Sir Peter MacCallum Department of Oncology - Research Publications

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Start date: 2010 × End date: 2019 × Author: Southey, Melissa × Author: Milne, Roger ×

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    Benign breast disease increases breast cancer risk independent of underlying familial risk profile: Findings from a Prospective Family Study Cohort
    Zeinomar, N ; Phillips, K-A ; Daly, MB ; Milne, RL ; Dite, GS ; MacInnis, RJ ; Liao, Y ; Kehm, RD ; Knight, JA ; Southey, MC ; Chung, WK ; Giles, GG ; McLachlan, S-A ; Friedlander, ML ; Weideman, PC ; Glendon, G ; Nesci, S ; Andrulis, IL ; Buys, SS ; John, EM ; Hopper, JL ; Terry, MB (WILEY, 2019-07-15)
    Benign breast disease (BBD) is an established breast cancer (BC) risk factor, but it is unclear whether the magnitude of the association applies to women at familial or genetic risk. This information is needed to improve BC risk assessment in clinical settings. Using the Prospective Family Study Cohort, we used Cox proportional hazards models to estimate hazard ratios (HRs) and 95% confidence intervals (CIs) for the association of BBD with BC risk. We also examined whether the association with BBD differed by underlying familial risk profile (FRP), calculated using absolute risk estimates from the Breast Ovarian Analysis of Disease Incidence and Carrier Estimation Algorithm (BOADICEA) model. During 176,756 person-years of follow-up (median: 10.9 years, maximum: 23.7) of 17,154 women unaffected with BC at baseline, we observed 968 incident cases of BC. A total of 4,704 (27%) women reported a history of BBD diagnosis at baseline. A history of BBD was associated with a greater risk of BC: HR = 1.31 (95% CI: 1.14-1.50), and did not differ by underlying FRP, with HRs of 1.35 (95% CI: 1.11-1.65), 1.26 (95% CI: 1.00-1.60), and 1.40 (95% CI: 1.01-1.93), for categories of full-lifetime BOADICEA score <20%, 20 to <35%, ≥35%, respectively. There was no difference in the association for women with BRCA1 mutations (HR: 1.64; 95% CI: 1.04-2.58), women with BRCA2 mutations (HR: 1.34; 95% CI: 0.78-2.3) or for women without a known BRCA1 or BRCA2 mutation (HR: 1.31; 95% CI: 1.13-1.53) (pinteraction  = 0.95). Women with a history of BBD have an increased risk of BC that is independent of, and multiplies, their underlying familial and genetic risk.
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    Body mass index and breast cancer survival: a Mendelian randomization analysis
    Guo, Q ; Burgess, S ; Turman, C ; Bolla, MK ; Wang, Q ; Lush, M ; Abraham, J ; Aittomaki, K ; Andrulis, IL ; Apicella, C ; Arndt, V ; Barrdahl, M ; Benitez, J ; Berg, CD ; Blomqvist, C ; Bojesen, SE ; Bonanni, B ; Brand, JS ; Brenner, H ; Broeks, A ; Burwinkel, B ; Caldas, C ; Campa, D ; Canzian, F ; Chang-Claude, J ; Chanock, SJ ; Chin, S-F ; Couch, FJ ; Cox, A ; Cross, SS ; Cybulski, C ; Czene, K ; Darabi, H ; Devilee, P ; Diver, WR ; Dunning, AM ; Earl, HM ; Eccles, DM ; Ekici, AB ; Eriksson, M ; Evans, DG ; Fasching, PA ; Figueroa, J ; Flesch-Janys, D ; Flyger, H ; Gapstur, SM ; Gaudet, MM ; Giles, GG ; Glendon, G ; Grip, M ; Gronwald, J ; Haeberle, L ; Haiman, CA ; Hall, P ; Hamann, U ; Hankinson, S ; Hartikainen, JM ; Hein, A ; Hiller, L ; Hogervorst, FB ; Holleczek, B ; Hooning, MJ ; Hoover, RN ; Humphreys, K ; Hunter, DJ ; Husing, A ; Jakubowska, A ; Jukkola-Vuorinen, A ; Kaaks, R ; Kabisch, M ; Kataja, V ; Knight, JA ; Koppert, LB ; Kosma, V-M ; Kristensen, VN ; Lambrechts, D ; Le Marchand, L ; Li, J ; Lindblom, A ; Lindstrom, S ; Lissowska, J ; Lubinski, J ; Machiela, MJ ; Mannermaa, A ; Manoukian, S ; Margolin, S ; Marme, F ; Martens, JWM ; McLean, C ; Menendez, P ; Milne, RL ; Mulligan, AM ; Muranen, TA ; Nevanlinna, H ; Neven, P ; Nielsen, SF ; Nordestgaard, BG ; Olson, JE ; Perez, JIA ; Peterlongo, P ; Phillips, K-A ; Poole, CJ ; Pylkas, K ; Radice, P ; Rahman, N ; Rudiger, T ; Rudolph, A ; Sawyer, EJ ; Schumacher, F ; Seibold, P ; Seynaeve, C ; Shah, M ; Smeets, A ; Southey, MC ; Tollenaar, RAEM ; Tomlinson, I ; Tsimiklis, H ; Ulmer, H-U ; Vachon, C ; van den Ouweland, AMW ; Van't Veer, LJ ; Wildiers, H ; Willett, W ; Winqvist, R ; Zamora, MP ; Chenevix-Trench, G ; Dork, T ; Easton, DF ; Garcia-Closas, M ; Kraft, P ; Hopper, JL ; Zheng, W ; Schmidt, MK ; Pharoah, PDP (OXFORD UNIV PRESS, 2017-12)
    BACKGROUND: There is increasing evidence that elevated body mass index (BMI) is associated with reduced survival for women with breast cancer. However, the underlying reasons remain unclear. We conducted a Mendelian randomization analysis to investigate a possible causal role of BMI in survival from breast cancer. METHODS: We used individual-level data from six large breast cancer case-cohorts including a total of 36 210 individuals (2475 events) of European ancestry. We created a BMI genetic risk score (GRS) based on genotypes at 94 known BMI-associated genetic variants. Association between the BMI genetic score and breast cancer survival was analysed by Cox regression for each study separately. Study-specific hazard ratios were pooled using fixed-effect meta-analysis. RESULTS: BMI genetic score was found to be associated with reduced breast cancer-specific survival for estrogen receptor (ER)-positive cases [hazard ratio (HR) = 1.11, per one-unit increment of GRS, 95% confidence interval (CI) 1.01-1.22, P = 0.03). We observed no association for ER-negative cases (HR = 1.00, per one-unit increment of GRS, 95% CI 0.89-1.13, P = 0.95). CONCLUSIONS: Our findings suggest a causal effect of increased BMI on reduced breast cancer survival for ER-positive breast cancer. There is no evidence of a causal effect of higher BMI on survival for ER-negative breast cancer cases.
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    Common Genetic Variation in Circadian Rhythm Genes and Risk of Epithelial Ovarian Cancer (EOC).
    Jim, HSL ; Lin, H-Y ; Tyrer, JP ; Lawrenson, K ; Dennis, J ; Chornokur, G ; Chen, Z ; Chen, AY ; Permuth-Wey, J ; Aben, KK ; Anton-Culver, H ; Antonenkova, N ; Bruinsma, F ; Bandera, EV ; Bean, YT ; Beckmann, MW ; Bisogna, M ; Bjorge, L ; Bogdanova, N ; Brinton, LA ; Brooks-Wilson, A ; Bunker, CH ; Butzow, R ; Campbell, IG ; Carty, K ; Chang-Claude, J ; Cook, LS ; Cramer, DW ; Cunningham, JM ; Cybulski, C ; Dansonka-Mieszkowska, A ; du Bois, A ; Despierre, E ; Sieh, W ; Doherty, JA ; Dörk, T ; Dürst, M ; Easton, DF ; Eccles, DM ; Edwards, RP ; Ekici, AB ; Fasching, PA ; Fridley, BL ; Gao, Y-T ; Gentry-Maharaj, A ; Giles, GG ; Glasspool, R ; Goodman, MT ; Gronwald, J ; Harter, P ; Hasmad, HN ; Hein, A ; Heitz, F ; Hildebrandt, MAT ; Hillemanns, P ; Hogdall, CK ; Hogdall, E ; Hosono, S ; Iversen, ES ; Jakubowska, A ; Jensen, A ; Ji, B-T ; Karlan, BY ; Kellar, M ; Kiemeney, LA ; Krakstad, C ; Kjaer, SK ; Kupryjanczyk, J ; Vierkant, RA ; Lambrechts, D ; Lambrechts, S ; Le, ND ; Lee, AW ; Lele, S ; Leminen, A ; Lester, J ; Levine, DA ; Liang, D ; Lim, BK ; Lissowska, J ; Lu, K ; Lubinski, J ; Lundvall, L ; Massuger, LFAG ; Matsuo, K ; McGuire, V ; McLaughlin, JR ; McNeish, I ; Menon, U ; Milne, RL ; Modugno, F ; Thomsen, L ; Moysich, KB ; Ness, RB ; Nevanlinna, H ; Eilber, U ; Odunsi, K ; Olson, SH ; Orlow, I ; Orsulic, S ; Palmieri Weber, R ; Paul, J ; Pearce, CL ; Pejovic, T ; Pelttari, LM ; Pike, MC ; Poole, EM ; Schernhammer, E ; Risch, HA ; Rosen, B ; Rossing, MA ; Rothstein, JH ; Rudolph, A ; Runnebaum, IB ; Rzepecka, IK ; Salvesen, HB ; Schwaab, I ; Shu, X-O ; Shvetsov, YB ; Siddiqui, N ; Song, H ; Southey, MC ; Spiewankiewicz, B ; Sucheston-Campbell, L ; Teo, S-H ; Terry, KL ; Thompson, PJ ; Tangen, IL ; Tworoger, SS ; van Altena, AM ; Vergote, I ; Walsh, CS ; Wang-Gohrke, S ; Wentzensen, N ; Whittemore, AS ; Wicklund, KG ; Wilkens, LR ; Wu, AH ; Wu, X ; Woo, Y-L ; Yang, H ; Zheng, W ; Ziogas, A ; Amankwah, E ; Berchuck, A ; Georgia Chenevix-Trench on behalf of the AOCS management group 95,96, ; Schildkraut, JM ; Kelemen, LE ; Ramus, SJ ; Monteiro, ANA ; Goode, EL ; Narod, SA ; Gayther, SA ; Pharoah, PDP ; Sellers, TA ; Phelan, CM (ClinMed International Library, 2015)
    Disruption in circadian gene expression, whether due to genetic variation or environmental factors (e.g., light at night, shiftwork), is associated with increased incidence of breast, prostate, gastrointestinal and hematologic cancers and gliomas. Circadian genes are highly expressed in the ovaries where they regulate ovulation; circadian disruption is associated with several ovarian cancer risk factors (e.g., endometriosis). However, no studies have examined variation in germline circadian genes as predictors of ovarian cancer risk and invasiveness. The goal of the current study was to examine single nucleotide polymorphisms (SNPs) in circadian genes BMAL1, CRY2, CSNK1E, NPAS2, PER3, REV1 and TIMELESS and downstream transcription factors KLF10 and SENP3 as predictors of risk of epithelial ovarian cancer (EOC) and histopathologic subtypes. The study included a test set of 3,761 EOC cases and 2,722 controls and a validation set of 44,308 samples including 18,174 (10,316 serous) cases and 26,134 controls from 43 studies participating in the Ovarian Cancer Association Consortium (OCAC). Analysis of genotype data from 36 genotyped SNPs and 4600 imputed SNPs indicated that the most significant association was rs117104877 in BMAL1 (OR = 0.79, 95% CI = 0.68-0.90, p = 5.59 × 10-4]. Functional analysis revealed a significant down regulation of BMAL1 expression following cMYC overexpression and increasing transformation in ovarian surface epithelial (OSE) cells as well as alternative splicing of BMAL1 exons in ovarian and granulosa cells. These results suggest that variation in circadian genes, and specifically BMAL1, may be associated with risk of ovarian cancer, likely through disruption of hormonal pathways.
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    Common germline polymorphisms associated with breast cancer-specific survival
    Pirie, A ; Guo, Q ; Kraft, P ; Canisius, S ; Eccles, DM ; Rahman, N ; Nevanlinna, H ; Chen, C ; Khan, S ; Tyrer, J ; Bolla, MK ; Wang, Q ; Dennis, J ; Michailidou, K ; Lush, M ; Dunning, AM ; Shah, M ; Czene, K ; Darabi, H ; Eriksson, M ; Lambrechts, D ; Weltens, C ; Leunen, K ; van Ongeval, C ; Nordestgaard, BG ; Nielsen, SF ; Flyger, H ; Rudolph, A ; Seibold, P ; Flesch-Janys, D ; Blomqvist, C ; Aittomaki, K ; Fagerholm, R ; Muranen, TA ; Olsen, JE ; Hallberg, E ; Vachon, C ; Knight, JA ; Glendon, G ; Mulligan, AM ; Broeks, A ; Cornelissen, S ; Haiman, CA ; Henderson, BE ; Schumacher, F ; Le Marchand, L ; Hopper, JL ; Tsimiklis, H ; Apicella, C ; Southey, MC ; Cross, SS ; Reed, MWR ; Giles, GG ; Milne, RL ; McLean, C ; Winqvist, R ; Pylkas, K ; Jukkola-Vuorinen, A ; Grip, M ; Hooning, MJ ; Hollestelle, A ; Martens, JWM ; van den Ouweland, AMW ; Marme, F ; Schneeweiss, A ; Yang, R ; Burwinkel, B ; Figueroa, J ; Chanock, SJ ; Lissowska, J ; Sawyer, EJ ; Tomlinson, I ; Kerin, MJ ; Miller, N ; Brenner, H ; Butterbach, K ; Holleczek, B ; Kataja, V ; Kosma, V-M ; Hartikainen, JM ; Li, J ; Brand, JS ; Humphreys, K ; Devilee, P ; Tollenaar, RAEM ; Seynaeve, C ; Radice, P ; Peterlongo, P ; Manoukian, S ; Ficarazzi, F ; Beckmann, MW ; Hein, A ; Ekici, AB ; Balleine, R ; Phillips, K-A ; Benitez, J ; Zamora, MP ; Perez, JIA ; Menendez, P ; Jakubowska, A ; Lubinski, J ; Gronwald, J ; Durda, K ; Hamann, U ; Kabisch, M ; Ulmer, HU ; Ruediger, T ; Margolin, S ; Kristensen, V ; Nord, S ; Evans, DG ; Abraham, J ; Earl, H ; Poole, CJ ; Hiller, L ; Dunn, JA ; Bowden, S ; Yang, R ; Campa, D ; Diver, WR ; Gapstur, SM ; Gaudet, MM ; Hankinson, S ; Hoover, RN ; Husing, A ; Kaaks, R ; Machiela, MJ ; Willett, W ; Barrdahl, M ; Canzian, F ; Chin, S-F ; Caldas, C ; Hunter, DJ ; Lindstrom, S ; Garcia-Closas, M ; Couch, FJ ; Chenevix-Trench, G ; Mannermaa, A ; Andrulis, IL ; Hall, P ; Chang-Claude, J ; Easton, DF ; Bojesen, SE ; Cox, A ; Fasching, PA ; Pharoah, PDP ; Schmidt, MK (BMC, 2015-04-22)
    INTRODUCTION: Previous studies have identified common germline variants nominally associated with breast cancer survival. These associations have not been widely replicated in further studies. The purpose of this study was to evaluate the association of previously reported SNPs with breast cancer-specific survival using data from a pooled analysis of eight breast cancer survival genome-wide association studies (GWAS) from the Breast Cancer Association Consortium. METHODS: A literature review was conducted of all previously published associations between common germline variants and three survival outcomes: breast cancer-specific survival, overall survival and disease-free survival. All associations that reached the nominal significance level of P value <0.05 were included. Single nucleotide polymorphisms that had been previously reported as nominally associated with at least one survival outcome were evaluated in the pooled analysis of over 37,000 breast cancer cases for association with breast cancer-specific survival. Previous associations were evaluated using a one-sided test based on the reported direction of effect. RESULTS: Fifty-six variants from 45 previous publications were evaluated in the meta-analysis. Fifty-four of these were evaluated in the full set of 37,954 breast cancer cases with 2,900 events and the two additional variants were evaluated in a reduced sample size of 30,000 samples in order to ensure independence from the previously published studies. Five variants reached nominal significance (P <0.05) in the pooled GWAS data compared to 2.8 expected under the null hypothesis. Seven additional variants were associated (P <0.05) with ER-positive disease. CONCLUSIONS: Although no variants reached genome-wide significance (P <5 x 10(-8)), these results suggest that there is some evidence of association between candidate common germline variants and breast cancer prognosis. Larger studies from multinational collaborations are necessary to increase the power to detect associations, between common variants and prognosis, at more stringent significance levels.
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    Identification of Novel Genetic Markers of Breast Cancer Survival
    Guo, Q ; Schmidt, MK ; Kraft, P ; Canisius, S ; Chen, C ; Khan, S ; Tyrer, J ; Bolla, MK ; Wang, Q ; Dennis, J ; Michailidou, K ; Lush, M ; Kar, S ; Beesley, J ; Dunning, AM ; Shah, M ; Czene, K ; Darabi, H ; Eriksson, M ; Lambrechts, D ; Weltens, C ; Leunen, K ; Bojesen, SE ; Nordestgaard, BG ; Nielsen, SF ; Flyger, H ; Chang-Claude, J ; Rudolph, A ; Seibold, P ; Flesch-Janys, D ; Blomqvist, C ; Aittomaeki, K ; Fagerholm, R ; Muranen, TA ; Couch, FJ ; Olson, JE ; Vachon, C ; Andrulis, IL ; Knight, JA ; Glendon, G ; Mulligan, AM ; Broeks, A ; Hogervorst, FB ; Haiman, CA ; Henderson, BE ; Schumacher, F ; Le Marchand, L ; Hopper, JL ; Tsimiklis, H ; Apicella, C ; Southey, MC ; Cox, A ; Cross, SS ; Reed, MWR ; Giles, GG ; Milne, RL ; McLean, C ; Winqvist, R ; Pylkaes, K ; Jukkola-Vuorinen, A ; Grip, M ; Hooning, MJ ; Hollestelle, A ; Martens, JWM ; Van den Ouweland, AMW ; Marme, F ; Schneeweiss, A ; Yang, R ; Burwinkel, B ; Figueroa, J ; Chanock, SJ ; Lissowska, J ; Sawyer, EJ ; Tomlinson, I ; Kerin, MJ ; Miller, N ; Brenner, H ; Dieffenbach, AK ; Arndt, V ; Holleczek, B ; Mannermaa, A ; Kataja, V ; Kosma, V-M ; Hartikainen, JM ; Li, J ; Brand, JS ; Humphreys, K ; Devilee, P ; Tollenaar, RAEM ; Seynaeve, C ; Radice, P ; Peterlongo, P ; Bonanni, B ; Mariani, P ; Fasching, PA ; Beckmann, MW ; Hein, A ; Ekici, AB ; Chenevix-Trench, G ; Balleine, R ; Phillips, K-A ; Benitez, J ; Zamora, MP ; Perez, JIA ; Menendez, P ; Jakubowska, A ; Lubinski, J ; Jaworska-Bieniek, K ; Durda, K ; Hamann, U ; Kabisch, M ; Ulmer, HU ; Ruediger, T ; Margolin, S ; Kristensen, V ; Nord, S ; Evans, DG ; Abraham, JE ; Earl, HM ; Hiller, L ; Dunn, JA ; Bowden, S ; Berg, C ; Campa, D ; Diver, WR ; Gapstur, SM ; Gaudet, MM ; Hankinson, SE ; Hoover, RN ; Huesing, A ; Kaaks, R ; Machiela, MJ ; Willett, W ; Barrdahl, M ; Canzian, F ; Chin, S-F ; Caldas, C ; Hunter, DJ ; Lindstrom, S ; Garcia-Closas, M ; Hall, P ; Easton, DF ; Eccles, DM ; Rahman, N ; Nevanlinna, H ; Pharoah, PDP (OXFORD UNIV PRESS INC, 2015-05)
    BACKGROUND: Survival after a diagnosis of breast cancer varies considerably between patients, and some of this variation may be because of germline genetic variation. We aimed to identify genetic markers associated with breast cancer-specific survival. METHODS: We conducted a large meta-analysis of studies in populations of European ancestry, including 37954 patients with 2900 deaths from breast cancer. Each study had been genotyped for between 200000 and 900000 single nucleotide polymorphisms (SNPs) across the genome; genotypes for nine million common variants were imputed using a common reference panel from the 1000 Genomes Project. We also carried out subtype-specific analyses based on 6881 estrogen receptor (ER)-negative patients (920 events) and 23059 ER-positive patients (1333 events). All statistical tests were two-sided. RESULTS: We identified one new locus (rs2059614 at 11q24.2) associated with survival in ER-negative breast cancer cases (hazard ratio [HR] = 1.95, 95% confidence interval [CI] = 1.55 to 2.47, P = 1.91 x 10(-8)). Genotyping a subset of 2113 case patients, of which 300 were ER negative, provided supporting evidence for the quality of the imputation. The association in this set of case patients was stronger for the observed genotypes than for the imputed genotypes. A second locus (rs148760487 at 2q24.2) was associated at genome-wide statistical significance in initial analyses; the association was similar in ER-positive and ER-negative case patients. Here the results of genotyping suggested that the finding was less robust. CONCLUSIONS: This is currently the largest study investigating genetic variation associated with breast cancer survival. Our results have potential clinical implications, as they confirm that germline genotype can provide prognostic information in addition to standard tumor prognostic factors.
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    Common Genetic Variation In Cellular Transport Genes and Epithelial Ovarian Cancer (EOC) Risk
    Chornokur, G ; Lin, H-Y ; Tyrer, JP ; Lawrenson, K ; Dennis, J ; Amankwah, EK ; Qu, X ; Tsai, Y-Y ; Jim, HSL ; Chen, Z ; Chen, AY ; Permuth-Wey, J ; Aben, KKH ; Anton-Culver, H ; Antonenkova, N ; Bruinsma, F ; Bandera, EV ; Bean, YT ; Beckmann, MW ; Bisogna, M ; Bjorge, L ; Bogdanova, N ; Brinton, LA ; Brooks-Wilson, A ; Bunker, CH ; Butzow, R ; Campbell, IG ; Carty, K ; Chang-Claude, J ; Cook, LS ; Cramer, DW ; Cunningham, JM ; Cybulski, C ; Dansonka-Mieszkowska, A ; du Bois, A ; Despierre, E ; Dicks, E ; Doherty, JA ; Dork, T ; Durst, M ; Easton, DF ; Eccles, DM ; Edwards, RP ; Ekici, AB ; Fasching, PA ; Fridley, BL ; Gao, Y-T ; Gentry-Maharaj, A ; Giles, GG ; Glasspool, R ; Goodman, MT ; Gronwald, J ; Harrington, P ; Harter, P ; Hein, A ; Heitz, F ; Hildebrandt, MAT ; Hillemanns, P ; Hogdall, CK ; Hogdall, E ; Hosono, S ; Jakubowska, A ; Jensen, A ; Ji, B-T ; Karlan, BY ; Kelemen, LE ; Kellar, M ; 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 ; Lim, BK ; Lissowska, J ; Lu, K ; Lubinski, J ; Lundvall, L ; Massuger, LFAG ; Matsuo, K ; McGuire, V ; McLaughlin, JR ; McNeish, I ; Menon, U ; Milne, RL ; Modugno, F ; Moysich, KB ; Ness, RB ; Nevanlinna, H ; Eilber, U ; Odunsi, K ; Olson, SH ; Orlow, I ; Orsulic, S ; Weber, RP ; Paul, J ; Pearce, CL ; Pejovic, T ; Pelttari, LM ; Pike, MC ; Poole, EM ; Risch, HA ; Rosen, B ; Rossing, MA ; Rothstein, JH ; Rudolph, A ; Runnebaum, IB ; Rzepecka, IK ; Salvesen, HB ; Schernhammer, E ; Schwaab, I ; Shu, X-O ; Shvetsov, YB ; Siddiqui, N ; Sieh, W ; Song, H ; Southey, MC ; Spiewankiewicz, B ; Sucheston, L ; Teo, S-H ; Terry, KL ; Thompson, PJ ; Thomsen, L ; Tangen, IL ; Tworoger, SS ; van Altena, AM ; Vierkant, RA ; Vergote, I ; Walsh, CS ; Wang-Gohrke, S ; Wentzensen, N ; Whittemore, AS ; Wicklund, KG ; Wilkens, LR ; Wu, AH ; Wu, X ; Woo, Y-L ; Yang, H ; Zheng, W ; Ziogas, A ; Hasmad, HN ; Berchuck, A ; Iversen, ES ; Schildkraut, JM ; Ramus, SJ ; Goode, EL ; Monteiro, ANA ; Gayther, SA ; Narod, SA ; Pharoah, PP ; Sellers, TA ; Phelan, CM ; Agoulnik, IU (PUBLIC LIBRARY SCIENCE, 2015-06-19)
    BACKGROUND: Defective cellular transport processes can lead to aberrant accumulation of trace elements, iron, small molecules and hormones in the cell, which in turn may promote the formation of reactive oxygen species, promoting DNA damage and aberrant expression of key regulatory cancer genes. As DNA damage and uncontrolled proliferation are hallmarks of cancer, including epithelial ovarian cancer (EOC), we hypothesized that inherited variation in the cellular transport genes contributes to EOC risk. METHODS: In total, DNA samples were obtained from 14,525 case subjects with invasive EOC and from 23,447 controls from 43 sites in the Ovarian Cancer Association Consortium (OCAC). Two hundred seventy nine SNPs, representing 131 genes, were genotyped using an Illumina Infinium iSelect BeadChip as part of the Collaborative Oncological Gene-environment Study (COGS). SNP analyses were conducted using unconditional logistic regression under a log-additive model, and the FDR q<0.2 was applied to adjust for multiple comparisons. RESULTS: The most significant evidence of an association for all invasive cancers combined and for the serous subtype was observed for SNP rs17216603 in the iron transporter gene HEPH (invasive: OR = 0.85, P = 0.00026; serous: OR = 0.81, P = 0.00020); this SNP was also associated with the borderline/low malignant potential (LMP) tumors (P = 0.021). Other genes significantly associated with EOC histological subtypes (p<0.05) included the UGT1A (endometrioid), SLC25A45 (mucinous), SLC39A11 (low malignant potential), and SERPINA7 (clear cell carcinoma). In addition, 1785 SNPs in six genes (HEPH, MGST1, SERPINA, SLC25A45, SLC39A11 and UGT1A) were imputed from the 1000 Genomes Project and examined for association with INV EOC in white-European subjects. The most significant imputed SNP was rs117729793 in SLC39A11 (per allele, OR = 2.55, 95% CI = 1.5-4.35, p = 5.66x10-4). CONCLUSION: These results, generated on a large cohort of women, revealed associations between inherited cellular transport gene variants and risk of EOC histologic subtypes.
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    PALB2, CHEK2 and ATM rare variants and cancer risk: data from COGS
    Southey, MC ; Goldgar, DE ; Winqvist, R ; Pylkas, K ; Couch, F ; Tischkowitz, M ; Foulkes, WD ; Dennis, J ; Michailidou, K ; van Rensburg, EJ ; Heikkinen, T ; Nevanlinna, H ; Hopper, JL ; Doerk, T ; Claes, KBM ; Reis-Filho, J ; Teo, ZL ; Radice, P ; Catucci, I ; Peterlongo, P ; Tsimiklis, H ; Odefrey, FA ; Dowty, JG ; Schmidt, MK ; Broeks, A ; Hogervorst, FB ; Verhoef, S ; Carpenter, J ; Clarke, C ; Scott, RJ ; Fasching, PA ; Haeberle, L ; Ekici, AB ; Beckmann, MW ; Peto, J ; dos-Santos-Silva, I ; Fletcher, O ; Johnson, N ; Bolla, MK ; Sawyer, EJ ; Tomlinson, I ; Kerin, MJ ; Miller, N ; Marme, F ; Burwinkel, B ; Yang, R ; Guenel, P ; Therese, T ; Menegaux, F ; Sanchez, M ; Bojesen, S ; Nielsen, SF ; Flyger, H ; Benitez, J ; Pilar Zamora, M ; Arias Perez, JI ; Menendez, P ; Anton-Culver, H ; Neuhausen, S ; Ziogas, A ; Clarke, CA ; Brenner, H ; Arndt, V ; Stegmaier, C ; Brauch, H ; Bruening, T ; Ko, Y-D ; Muranen, TA ; Aittomaki, K ; Blomqvist, C ; Bogdanova, NV ; Antonenkova, NN ; Lindblom, A ; Margolin, S ; Mannermaa, A ; Kataja, V ; Kosma, V-M ; Hartikainen, JM ; Spurdle, AB ; Wauters, E ; Smeets, D ; Beuselinck, B ; Floris, G ; Chang-Claude, J ; Rudolph, A ; Seibold, P ; Flesch-Janys, D ; Olson, JE ; Vachon, C ; Pankratz, VS ; McLean, C ; Haiman, CA ; Henderson, BE ; Schumacher, F ; Le Marchand, L ; Kristensen, V ; Alnaes, GG ; Zheng, W ; Hunter, DJ ; Lindstrom, S ; Hankinson, SE ; Kraft, P ; Andrulis, I ; Knight, JA ; Glendon, G ; Mulligan, AM ; Jukkola-Vuorinen, A ; Grip, M ; Kauppila, S ; Devilee, P ; Tollenaar, RAEM ; Seynaeve, C ; Hollestelle, A ; Garcia-Closas, M ; Figueroa, J ; Chanock, SJ ; Lissowska, J ; Czene, K ; Darabi, H ; Eriksson, M ; Eccles, DM ; Rafiq, S ; Tapper, WJ ; Gerty, SM ; Hooning, MJ ; Martens, JWM ; Collee, JM ; Tilanus-Linthorst, M ; Hall, P ; Li, J ; Brand, JS ; Humphreys, K ; Cox, A ; Reed, MWR ; Luccarini, C ; Baynes, C ; Dunning, AM ; Hamann, U ; Torres, D ; Ulmer, HU ; Ruediger, T ; Jakubowska, A ; Lubinski, J ; Jaworska, K ; Durda, K ; Slager, S ; Toland, AE ; Ambrosone, CB ; Yannoukakos, D ; Swerdlow, A ; Ashworth, A ; Orr, N ; Jones, M ; Gonzalez-Neira, A ; Pita, G ; Rosario Alonso, M ; Alvarez, N ; Herrero, D ; Tessier, DC ; Vincent, D ; Bacot, F ; Simard, J ; Dumont, M ; Soucy, P ; Eeles, R ; Muir, K ; Wiklund, F ; Gronberg, H ; Schleutker, J ; Nordestgaard, BG ; Weischer, M ; Travis, RC ; Neal, D ; Donovan, JL ; Hamdy, FC ; Khaw, K-T ; Stanford, JL ; Blot, WJ ; Thibodeau, S ; Schaid, DJ ; Kelley, JL ; Maier, C ; Kibel, AS ; Cybulski, C ; Cannon-Albright, L ; Butterbach, K ; Park, J ; Kaneva, R ; Batra, J ; Teixeira, MR ; Kote-Jarai, Z ; Al Olama, AA ; Benlloch, S ; Renner, SP ; Hartmann, A ; Hein, A ; Ruebner, M ; Lambrechts, D ; Van Nieuwenhuysen, E ; Vergote, I ; Lambretchs, S ; Doherty, JA ; Rossing, MA ; Nickels, S ; Eilber, U ; Wang-Gohrke, S ; Odunsi, K ; Sucheston-Campbell, LE ; Friel, G ; Lurie, G ; Killeen, JL ; Wilkens, LR ; Goodman, MT ; Runnebaum, I ; Hillemanns, PA ; Pelttari, LM ; Butzow, R ; Modugno, F ; Edwards, RP ; Ness, RB ; Moysich, KB ; du Bois, A ; Heitz, F ; Harter, P ; Kommoss, S ; Karlan, BY ; Walsh, C ; Lester, J ; Jensen, A ; Kjaer, SK ; Hogdall, E ; Peissel, B ; Bonanni, B ; Bernard, L ; Goode, EL ; Fridley, BL ; Vierkant, RA ; Cunningham, JM ; Larson, MC ; Fogarty, ZC ; Kalli, KR ; Liang, D ; Lu, KH ; Hildebrandt, MAT ; Wu, X ; Levine, DA ; Dao, F ; Bisogna, M ; Berchuck, A ; Iversen, ES ; Marks, JR ; Akushevich, L ; Cramer, DW ; Schildkraut, J ; Terry, KL ; Poole, EM ; Stampfer, M ; Tworoger, SS ; Bandera, EV ; Orlow, I ; Olson, SH ; Bjorge, L ; Salvesen, HB ; van Altena, AM ; Aben, KKH ; Kiemeney, LA ; Massuger, LFAG ; Pejovic, T ; Bean, Y ; Brooks-Wilson, A ; Kelemen, LE ; Cook, LS ; Le, ND ; Grski, B ; Gronwald, J ; Menkiszak, J ; Hogdall, CK ; Lundvall, L ; Nedergaard, L ; Engelholm, SA ; Dicks, E ; Tyrer, J ; Campbell, I ; McNeish, I ; Paul, J ; Siddiqui, N ; Glasspool, R ; Whittemore, AS ; Rothstein, JH ; McGuire, V ; Sieh, W ; Cai, H ; Shu, X-O ; Teten, RT ; Sutphen, R ; McLaughlin, JR ; Narod, SA ; Phelan, CM ; Monteiro, AN ; Fenstermacher, D ; Lin, H-Y ; Permuth, JB ; Sellers, TA ; Chen, YA ; Tsai, Y-Y ; Chen, Z ; Gentry-Maharaj, A ; Gayther, SA ; Ramus, SJ ; Menon, U ; Wu, AH ; Pearce, CL ; Van den Berg, D ; Pike, MC ; Dansonka-Mieszkowska, A ; Plisiecka-Halasa, J ; Moes-Sosnowska, J ; Kupryjanczyk, J ; Pharoah, PDP ; Song, H ; Winship, I ; Chenevix-Trench, G ; Giles, GG ; Tavtigian, SV ; Easton, DF ; Milne, RL (BMJ PUBLISHING GROUP, 2016-12)
    BACKGROUND: The rarity of mutations in PALB2, CHEK2 and ATM make it difficult to estimate precisely associated cancer risks. Population-based family studies have provided evidence that at least some of these mutations are associated with breast cancer risk as high as those associated with rare BRCA2 mutations. We aimed to estimate the relative risks associated with specific rare variants in PALB2, CHEK2 and ATM via a multicentre case-control study. METHODS: We genotyped 10 rare mutations using the custom iCOGS array: PALB2 c.1592delT, c.2816T>G and c.3113G>A, CHEK2 c.349A>G, c.538C>T, c.715G>A, c.1036C>T, c.1312G>T, and c.1343T>G and ATM c.7271T>G. We assessed associations with breast cancer risk (42 671 cases and 42 164 controls), as well as prostate (22 301 cases and 22 320 controls) and ovarian (14 542 cases and 23 491 controls) cancer risk, for each variant. RESULTS: For European women, strong evidence of association with breast cancer risk was observed for PALB2 c.1592delT OR 3.44 (95% CI 1.39 to 8.52, p=7.1×10-5), PALB2 c.3113G>A OR 4.21 (95% CI 1.84 to 9.60, p=6.9×10-8) and ATM c.7271T>G OR 11.0 (95% CI 1.42 to 85.7, p=0.0012). We also found evidence of association with breast cancer risk for three variants in CHEK2, c.349A>G OR 2.26 (95% CI 1.29 to 3.95), c.1036C>T OR 5.06 (95% CI 1.09 to 23.5) and c.538C>T OR 1.33 (95% CI 1.05 to 1.67) (p≤0.017). Evidence for prostate cancer risk was observed for CHEK2 c.1343T>G OR 3.03 (95% CI 1.53 to 6.03, p=0.0006) for African men and CHEK2 c.1312G>T OR 2.21 (95% CI 1.06 to 4.63, p=0.030) for European men. No evidence of association with ovarian cancer was found for any of these variants. CONCLUSIONS: This report adds to accumulating evidence that at least some variants in these genes are associated with an increased risk of breast cancer that is clinically important.
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    Adult height is associated with increased risk of ovarian cancer: a Mendelian randomisation study
    Dixon-Suen, SC ; Nagle, CM ; Thrift, AP ; Pharoah, PDP ; Ewing, A ; Pearce, CL ; Zheng, W ; Chenevix-Trench, G ; Fasching, PA ; Beckmann, MW ; Lambrechts, D ; Vergote, I ; Lambrechts, S ; Van Nieuwenhuysen, E ; Rossing, MA ; Doherty, JA ; Wicklund, KG ; Chang-Claude, J ; Jung, AY ; Moysich, KB ; Odunsi, K ; Goodman, MT ; Wilkens, LR ; Thompson, PJ ; Shvetsov, YB ; Doerk, T ; Park-Simon, T-W ; Hillemanns, P ; Bogdanova, N ; Butzow, R ; Nevanlinna, H ; Pelttari, LM ; Leminen, A ; Modugno, F ; Ness, RB ; Edwards, RP ; Kelley, JL ; Heitz, F ; du Bois, A ; Harter, P ; Schwaab, I ; Karlan, BY ; Lester, J ; Orsulic, S ; Rimel, BJ ; Kjaer, SK ; Hogdall, E ; Jensen, A ; Goode, EL ; Fridley, BL ; Cunningham, JM ; Winham, SJ ; Giles, GG ; Bruinsma, F ; Milne, RL ; Southey, MC ; Hildebrandt, MAT ; Wu, X ; Lu, KH ; Liang, D ; Levine, DA ; Bisogna, M ; Schildkraut, JM ; Berchuck, A ; Cramer, DW ; Terry, KL ; Bandera, EV ; Olson, SH ; Salvesen, HB ; Thomsen, LCV ; Kopperud, RK ; Bjorge, L ; Kiemeney, LA ; Massuger, LFAG ; Pejovic, T ; Bruegl, A ; Cook, LS ; Le, ND ; Swenerton, KD ; Brooks-Wilson, A ; Kelemen, LE ; Lubinski, J ; Huzarski, T ; Gronwald, J ; Menkiszak, J ; Wentzensen, N ; Brinton, L ; Yang, H ; Lissowska, J ; Hogdall, CK ; Lundvall, L ; Song, H ; Tyrer, JP ; Campbell, I ; Eccles, D ; Paul, J ; Glasspool, R ; Siddiqui, N ; Whittemore, AS ; Sieh, W ; McGuire, V ; Rothstein, JH ; Narod, SA ; Phelan, C ; Risch, HA ; McLaughlin, JR ; Anton-Culver, H ; Ziogas, A ; Menon, U ; Gayther, SA ; Ramus, SJ ; Gentry-Maharaj, A ; Wu, AH ; Pike, MC ; Tseng, C-C ; Kupryjanczyk, J ; Dansonka-Mieszkowska, A ; Budzilowska, A ; Rzepecka, IK ; Webb, PM (NATURE PUBLISHING GROUP, 2018-04)
    BACKGROUND: Observational studies suggest greater height is associated with increased ovarian cancer risk, but cannot exclude bias and/or confounding as explanations for this. Mendelian randomisation (MR) can provide evidence which may be less prone to bias. METHODS: We pooled data from 39 Ovarian Cancer Association Consortium studies (16,395 cases; 23,003 controls). We applied two-stage predictor-substitution MR, using a weighted genetic risk score combining 609 single-nucleotide polymorphisms. Study-specific odds ratios (OR) and 95% confidence intervals (CI) for the association between genetically predicted height and risk were pooled using random-effects meta-analysis. RESULTS: Greater genetically predicted height was associated with increased ovarian cancer risk overall (pooled-OR (pOR) = 1.06; 95% CI: 1.01-1.11 per 5 cm increase in height), and separately for invasive (pOR = 1.06; 95% CI: 1.01-1.11) and borderline (pOR = 1.15; 95% CI: 1.02-1.29) tumours. CONCLUSIONS: Women with a genetic propensity to being taller have increased risk of ovarian cancer. This suggests genes influencing height are involved in pathways promoting ovarian carcinogenesis.
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    Fine-mapping of prostate cancer susceptibility loci in a large meta-analysis identifies candidate causal variants
    Dadaev, T ; Saunders, EJ ; Newcombe, PJ ; Anokian, E ; Leongamornlert, DA ; Brook, MN ; Cieza-Borrella, C ; Mijuskovic, M ; Wakerell, S ; Al Olama, AA ; Schumacher, FR ; Berndt, SI ; Benlloch, S ; Ahmed, M ; Goh, C ; Sheng, X ; Zhang, Z ; Muir, K ; Govindasami, K ; Lophatananon, A ; Stevens, VL ; Gapstur, SM ; Carter, BD ; Tangen, CM ; Goodman, P ; Thompson, IM ; Batra, J ; Chambers, S ; Moya, L ; Clements, J ; Horvath, L ; Tilley, W ; Risbridger, G ; Gronberg, H ; Aly, M ; Nordstrom, T ; Pharoah, P ; Pashayan, N ; Schleutker, J ; Tammela, TLJ ; Sipeky, C ; Auvinen, A ; Albanes, D ; Weinstein, S ; Wolk, A ; Hakansson, N ; West, C ; Dunning, AM ; Burnet, N ; Mucci, L ; Giovannucci, E ; Andriole, G ; Cussenot, O ; Cancel-Tassin, G ; Koutros, S ; Freeman, LEB ; Sorensen, KD ; Orntoft, TF ; Borre, M ; Maehle, L ; Grindedal, EM ; Neal, DE ; Donovan, JL ; Hamdy, FC ; Martin, RM ; Travis, RC ; Key, TJ ; Hamilton, RJ ; Fleshner, NE ; Finelli, A ; Ingles, SA ; Stern, MC ; Rosenstein, B ; Kerns, S ; Ostrer, H ; Lu, Y-J ; Zhang, H-W ; Feng, N ; Mao, X ; Guo, X ; Wang, G ; Sun, Z ; Giles, GG ; Southey, MC ; MacInnis, RJ ; FitzGerald, LM ; Kibel, AS ; Drake, BF ; Vega, A ; Gomez-Caamano, A ; Fachal, L ; Szulkin, R ; Eklund, M ; Kogevinas, M ; Llorca, J ; Castano-Vinyals, G ; Penney, KL ; Stampfer, M ; Park, JY ; Sellers, TA ; Lin, H-Y ; Stanford, JL ; Cybulski, C ; Wokolorczyk, D ; Lubinski, J ; Ostrander, EA ; Geybels, MS ; Nordestgaard, BG ; Nielsen, SF ; Weisher, M ; Bisbjerg, R ; Roder, MA ; Iversen, P ; Brenner, H ; Cuk, K ; Holleczek, B ; Maier, C ; Luedeke, M ; Schnoeller, T ; Kim, J ; Logothetis, CJ ; John, EM ; Teixeira, MR ; Paulo, P ; Cardoso, M ; Neuhausen, SL ; Steele, L ; Ding, YC ; De Ruyck, K ; De Meerleer, G ; Ost, P ; Razack, A ; Lim, J ; Teo, S-H ; Lin, DW ; Newcomb, LF ; Lessel, D ; Gamulin, M ; Kulis, T ; Kaneva, R ; Usmani, N ; Slavov, C ; Mitev, V ; Parliament, M ; Singhal, S ; Claessens, F ; Joniau, S ; Van den Broeck, T ; Larkin, S ; Townsend, PA ; Aukim-Hastie, C ; Gago-Dominguez, M ; Castelao, JE ; Martinez, ME ; Roobol, MJ ; Jenster, G ; van Schaik, RHN ; Menegaux, F ; Truong, T ; Koudou, YA ; Xu, J ; Khaw, K-T ; Cannon-Albright, L ; Pandha, H ; Michael, A ; Kierzek, A ; Thibodeau, SN ; McDonnell, SK ; Schaid, DJ ; Lindstrom, S ; Turman, C ; Ma, J ; Hunter, DJ ; Riboli, E ; Siddiq, A ; Canzian, F ; Kolonel, LN ; Le Marchand, L ; Hoover, RN ; Machiela, MJ ; Kraft, P ; Freedman, M ; Wiklund, F ; Chanock, S ; Henderson, BE ; Easton, DF ; Haiman, CA ; Eeles, RA ; Conti, DV ; Kote-Jarai, Z (NATURE PORTFOLIO, 2018-06-11)
    Prostate cancer is a polygenic disease with a large heritable component. A number of common, low-penetrance prostate cancer risk loci have been identified through GWAS. Here we apply the Bayesian multivariate variable selection algorithm JAM to fine-map 84 prostate cancer susceptibility loci, using summary data from a large European ancestry meta-analysis. We observe evidence for multiple independent signals at 12 regions and 99 risk signals overall. Only 15 original GWAS tag SNPs remain among the catalogue of candidate variants identified; the remainder are replaced by more likely candidates. Biological annotation of our credible set of variants indicates significant enrichment within promoter and enhancer elements, and transcription factor-binding sites, including AR, ERG and FOXA1. In 40 regions at least one variant is colocalised with an eQTL in prostate cancer tissue. The refined set of candidate variants substantially increase the proportion of familial relative risk explained by these known susceptibility regions, which highlights the importance of fine-mapping studies and has implications for clinical risk profiling.
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    Age-specific breast cancer risk by body mass index and familial risk: prospective family study cohort (ProF-SC)
    Hopper, JL ; Dite, GS ; MacInnis, RJ ; Liao, Y ; Zeinomar, N ; Knight, JA ; Southey, MC ; Milne, RL ; Chung, WK ; Giles, GG ; Genkinger, JM ; McLachlan, S-A ; Friedlander, ML ; Antoniou, AC ; Weideman, PC ; Glendon, G ; Nesci, S ; Andrulis, IL ; Buys, SS ; Daly, MB ; John, EM ; Phillips, KA ; Terry, MB (BMC, 2018-11-03)
    BACKGROUND: The association between body mass index (BMI) and risk of breast cancer depends on time of life, but it is unknown whether this association depends on a woman's familial risk. METHODS: We conducted a prospective study of a cohort enriched for familial risk consisting of 16,035 women from 6701 families in the Breast Cancer Family Registry and the Kathleen Cunningham Foundation Consortium for Research into Familial Breast Cancer followed for up to 20 years (mean 10.5 years). There were 896 incident breast cancers (mean age at diagnosis 55.7 years). We used Cox regression to model BMI risk associations as a function of menopausal status, age, and underlying familial risk based on pedigree data using the Breast and Ovarian Analysis of Disease Incidence and Carrier Estimation Algorithm (BOADICEA), all measured at baseline. RESULTS: The strength and direction of the BMI risk association depended on baseline menopausal status (P < 0.001); after adjusting for menopausal status, the association did not depend on age at baseline (P = 0.6). In terms of absolute risk, the negative association with BMI for premenopausal women has a much smaller influence than the positive association with BMI for postmenopausal women. Women at higher familial risk have a much larger difference in absolute risk depending on their BMI than women at lower familial risk. CONCLUSIONS: The greater a woman's familial risk, the greater the influence of BMI on her absolute postmenopausal breast cancer risk. Given that age-adjusted BMI is correlated across adulthood, maintaining a healthy weight throughout adult life is particularly important for women with a family history of breast cancer.