Common breast cancer susceptibility variants in LSP1 and RAD51L1 are associated with mammographic density measures that predict breast cancer risk.

نویسندگان

  • Celine M Vachon
  • Christopher G Scott
  • Peter A Fasching
  • Per Hall
  • Rulla M Tamimi
  • Jingmei Li
  • Jennifer Stone
  • Carmel Apicella
  • Fabrice Odefrey
  • Gretchen L Gierach
  • Sebastian M Jud
  • Katharina Heusinger
  • Matthias W Beckmann
  • Marina Pollan
  • Pablo Fernández-Navarro
  • Anna Gonzalez-Neira
  • Javier Benitez
  • Carla H van Gils
  • Mariëtte Lokate
  • N Charlotte Onland-Moret
  • Petra H M Peeters
  • Judith Brown
  • Jean Leyland
  • Jajini S Varghese
  • Douglas F Easton
  • Deborah J Thompson
  • Robert N Luben
  • Ruth M L Warren
  • Nicholas J Wareham
  • Ruth J F Loos
  • Kay-Tee Khaw
  • Giske Ursin
  • Eunjung Lee
  • Simon A Gayther
  • Susan J Ramus
  • Rosalind A Eeles
  • Martin O Leach
  • Gek Kwan-Lim
  • Fergus J Couch
  • Graham G Giles
  • Laura Baglietto
  • Kavitha Krishnan
  • Melissa C Southey
  • Loic Le Marchand
  • Laurence N Kolonel
  • Christy Woolcott
  • Gertraud Maskarinec
  • Christopher A Haiman
  • Kate Walker
  • Nichola Johnson
  • Valeria A McCormack
  • Margarethe Biong
  • Grethe I G Alnaes
  • Inger Torhild Gram
  • Vessela N Kristensen
  • Anne-Lise Børresen-Dale
  • Sara Lindström
  • Susan E Hankinson
  • David J Hunter
  • Irene L Andrulis
  • Julia A Knight
  • Norman F Boyd
  • Jonine D Figuero
  • Jolanta Lissowska
  • Ewa Wesolowska
  • Beata Peplonska
  • Agnieszka Bukowska
  • Edyta Reszka
  • JianJun Liu
  • Louise Eriksson
  • Kamila Czene
  • Tina Audley
  • Anna H Wu
  • V Shane Pankratz
  • John L Hopper
  • Isabel dos-Santos-Silva
چکیده

BACKGROUND Mammographic density adjusted for age and body mass index (BMI) is a heritable marker of breast cancer susceptibility. Little is known about the biologic mechanisms underlying the association between mammographic density and breast cancer risk. We examined whether common low-penetrance breast cancer susceptibility variants contribute to interindividual differences in mammographic density measures. METHODS We established an international consortium (DENSNP) of 19 studies from 10 countries, comprising 16,895 Caucasian women, to conduct a pooled cross-sectional analysis of common breast cancer susceptibility variants in 14 independent loci and mammographic density measures. Dense and nondense areas, and percent density, were measured using interactive-thresholding techniques. Mixed linear models were used to assess the association between genetic variants and the square roots of mammographic density measures adjusted for study, age, case status, BMI, and menopausal status. RESULTS Consistent with their breast cancer associations, the C-allele of rs3817198 in LSP1 was positively associated with both adjusted dense area (P = 0.00005) and adjusted percent density (P = 0.001), whereas the A-allele of rs10483813 in RAD51L1 was inversely associated with adjusted percent density (P = 0.003), but not with adjusted dense area (P = 0.07). CONCLUSION We identified two common breast cancer susceptibility variants associated with mammographic measures of radiodense tissue in the breast gland. IMPACT We examined the association of 14 established breast cancer susceptibility loci with mammographic density phenotypes within a large genetic consortium and identified two breast cancer susceptibility variants, LSP1-rs3817198 and RAD51L1-rs10483813, associated with mammographic measures and in the same direction as the breast cancer association.

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Common genetic variants associated with breast cancer and mammographic density measures that predict disease.

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عنوان ژورنال:
  • Cancer epidemiology, biomarkers & prevention : a publication of the American Association for Cancer Research, cosponsored by the American Society of Preventive Oncology

دوره 21 7  شماره 

صفحات  -

تاریخ انتشار 2012