; Timorek, A ; Rzepecka, IK ; Kupryjanczyk, J ; Freedman, M ; Noushmehr, H ; Easton, DF ; Offit, K ; Couch, FJ ; Gayther, S ; Pharoah, PP ; Antoniou, AC ; Chenevix-Trench, G (NATURE PORTFOLIO, 2015-02)
    Genome-wide association studies (GWAS) have identified 12 epithelial ovarian cancer (EOC) susceptibility alleles. The pattern of association at these loci is consistent in BRCA1 and BRCA2 mutation carriers who are at high risk of EOC. After imputation to 1000 Genomes Project data, we assessed associations of 11 million genetic variants with EOC risk from 15,437 cases unselected for family history and 30,845 controls and from 15,252 BRCA1 mutation carriers and 8,211 BRCA2 mutation carriers (3,096 with ovarian cancer), and we combined the results in a meta-analysis. This new study design yielded increased statistical power, leading to the discovery of six new EOC susceptibility loci. Variants at 1p36 (nearest gene, WNT4), 4q26 (SYNPO2), 9q34.2 (ABO) and 17q11.2 (ATAD5) were associated with EOC risk, and at 1p34.3 (RSPO1) and 6p22.1 (GPX6) variants were specifically associated with the serous EOC subtype, all with P < 5 × 10(-8). Incorporating these variants into risk assessment tools will improve clinical risk predictions for BRCA1 and BRCA2 mutation carriers.
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    Candidate locus analysis of the TERT-CLPTM1L cancer risk region on chromosome 5p15 identifies multiple independent variants associated with endometrial cancer risk
    Carvajal-Carmona, LG ; O'Mara, TA ; Painter, JN ; Lose, FA ; Dennis, J ; Michailidou, K ; Tyrer, JP ; Ahmed, S ; Ferguson, K ; Healey, CS ; Pooley, K ; Beesley, J ; Cheng, T ; Jones, A ; Howarth, K ; Martin, L ; Gorman, M ; Hodgson, S ; Wentzensen, N ; Fasching, PA ; Hein, A ; Beckmann, MW ; Renner, SP ; Doerk, T ; Hillemanns, P ; Duerst, M ; Runnebaum, I ; Lambrechts, D ; Coenegrachts, L ; Schrauwen, S ; Amant, F ; Winterhoff, B ; Dowdy, SC ; Goode, EL ; Teoman, A ; Salvesen, HB ; Trovik, J ; Njolstad, TS ; Werner, HMJ ; Scott, RJ ; Ashton, K ; Proietto, T ; Otton, G ; Wersaell, O ; Mints, M ; Tham, E ; Hall, P ; Czene, K ; Liu, J ; Li, J ; Hopper, JL ; Southey, MC ; Ekici, AB ; Ruebner, M ; Johnson, N ; Peto, J ; Burwinkel, B ; Marme, F ; Brenner, H ; Dieffenbach, AK ; Meindl, A ; Brauch, H ; Lindblom, A ; Depreeuw, J ; Moisse, M ; Chang-Claude, J ; Rudolph, A ; Couch, FJ ; Olson, JE ; Giles, GG ; Bruinsma, F ; Cunningham, JM ; Fridley, BL ; Borresen-Dale, A-L ; Kristensen, VN ; Cox, A ; Swerdlow, AJ ; Orr, N ; Bolla, MK ; Wang, Q ; Weber, RP ; Chen, Z ; Shah, M ; Pharoah, PDP ; Dunning, AM ; Tomlinson, I ; Easton, DF ; Spurdle, AB ; Thompson, DJ (SPRINGER, 2015-02)
    Several studies have reported associations between multiple cancer types and single-nucleotide polymorphisms (SNPs) on chromosome 5p15, which harbours TERT and CLPTM1L, but no such association has been reported with endometrial cancer. To evaluate the role of genetic variants at the TERT-CLPTM1L region in endometrial cancer risk, we carried out comprehensive fine-mapping analyses of genotyped and imputed SNPs using a custom Illumina iSelect array which includes dense SNP coverage of this region. We examined 396 SNPs (113 genotyped, 283 imputed) in 4,401 endometrial cancer cases and 28,758 controls. Single-SNP and forward/backward logistic regression models suggested evidence for three variants independently associated with endometrial cancer risk (P = 4.9 × 10(-6) to P = 7.7 × 10(-5)). Only one falls into a haplotype previously associated with other cancer types (rs7705526, in TERT intron 1), and this SNP has been shown to alter TERT promoter activity. One of the novel associations (rs13174814) maps to a second region in the TERT promoter and the other (rs62329728) is in the promoter region of CLPTM1L; neither are correlated with previously reported cancer-associated SNPs. Using TCGA RNASeq data, we found significantly increased expression of both TERT and CLPTM1L in endometrial cancer tissue compared with normal tissue (TERT P = 1.5 × 10(-18), CLPTM1L P = 1.5 × 10(-19)). Our study thus reports a novel endometrial cancer risk locus and expands the spectrum of cancer types associated with genetic variation at 5p15, further highlighting the importance of this region for cancer susceptibility.
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    Genome-wide association study identifies multiple loci associated with both mammographic density and breast cancer risk
    Lindstroem, S ; Thompson, DJ ; Paterson, AD ; Li, J ; Gierach, GL ; Scott, C ; Stone, J ; Douglas, JA ; dos-Santos-Silva, I ; Fernandez-Navarro, P ; Verghase, J ; Smith, P ; Brown, J ; Luben, R ; Wareham, NJ ; Loos, RJF ; Heit, JA ; Pankratz, VS ; Norman, A ; Goode, EL ; Cunningham, JM ; Deandrade, M ; Vierkant, RA ; Czene, K ; Fasching, PA ; Baglietto, L ; Southey, MC ; Giles, GG ; Shah, KP ; Chan, H-P ; Helvie, MA ; Beck, AH ; Knoblauch, NW ; Hazra, A ; Hunter, DJ ; Kraft, P ; Pollan, M ; Figueroa, JD ; Couch, FJ ; Hopper, JL ; Hall, P ; Easton, DF ; Boyd, NF ; Vachon, CM ; Tamimi, RM (NATURE PORTFOLIO, 2014-10)
    Mammographic density reflects the amount of stromal and epithelial tissues in relation to adipose tissue in the breast and is a strong risk factor for breast cancer. Here we report the results from meta-analysis of genome-wide association studies (GWAS) of three mammographic density phenotypes: dense area, non-dense area and percent density in up to 7,916 women in stage 1 and an additional 10,379 women in stage 2. We identify genome-wide significant (P<5 × 10(-8)) loci for dense area (AREG, ESR1, ZNF365, LSP1/TNNT3, IGF1, TMEM184B and SGSM3/MKL1), non-dense area (8p11.23) and percent density (PRDM6, 8p11.23 and TMEM184B). Four of these regions are known breast cancer susceptibility loci, and four additional regions were found to be associated with breast cancer (P<0.05) in a large meta-analysis. These results provide further evidence of a shared genetic basis between mammographic density and breast cancer and illustrate the power of studying intermediate quantitative phenotypes to identify putative disease-susceptibility loci.
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    Genome-wide association study identifies multiple susceptibility loci for diffuse large B cell lymphoma
    Cerhan, JR ; Berndt, SI ; Vijai, J ; Ghesquieres, H ; McKay, J ; Wang, SS ; Wang, Z ; Yeager, M ; Conde, L ; de Bakker, PIW ; Nieters, A ; Cox, D ; Burdett, L ; Monnereau, A ; Flowers, CR ; De Roos, AJ ; Brooks-Wilson, AR ; Lan, Q ; Severi, G ; Melbye, M ; Gu, J ; Jackson, RD ; Kane, E ; Teras, LR ; Purdue, MP ; Vajdic, CM ; Spinelli, JJ ; Giles, GG ; Albanes, D ; Kelly, RS ; Zucca, M ; Bertrand, KA ; Zeleniuch-Jacquotte, A ; Lawrence, C ; Hutchinson, A ; Zhi, D ; Habermann, TM ; Link, BK ; Novak, AJ ; Dogan, A ; Asmann, YW ; Liebow, M ; Thompson, CA ; Ansell, SM ; Witzig, TE ; Weiner, GJ ; Veron, AS ; Zelenika, D ; Tilly, H ; Haioun, C ; Molina, TJ ; Hjalgrim, H ; Glimelius, B ; Adami, H-O ; Bracci, PM ; Riby, J ; Smith, MT ; Holly, EA ; Cozen, W ; Hartge, P ; Morton, LM ; Severson, RK ; Tinker, LF ; North, KE ; Becker, N ; Benavente, Y ; Boffetta, P ; Brennan, P ; Foretova, L ; Maynadie, M ; Staines, A ; Lightfoot, T ; Crouch, S ; Smith, A ; Roman, E ; Diver, WR ; Offit, K ; Zelenetz, A ; Klein, RJ ; Villano, DJ ; Zheng, T ; Zhang, Y ; Holford, TR ; Kricker, A ; Turner, J ; Southey, MC ; Clavel, J ; Virtamo, J ; Weinstein, S ; Riboli, E ; Vineis, P ; Kaaks, R ; Trichopoulos, D ; Vermeulen, RCH ; Boeing, H ; Tjonneland, A ; Angelucci, E ; Di Lollo, S ; Rais, M ; Birmann, BM ; Laden, F ; Giovannucci, E ; Kraft, P ; Huang, J ; Ma, B ; Ye, Y ; Chiu, BCH ; Sampson, J ; Liang, L ; Park, J-H ; Chung, CC ; Weisenburger, DD ; Chatterjee, N ; Fraumeni, JF ; Slager, SL ; Wu, X ; de Sanjose, S ; Smedby, KE ; Salles, G ; Skibola, CF ; Rothman, N ; Chanock, SJ (NATURE PUBLISHING GROUP, 2014-11)
    Diffuse large B cell lymphoma (DLBCL) is the most common lymphoma subtype and is clinically aggressive. To identify genetic susceptibility loci for DLBCL, we conducted a meta-analysis of 3 new genome-wide association studies (GWAS) and 1 previous scan, totaling 3,857 cases and 7,666 controls of European ancestry, with additional genotyping of 9 promising SNPs in 1,359 cases and 4,557 controls. In our multi-stage analysis, five independent SNPs in four loci achieved genome-wide significance marked by rs116446171 at 6p25.3 (EXOC2; P = 2.33 × 10(-21)), rs2523607 at 6p21.33 (HLA-B; P = 2.40 × 10(-10)), rs79480871 at 2p23.3 (NCOA1; P = 4.23 × 10(-8)) and two independent SNPs, rs13255292 and rs4733601, at 8q24.21 (PVT1; P = 9.98 × 10(-13) and 3.63 × 10(-11), respectively). These data provide substantial new evidence for genetic susceptibility to this B cell malignancy and point to pathways involved in immune recognition and immune function in the pathogenesis of DLBCL.