Melbourne School of Population and Global Health - Research Publications

Permanent URI for this collection

http://hdl.handle.net/11343/247

Filters

2008 - 2009 1 2010 - 2012 10
11
Reset filters

Settings
Statistics
Citations
Author: Giles, Graham × Author: Southey, Melissa × Author: Baglietto, Laura × End date: 2012 ×

Search Results

Now showing 1 - 10 of 11
  • Item
    No Preview Available
    Genome-wide association analysis identifies three new breast cancer susceptibility loci
    Ghoussaini, M ; Fletcher, O ; Michailidou, K ; Turnbull, C ; Schmidt, MK ; Dicks, E ; Dennis, J ; Wang, Q ; Humphreys, MK ; Luccarini, C ; Baynes, C ; Conroy, D ; Maranian, M ; Ahmed, S ; Driver, K ; Johnson, N ; Orr, N ; Silva, IDS ; Waisfisz, Q ; Meijers-Heijboer, H ; Uitterlinden, AG ; Rivadeneira, F ; Hall, P ; Czene, K ; Irwanto, A ; Liu, J ; Nevanlinna, H ; Aittomaki, K ; Blomqvist, C ; Meindl, A ; Schmutzler, RK ; Mueller-Myhsok, B ; Lichtner, P ; Chang-Claude, J ; Hein, R ; Nickels, S ; Flesch-Janys, D ; Tsimiklis, H ; Makalic, E ; Schmidt, D ; Bui, M ; Hopper, JL ; Apicella, C ; Park, DJ ; Southey, M ; Hunter, DJ ; Chanock, SJ ; Broeks, A ; Verhoef, S ; Hogervorst, FBL ; Fasching, PA ; Lux, MP ; Beckmann, MW ; Ekici, AB ; Sawyer, E ; Tomlinson, I ; Kerin, M ; Marme, F ; Schneeweiss, A ; Sohn, C ; Burwinkel, B ; Guenel, P ; Truong, T ; Cordina-Duverger, E ; Menegaux, F ; Bojesen, SE ; Nordestgaard, BG ; Nielsen, SF ; Flyger, H ; Milne, RL ; Rosario Alonso, M ; Gonzalez-Neira, A ; Benitez, J ; Anton-Culver, H ; Ziogas, A ; Bernstein, L ; Dur, CC ; Brenner, H ; Mueller, H ; Arndt, V ; Stegmaier, C ; Justenhoven, C ; Brauch, H ; Bruening, T ; Wang-Gohrke, S ; Eilber, U ; Doerk, T ; Schuermann, P ; Bremer, M ; Hillemanns, P ; Bogdanova, NV ; Antonenkova, NN ; Rogov, YI ; Karstens, JH ; Bermisheva, M ; Prokofieva, D ; Khusnutdinova, E ; Lindblom, A ; Margolin, S ; Mannermaa, A ; Kataja, V ; Kosma, V-M ; Hartikainen, JM ; Lambrechts, D ; Yesilyurt, BT ; Floris, G ; Leunen, K ; Manoukian, S ; Bonanni, B ; Fortuzzi, S ; Peterlongo, P ; Couch, FJ ; Wang, X ; Stevens, K ; Lee, A ; Giles, GG ; Baglietto, L ; Severi, G ; McLean, C ; Alnaes, GG ; Kristensen, V ; Borrensen-Dale, A-L ; John, EM ; Miron, A ; Winqvist, R ; Pylkas, K ; Jukkola-Vuorinen, A ; Kauppila, S ; Andrulis, IL ; Glendon, G ; Mulligan, AM ; Devilee, P ; van Asperen, CJ ; Tollenaar, RAEM ; Seynaeve, C ; Figueroa, JD ; Garcia-Closas, M ; Brinton, L ; Lissowska, J ; Hooning, MJ ; Hollestelle, A ; Oldenburg, RA ; van den Ouweland, AMW ; Cox, A ; Reed, MWR ; Shah, M ; Jakubowska, A ; Lubinski, J ; Jaworska, K ; Durda, K ; Jones, M ; Schoemaker, M ; Ashworth, A ; Swerdlow, A ; Beesley, J ; Chen, X ; Muir, KR ; Lophatananon, A ; Rattanamongkongul, S ; Chaiwerawattana, A ; Kang, D ; Yoo, K-Y ; Noh, D-Y ; Shen, C-Y ; Yu, J-C ; Wu, P-E ; Hsiung, C-N ; Perkins, A ; Swann, R ; Velentzis, L ; Eccles, DM ; Tapper, WJ ; Gerty, SM ; Graham, NJ ; Ponder, BAJ ; Chenevix-Trench, G ; Pharoah, PDP ; Lathrop, M ; Dunning, AM ; Rahman, N ; Peto, J ; Easton, DF (NATURE PUBLISHING GROUP, 2012-03)
    Breast cancer is the most common cancer among women. To date, 22 common breast cancer susceptibility loci have been identified accounting for ∼8% of the heritability of the disease. We attempted to replicate 72 promising associations from two independent genome-wide association studies (GWAS) in ∼70,000 cases and ∼68,000 controls from 41 case-control studies and 9 breast cancer GWAS. We identified three new breast cancer risk loci at 12p11 (rs10771399; P = 2.7 × 10(-35)), 12q24 (rs1292011; P = 4.3 × 10(-19)) and 21q21 (rs2823093; P = 1.1 × 10(-12)). rs10771399 was associated with similar relative risks for both estrogen receptor (ER)-negative and ER-positive breast cancer, whereas the other two loci were associated only with ER-positive disease. Two of the loci lie in regions that contain strong plausible candidate genes: PTHLH (12p11) has a crucial role in mammary gland development and the establishment of bone metastasis in breast cancer, and NRIP1 (21q21) encodes an ER cofactor and has a role in the regulation of breast cancer cell growth.
  • Item
    Thumbnail Image
    Evaluation of variation in the phosphoinositide-3-kinase catalytic subunit alpha oncogene and breast cancer risk
    Stevens, KN ; Garcia-Closas, M ; Fredericksen, Z ; Kosel, M ; Pankratz, VS ; Hopper, JL ; Dite, GS ; Apicella, C ; Southey, MC ; Schmidt, MK ; Broeks, A ; Van 't Veer, LJ ; Tollenaar, RAEM ; Fasching, PA ; Beckmann, MW ; Hein, A ; Ekici, AB ; Johnson, N ; Peto, J ; Silva, IDS ; Gibson, L ; Sawyer, E ; Tomlinson, I ; Kerin, MJ ; Chanock, S ; Lissowska, J ; Hunter, DJ ; Hoover, RN ; Thomas, GD ; Milne, RL ; Perez, JIA ; Gonzalez-Neira, A ; Benitez, J ; Burwinkel, B ; Meindl, A ; Schmutzler, RK ; Bartrar, CR ; Hamann, U ; Ko, YD ; Bruening, T ; Chang-Claude, J ; Hein, R ; Wang-Gohrke, S ; Doerk, T ; Schuermann, P ; Bremer, M ; Hillemanns, P ; Bogdanova, N ; Zalutsky, JV ; Rogov, YI ; Antonenkova, N ; Lindblom, A ; Margolin, S ; Mannermaa, A ; Kataja, V ; Kosma, V-M ; Hartikainen, J ; Chenevix-Trench, G ; Chen, X ; Peterlongo, P ; Bonanni, B ; Bernard, L ; Manoukian, S ; Wang, X ; Cerhan, J ; Vachon, CM ; Olson, J ; Giles, GG ; Baglietto, L ; McLean, CA ; Severi, G ; John, EM ; Miron, A ; Winqvist, R ; Pylkaes, K ; Jukkola-Vuorinen, A ; Grip, M ; Andrulis, I ; Knight, JA ; Glendon, G ; Mulligan, AM ; Cox, A ; Brock, IW ; Elliott, G ; Cross, SS ; Pharoah, PP ; Dunning, AM ; Pooley, KA ; Humphreys, MK ; Wang, J ; Kang, D ; Yoo, K-Y ; Noh, D-Y ; Sangrajrang, S ; Gabrieau, V ; Brennan, P ; Mckay, J ; Anton-Culver, H ; Ziogas, A ; Couch, FJ ; Easton, DF (NATURE PUBLISHING GROUP, 2011-12-06)
    BACKGROUND: Somatic mutations in phosphoinositide-3-kinase catalytic subunit alpha (PIK3CA) are frequent in breast tumours and have been associated with oestrogen receptor (ER) expression, human epidermal growth factor receptor-2 overexpression, lymph node metastasis and poor survival. The goal of this study was to evaluate the association between inherited variation in this oncogene and risk of breast cancer. METHODS: A single-nucleotide polymorphism from the PIK3CA locus that was associated with breast cancer in a study of Caucasian breast cancer cases and controls from the Mayo Clinic (MCBCS) was genotyped in 5436 cases and 5280 controls from the Cancer Genetic Markers of Susceptibility (CGEMS) study and in 30 949 cases and 29 788 controls from the Breast Cancer Association Consortium (BCAC). RESULTS: Rs1607237 was significantly associated with a decreased risk of breast cancer in MCBCS, CGEMS and all studies of white Europeans combined (odds ratio (OR)=0.97, 95% confidence interval (CI) 0.95-0.99, P=4.6 × 10(-3)), but did not reach significance in the BCAC replication study alone (OR=0.98, 95% CI 0.96-1.01, P=0.139). CONCLUSION: Common germline variation in PIK3CA does not have a strong influence on the risk of breast cancer.
  • Item
    Thumbnail Image
    Plasma concentration of Propionibacterium acnes antibodies and prostate cancer risk: results from an Australian population-based case-control study
    Severi, G ; Shannon, BA ; Hoang, HN ; Baglietto, L ; English, DR ; Hopper, JL ; Pedersen, J ; Southey, MC ; Sinclair, R ; Cohen, RJ ; Giles, GG (NATURE PUBLISHING GROUP, 2010-07-27)
    BACKGROUND: Recent studies in prostatic tissue suggest that Propionibacterium acnes (P. acnes), a bacterium associated with acne that normally lives on the skin, is the most prevalent bacterium in the prostate and in men with benign prostatic hyperplasia. Its prevalence is higher in samples from patients subsequently diagnosed with prostate cancer. The aim of our study was to test whether circulating levels of P. acnes antibodies are associated with prostate cancer risk and tumour characteristics using plasma samples from a population-based case-control study. METHODS: We measured plasma concentration of P. acnes antibodies for 809 cases and 584 controls using a recently developed ELISA assay. We compared antibody titres between cases and controls using unconditional logistic regression adjusted for batch and variables associated with the study design (i.e., age, year of selection and centre). The primary analysis included P. acnes titres in the model as a dichotomous variable using the median value for controls as the cut-off value. RESULTS: P. acnes antibody titres for both cases and controls ranged from 1 : 16 (i.e., low concentration) to 1 : 65,536 (i.e., high concentration; median value=1 : 1024). The odds ratio for prostate cancer associated with titres at or above the median value was 0.73 (95% CI 0.58-0.91, P=0.005). The association appeared to be particularly strong for advanced prostate cancer (AJCC Stage grouping III-IV) for which the odds ratio was 0.59 (95% CI 0.43-0.81, P=0.001) but there was insufficient evidence that the association differed by tumour stage (p heterogeneity=0.07). CONCLUSION: These results need to be confirmed in prospective studies but they are consistent with the hypothesis that P. acnes has a role in prostate cancer.
  • Item
    No Preview Available
    Subtyping of Breast Cancer by Immunohistochemistry to Investigate a Relationship between Subtype and Short and Long Term Survival: A Collaborative Analysis of Data for 10,159 Cases from 12 Studies
    Blows, FM ; Driver, KE ; Schmidt, MK ; Broeks, A ; van Leeuwen, FE ; Wesseling, J ; Cheang, MC ; Gelmon, K ; Nielsen, TO ; Blomqvist, C ; Heikkila, P ; Heikkinen, T ; Nevanlinna, H ; Akslen, LA ; Begin, LR ; Foulkes, WD ; Couch, FJ ; Wang, X ; Cafourek, V ; Olson, JE ; Baglietto, L ; Giles, GG ; Severi, G ; McLean, CA ; Southey, MC ; Rakha, E ; Green, AR ; Ellis, IO ; Sherman, ME ; Lissowska, J ; Anderson, WF ; Cox, A ; Cross, SS ; Reed, MWR ; Provenzano, E ; Dawson, S-J ; Dunning, AM ; Humphreys, M ; Easton, DF ; Garcia-Closas, M ; Caldas, C ; Pharoah, PD ; Huntsman, D ; Marincola, FM (PUBLIC LIBRARY SCIENCE, 2010-05)
    BACKGROUND: Immunohistochemical markers are often used to classify breast cancer into subtypes that are biologically distinct and behave differently. The aim of this study was to estimate mortality for patients with the major subtypes of breast cancer as classified using five immunohistochemical markers, to investigate patterns of mortality over time, and to test for heterogeneity by subtype. METHODS AND FINDINGS: We pooled data from more than 10,000 cases of invasive breast cancer from 12 studies that had collected information on hormone receptor status, human epidermal growth factor receptor-2 (HER2) status, and at least one basal marker (cytokeratin [CK]5/6 or epidermal growth factor receptor [EGFR]) together with survival time data. Tumours were classified as luminal and nonluminal tumours according to hormone receptor expression. These two groups were further subdivided according to expression of HER2, and finally, the luminal and nonluminal HER2-negative tumours were categorised according to expression of basal markers. Changes in mortality rates over time differed by subtype. In women with luminal HER2-negative subtypes, mortality rates were constant over time, whereas mortality rates associated with the luminal HER2-positive and nonluminal subtypes tended to peak within 5 y of diagnosis and then decline over time. In the first 5 y after diagnosis the nonluminal tumours were associated with a poorer prognosis, but over longer follow-up times the prognosis was poorer in the luminal subtypes, with the worst prognosis at 15 y being in the luminal HER2-positive tumours. Basal marker expression distinguished the HER2-negative luminal and nonluminal tumours into different subtypes. These patterns were independent of any systemic adjuvant therapy. CONCLUSIONS: The six subtypes of breast cancer defined by expression of five markers show distinct behaviours with important differences in short term and long term prognosis. Application of these markers in the clinical setting could have the potential to improve the targeting of adjuvant chemotherapy to those most likely to benefit. The different patterns of mortality over time also suggest important biological differences between the subtypes that may result in differences in response to specific therapies, and that stratification of breast cancers by clinically relevant subtypes in clinical trials is urgently required.
  • Item
    No Preview Available
    Heterogeneity of breast cancer associations with five susceptibility loci by clinical and pathological characteristics
    Garcia-Closas, M ; Hall, P ; Nevanlinna, H ; Pooley, K ; Morrison, J ; Richesson, DA ; Bojesen, SE ; Nordestgaard, BG ; Axelsson, CK ; Arias, JI ; Milne, RL ; Ribas, G ; Gonzalez-Neira, A ; Benitez, J ; Zamora, P ; Brauch, H ; Justenhoven, C ; Hamann, U ; Ko, Y-D ; Bruening, T ; Haas, S ; Doerk, T ; Schuermann, P ; Hillemanns, P ; Bogdanova, N ; Bremer, M ; Karstens, JH ; Fagerholm, R ; Aaltonen, K ; Aittomaki, K ; Von Smitten, K ; Blomqvist, C ; Mannermaa, A ; Uusitupa, M ; Eskelinen, M ; Tengstrom, M ; Kosma, V-M ; Kataja, V ; Chenevix-Trench, G ; Spurdle, AB ; Beesley, J ; Chen, X ; Devilee, P ; Van Asperen, CJ ; Jacobi, CE ; Tollenaar, RAEM ; Huijts, PEA ; Klijn, JGM ; Chang-Claude, J ; Kropp, S ; Slanger, T ; Flesch-Janys, D ; Mutschelknauss, E ; Salazar, R ; Wang-Gohrke, S ; Couch, F ; Goode, EL ; Olson, JE ; Vachon, C ; Fredericksen, ZS ; Giles, GG ; Baglietto, L ; Severi, G ; Hopper, JL ; English, DR ; Southey, MC ; Haiman, CA ; Henderson, BE ; Kolonel, LN ; Le Marchand, L ; Stram, DO ; Hunter, DJ ; Hankinson, SE ; Cox, DG ; Tamimi, R ; Kraft, P ; Sherman, ME ; Chanock, SJ ; Lissowska, J ; Brinton, LA ; Peplonska, B ; Klijn, JGM ; Hooning, MJ ; Meijers-Heijboer, H ; Collee, JM ; Van den Ouweland, A ; Uitterlinden, AG ; Liu, J ; Lin, LY ; Yuqing, L ; Humphreys, K ; Czene, K ; Cox, A ; Balasubramanian, SP ; Cross, SS ; Reed, MWR ; Blows, F ; Driver, K ; Dunning, A ; Tyrer, J ; Ponder, BAJ ; Sangrajrang, S ; Brennan, P ; Mckay, J ; Odefrey, F ; Gabrieau, V ; Sigurdson, A ; Doody, M ; Struewing, JP ; Alexander, B ; Easton, DF ; Pharoah, PD ; Leal, SM (PUBLIC LIBRARY SCIENCE, 2008-04)
    A three-stage genome-wide association study recently identified single nucleotide polymorphisms (SNPs) in five loci (fibroblast growth receptor 2 (FGFR2), trinucleotide repeat containing 9 (TNRC9), mitogen-activated protein kinase 3 K1 (MAP3K1), 8q24, and lymphocyte-specific protein 1 (LSP1)) associated with breast cancer risk. We investigated whether the associations between these SNPs and breast cancer risk varied by clinically important tumor characteristics in up to 23,039 invasive breast cancer cases and 26,273 controls from 20 studies. We also evaluated their influence on overall survival in 13,527 cases from 13 studies. All participants were of European or Asian origin. rs2981582 in FGFR2 was more strongly related to ER-positive (per-allele OR (95%CI) = 1.31 (1.27-1.36)) than ER-negative (1.08 (1.03-1.14)) disease (P for heterogeneity = 10(-13)). This SNP was also more strongly related to PR-positive, low grade and node positive tumors (P = 10(-5), 10(-8), 0.013, respectively). The association for rs13281615 in 8q24 was stronger for ER-positive, PR-positive, and low grade tumors (P = 0.001, 0.011 and 10(-4), respectively). The differences in the associations between SNPs in FGFR2 and 8q24 and risk by ER and grade remained significant after permutation adjustment for multiple comparisons and after adjustment for other tumor characteristics. Three SNPs (rs2981582, rs3803662, and rs889312) showed weak but significant associations with ER-negative disease, the strongest association being for rs3803662 in TNRC9 (1.14 (1.09-1.21)). rs13281615 in 8q24 was associated with an improvement in survival after diagnosis (per-allele HR = 0.90 (0.83-0.97). The association was attenuated and non-significant after adjusting for known prognostic factors. Our findings show that common genetic variants influence the pathological subtype of breast cancer and provide further support for the hypothesis that ER-positive and ER-negative disease are biologically distinct. Understanding the etiologic heterogeneity of breast cancer may ultimately result in improvements in prevention, early detection, and treatment.
  • Item
    Thumbnail Image
    Breast Cancer Risk and 6q22.33: Combined Results from Breast Cancer Association Consortium and Consortium of Investigators on Modifiers of BRCA1/2
    Kirchhoff, T ; Gaudet, MM ; Antoniou, AC ; McGuffog, L ; Humphreys, MK ; Dunning, AM ; Bojesen, SE ; Nordestgaard, BG ; Flyger, H ; Kang, D ; Yoo, K-Y ; Noh, D-Y ; Ahn, S-H ; Dork, T ; Schuermann, P ; Karstens, JH ; Hillemanns, P ; Couch, FJ ; Olson, J ; Vachon, C ; Wang, X ; Cox, A ; Brock, I ; Elliott, G ; Reed, MWR ; Burwinkel, B ; Meindl, A ; Brauch, H ; Hamann, U ; Ko, Y-D ; Broeks, A ; Schmidt, MK ; Van 't Veer, LJ ; Braaf, LM ; Johnson, N ; Fletcher, O ; Gibson, L ; Peto, J ; Turnbull, C ; Seal, S ; Renwick, A ; Rahman, N ; Wu, P-E ; Yu, J-C ; Hsiung, C-N ; Shen, C-Y ; Southey, MC ; Hopper, JL ; Hammet, F ; Van Dorpe, T ; Dieudonne, A-S ; Hatse, S ; Lambrechts, D ; Andrulis, IL ; Bogdanova, N ; Antonenkova, N ; Rogov, JI ; Prokofieva, D ; Bermisheva, M ; Khusnutdinova, E ; van Asperen, CJ ; Tollenaar, RAEM ; Hooning, MJ ; Devilee, P ; Margolin, S ; Lindblom, A ; Milne, RL ; Ignacio Arias, J ; Pilar Zamora, M ; Benitez, J ; Severi, G ; Baglietto, L ; Giles, GG ; Spurdle, AB ; Beesley, J ; Chen, X ; Holland, H ; Healey, S ; Wang-Gohrke, S ; Chang-Claude, J ; Mannermaa, A ; Kosma, V-M ; Kauppinen, J ; Kataja, V ; Agnarsson, BA ; Caligo, MA ; Godwin, AK ; Nevanlinna, H ; Heikkinen, T ; Fredericksen, Z ; Lindor, N ; Nathanson, KL ; Domchek, SM ; Loman, N ; Karlsson, P ; Askmalm, MS ; Melin, B ; von Wachenfeldt, A ; Hogervorst, FBL ; Verheus, M ; Rookus, MA ; Seynaeve, C ; Oldenburg, RA ; Ligtenberg, MJ ; Ausems, MGEM ; Aalfs, CM ; Gille, HJP ; Wijnen, JT ; Garcia, EBG ; Peock, S ; Cook, M ; Oliver, CT ; Frost, D ; Luccarini, C ; Pichert, G ; Davidson, R ; Chu, C ; Eccles, D ; Ong, K-R ; Cook, J ; Douglas, F ; Hodgson, S ; Evans, DG ; Eeles, R ; Gold, B ; Pharoah, PDP ; Offit, K ; Chenevix-Trench, G ; Easton, DF ; Prokunina-Olsson, L (PUBLIC LIBRARY SCIENCE, 2012-06-29)
    Recently, a locus on chromosome 6q22.33 (rs2180341) was reported to be associated with increased breast cancer risk in the Ashkenazi Jewish (AJ) population, and this association was also observed in populations of non-AJ European ancestry. In the present study, we performed a large replication analysis of rs2180341 using data from 31,428 invasive breast cancer cases and 34,700 controls collected from 25 studies in the Breast Cancer Association Consortium (BCAC). In addition, we evaluated whether rs2180341 modifies breast cancer risk in 3,361 BRCA1 and 2,020 BRCA2 carriers from 11 centers in the Consortium of Investigators of Modifiers of BRCA1/2 (CIMBA). Based on the BCAC data from women of European ancestry, we found evidence for a weak association with breast cancer risk for rs2180341 (per-allele odds ratio (OR) = 1.03, 95% CI 1.00-1.06, p = 0.023). There was evidence for heterogeneity in the ORs among studies (I(2) = 49.3%; p = <0.004). In CIMBA, we observed an inverse association with the minor allele of rs2180341 and breast cancer risk in BRCA1 mutation carriers (per-allele OR = 0.89, 95%CI 0.80-1.00, p = 0.048), indicating a potential protective effect of this allele. These data suggest that that 6q22.33 confers a weak effect on breast cancer risk.
  • Item
    Thumbnail Image
    PREDICT Plus: development and validation of a prognostic model for early breast cancer that includes HER2
    Wishart, GC ; Bajdik, CD ; Dicks, E ; Provenzano, E ; Schmidt, MK ; Sherman, M ; Greenberg, DC ; Green, AR ; Gelmon, KA ; Kosma, V-M ; Olson, JE ; Beckmann, MW ; Winqvist, R ; Cross, SS ; Severi, G ; Huntsman, D ; Pylkas, K ; Ellis, I ; Nielsen, TO ; Giles, G ; Blomqvist, C ; Fasching, PA ; Couch, FJ ; Rakha, E ; Foulkes, WD ; Blows, FM ; Begin, LR ; van't Veer, LJ ; Southey, M ; Nevanlinna, H ; Mannermaa, A ; Cox, A ; Cheang, M ; Baglietto, L ; Caldas, C ; Garcia-Closas, M ; Pharoah, PDP (NATURE PUBLISHING GROUP, 2012-08-21)
    BACKGROUND: Predict (www.predict.nhs.uk) is an online, breast cancer prognostication and treatment benefit tool. The aim of this study was to incorporate the prognostic effect of HER2 status in a new version (Predict+), and to compare its performance with the original Predict and Adjuvant!. METHODS: The prognostic effect of HER2 status was based on an analysis of data from 10 179 breast cancer patients from 14 studies in the Breast Cancer Association Consortium. The hazard ratio estimates were incorporated into Predict. The validation study was based on 1653 patients with early-stage invasive breast cancer identified from the British Columbia Breast Cancer Outcomes Unit. Predicted overall survival (OS) and breast cancer-specific survival (BCSS) for Predict+, Predict and Adjuvant! were compared with observed outcomes. RESULTS: All three models performed well for both OS and BCSS. Both Predict models provided better BCSS estimates than Adjuvant!. In the subset of patients with HER2-positive tumours, Predict+ performed substantially better than the other two models for both OS and BCSS. CONCLUSION: Predict+ is the first clinical breast cancer prognostication tool that includes tumour HER2 status. Use of the model might lead to more accurate absolute treatment benefit predictions for individual patients.
  • Item
    Thumbnail Image
    Assessing interactions between the associations of common genetic susceptibility variants, reproductive history and body mass index with breast cancer risk in the breast cancer association consortium: a combined case-control study
    Milne, RL ; Gaudet, MM ; Spurdle, AB ; Fasching, PA ; Couch, FJ ; Benitez, J ; Arias Perez, JI ; Pilar Zamora, M ; Malats, N ; dos Santos Silva, I ; Gibson, LJ ; Fletcher, O ; Johnson, N ; Anton-Culver, H ; Ziogas, A ; Figueroa, J ; Brinton, L ; Sherman, ME ; Lissowska, J ; Hopper, JL ; Dite, GS ; Apicella, C ; Southey, MC ; Sigurdson, AJ ; Linet, MS ; Schonfeld, SJ ; Freedman, DM ; Mannermaa, A ; Kosma, V-M ; Kataja, V ; Auvinen, P ; Andrulis, IL ; Glendon, G ; Knight, JA ; Weerasooriya, N ; Cox, A ; Reed, MWR ; Cross, SS ; Dunning, AM ; Ahmed, S ; Shah, M ; Brauch, H ; Ko, Y-D ; Bruening, T ; Lambrechts, D ; Reumers, J ; Smeets, A ; Wang-Gohrke, S ; Hall, P ; Czene, K ; Liu, J ; Irwanto, AK ; Chenevix-Trench, G ; Holland, H ; Giles, GG ; Baglietto, L ; Severi, G ; Bojensen, SE ; Nordestgaard, BG ; Flyger, H ; John, EM ; West, DW ; Whittemore, AS ; Vachon, C ; Olson, JE ; Fredericksen, Z ; Kosel, M ; Hein, R ; Vrieling, A ; Flesch-Janys, D ; Heinz, J ; Beckmann, MW ; Heusinger, K ; Ekici, AB ; Haeberle, L ; Humphreys, MK ; Morrison, J ; Easton, DF ; Pharoah, PD ; Garcia-Closas, M ; Goode, EL ; Chang-Claude, J (BIOMED CENTRAL LTD, 2010)
    INTRODUCTION: Several common breast cancer genetic susceptibility variants have recently been identified. We aimed to determine how these variants combine with a subset of other known risk factors to influence breast cancer risk in white women of European ancestry using case-control studies participating in the Breast Cancer Association Consortium. METHODS: We evaluated two-way interactions between each of age at menarche, ever having had a live birth, number of live births, age at first birth and body mass index (BMI) and each of 12 single nucleotide polymorphisms (SNPs) (10q26-rs2981582 (FGFR2), 8q24-rs13281615, 11p15-rs3817198 (LSP1), 5q11-rs889312 (MAP3K1), 16q12-rs3803662 (TOX3), 2q35-rs13387042, 5p12-rs10941679 (MRPS30), 17q23-rs6504950 (COX11), 3p24-rs4973768 (SLC4A7), CASP8-rs17468277, TGFB1-rs1982073 and ESR1-rs3020314). Interactions were tested for by fitting logistic regression models including per-allele and linear trend main effects for SNPs and risk factors, respectively, and single-parameter interaction terms for linear departure from independent multiplicative effects. RESULTS: These analyses were applied to data for up to 26,349 invasive breast cancer cases and up to 32,208 controls from 21 case-control studies. No statistical evidence of interaction was observed beyond that expected by chance. Analyses were repeated using data from 11 population-based studies, and results were very similar. CONCLUSIONS: The relative risks for breast cancer associated with the common susceptibility variants identified to date do not appear to vary across women with different reproductive histories or body mass index (BMI). The assumption of multiplicative combined effects for these established genetic and other risk factors in risk prediction models appears justified.
  • Item
    Thumbnail Image
    A PALB2 mutation associated with high risk of breast cancer
    Southey, MC ; Teo, ZL ; Dowty, JG ; Odefrey, FA ; Park, DJ ; Tischkowitz, M ; Sabbaghian, N ; Apicella, C ; Byrnes, GB ; Winship, I ; Baglietto, L ; Giles, GG ; Goldgar, DE ; Foulkes, WD ; Hopper, JL (BMC, 2010)
    NTRODUCTION: As a group, women who carry germline mutations in partner and localizer of breast cancer 2 susceptibility protein (PALB2) are at increased risk of breast cancer. Little is known about by how much or whether risk differs by mutation or family history, owing to the paucity of studies of cases unselected for family history. METHODS: We screened 1,403 case probands for PALB2 mutations in a population-based study of Australian women with invasive breast cancer stratified by age at onset. The age-specific risk of breast cancer was estimated from the cancer histories of first- and second-degree relatives of mutation-carrying probands using a modified segregation analysis that included a polygenic modifier and was conditioned on the carrier case proband. Further screening for PALB2 c.3113G > A (W1038X) was conducted for 779 families with multiple cases of breast cancer ascertained through family cancer clinics in Australia and New Zealand and 764 population-based controls. RESULTS: We found five independent case probands in the population-based sample with the protein-truncating mutation PALB2 c.3113G > A (W1038X); 2 of 695 were diagnosed before age 40 years and 3 of 708 were diagnosed when between ages 40 and 59 years. Both of the two early-onset carrier case probands had very strong family histories of breast cancer. Further testing found that the mutation segregated with breast cancer in these families. No c.3113G > A (W1038X) carriers were found in 764 population-based unaffected controls. The hazard ratio was estimated to be 30.1 (95% confidence interval (CI), 7.5 to 120; P < 0.0001), and the corresponding cumulative risk estimates were 49% (95% CI, 15 to 93) to age 50 and 91% (95% CI, 44 to 100) to age 70. We found another eight families carrying this mutation in 779 families with multiple cases of breast cancer ascertained through family cancer clinics. CONCLUSIONS: The PALB2 c.3113G > A mutation appears to be associated with substantial risks of breast cancer that are of clinical relevance.
  • Item
    Thumbnail Image
    Comparison of 6q25 Breast Cancer Hits from Asian and European Genome Wide Association Studies in the Breast Cancer Association Consortium (BCAC)
    Hein, R ; Maranian, M ; Hopper, JL ; Kapuscinski, MK ; Southey, MC ; Park, DJ ; Schmidt, MK ; Broeks, A ; Hogervorst, FBL ; Bueno-de-Mesquit, HB ; Muir, KR ; Lophatananon, A ; Rattanamongkongul, S ; Puttawibul, P ; Fasching, PA ; Hein, A ; Ekici, AB ; Beckmann, MW ; Fletcher, O ; Johnson, N ; Silva, IDS ; Peto, J ; Sawyer, E ; Tomlinson, I ; Kerin, M ; Miller, N ; Marmee, F ; Schneeweiss, A ; Sohn, C ; Burwinkel, B ; Guenel, P ; Cordina-Duverger, E ; Menegaux, F ; Truong, T ; Bojesen, SE ; Nordestgaard, BG ; Flyger, H ; Milne, RL ; Arias Perez, JI ; Pilar Zamora, M ; Benitez, J ; Anton-Culver, H ; Ziogas, A ; Bernstein, L ; Clarke, CA ; Brenner, H ; Mueller, H ; Arndt, V ; Stegmaier, C ; Rahman, N ; Seal, S ; Turnbull, C ; Renwick, A ; Meindl, A ; Schott, S ; Bartram, CR ; Schmutzler, RK ; Brauch, H ; Hamann, U ; Ko, Y-D ; Wang-Gohrke, S ; Doerk, T ; Schuermann, P ; Karstens, JH ; Hillemanns, P ; Nevanlinna, H ; Heikkinen, T ; Aittomaki, K ; Blomqvist, C ; Bogdanova, NV ; Zalutsky, IV ; Antonenkova, NN ; Bermisheva, M ; Prokovieva, D ; Farahtdinova, A ; Khusnutdinova, E ; Lindblom, A ; Margolin, S ; Mannermaa, A ; Kataja, V ; Kosma, V-M ; Hartikainen, J ; Chen, X ; Beesley, J ; Lambrechts, D ; Zhao, H ; Neven, P ; Wildiers, H ; Nickels, S ; Flesch-Janys, D ; Radice, P ; Peterlongo, P ; Manoukian, S ; Barile, M ; Couch, FJ ; Olson, JE ; Wang, X ; Fredericksen, Z ; Giles, GG ; Baglietto, L ; McLean, CA ; Severi, G ; Offit, K ; Robson, M ; Gaudet, MM ; Vijai, J ; Alnaes, GG ; Kristensen, V ; Borresen-Dale, A-L ; John, EM ; Miron, A ; Winqvist, R ; Pylkas, K ; Jukkola-Vuorinen, A ; Grip, M ; Andrulis, IL ; Knight, JA ; Glendon, G ; Mulligan, AM ; Figueroa, JD ; Garcia-Closas, M ; Lissowska, J ; Sherman, ME ; Hooning, M ; Martens, JWM ; Seynaeve, C ; Collee, M ; Hall, P ; Humpreys, K ; Czene, K ; Liu, J ; Cox, A ; Brock, IW ; Cross, SS ; Reed, MWR ; Ahmed, S ; Ghoussaini, M ; Pharoah, PDP ; Kang, D ; Yoo, K-Y ; Noh, D-Y ; Jakubowska, A ; Jaworska, K ; Durda, K ; Zlowocka, E ; Sangrajrang, S ; Gaborieau, V ; Brennan, P ; McKay, J ; Shen, C-Y ; Yu, J-C ; Hsu, H-M ; Hou, M-F ; Orr, N ; Schoemaker, M ; Ashworth, A ; Swerdlow, A ; Trentham-Dietz, A ; Newcomb, PA ; Titus, L ; Egan, KM ; Chenevix-Trench, G ; Antoniou, AC ; Humphreys, MK ; Morrison, J ; Chang-Claude, J ; Easton, DF ; Dunning, AM ; Chan, KYK (PUBLIC LIBRARY SCIENCE, 2012-08-07)
    The 6q25.1 locus was first identified via a genome-wide association study (GWAS) in Chinese women and marked by single nucleotide polymorphism (SNP) rs2046210, approximately 180 Kb upstream of ESR1. There have been conflicting reports about the association of this locus with breast cancer in Europeans, and a GWAS in Europeans identified a different SNP, tagged here by rs12662670. We examined the associations of both SNPs in up to 61,689 cases and 58,822 controls from forty-four studies collaborating in the Breast Cancer Association Consortium, of which four studies were of Asian and 39 of European descent. Logistic regression was used to estimate odds ratios (OR) and 95% confidence intervals (CI). Case-only analyses were used to compare SNP effects in Estrogen Receptor positive (ER+) versus negative (ER-) tumours. Models including both SNPs were fitted to investigate whether the SNP effects were independent. Both SNPs are significantly associated with breast cancer risk in both ethnic groups. Per-allele ORs are higher in Asian than in European studies [rs2046210: OR (A/G) = 1.36 (95% CI 1.26-1.48), p = 7.6 × 10(-14) in Asians and 1.09 (95% CI 1.07-1.11), p = 6.8 × 10(-18) in Europeans. rs12662670: OR (G/T) = 1.29 (95% CI 1.19-1.41), p = 1.2 × 10(-9) in Asians and 1.12 (95% CI 1.08-1.17), p = 3.8 × 10(-9) in Europeans]. SNP rs2046210 is associated with a significantly greater risk of ER- than ER+ tumours in Europeans [OR (ER-) = 1.20 (95% CI 1.15-1.25), p = 1.8 × 10(-17) versus OR (ER+) = 1.07 (95% CI 1.04-1.1), p = 1.3 × 10(-7), p(heterogeneity) = 5.1 × 10(-6)]. In these Asian studies, by contrast, there is no clear evidence of a differential association by tumour receptor status. Each SNP is associated with risk after adjustment for the other SNP. These results suggest the presence of two variants at 6q25.1 each independently associated with breast cancer risk in Asians and in Europeans. Of these two, the one tagged by rs2046210 is associated with a greater risk of ER- tumours.