Identification of 31 loci for mammographic density phenotypes and their associations with breast cancer risk

Achacoso, Ninah; Acton, Luana; Alexeeff, Stacey E.; Easton, Douglas F.; Graff, Rebecca E.; Habel, Laurel A.; Jorgenson, Eric; Klein, Robert J.; Liang, Rhea Y.; Lipson, Jafi A.; McBride, Russell B.; McGuire, Valerie; Risch, Neil; Rothstein, Joseph H.; Rubin, Daniel L.; Sakoda, Lori C.; Schaefer, Catherine; Sieh, Weiva; Whittemore, Alice S.; Yaffe, Martin J.

Identification of 31 loci for mammographic density phenotypes and their associations with breast cancer risk

Authors: Ninah Achacoso
Luana Acton
Stacey E. Alexeeff
Douglas F. Easton
Rebecca E. Graff
Laurel A. Habel
Eric Jorgenson
Robert J. Klein
Rhea Y. Liang
Jafi A. Lipson
Russell B. McBride
Valerie McGuire
Neil Risch
Joseph H. Rothstein
Daniel L. Rubin
Lori C. Sakoda
Catherine Schaefer
Weiva Sieh
Alice S. Whittemore
Martin J. Yaffe
Publication date: 1 October 2020
Publisher: Nature Communications
Doi

Abstract

Funder: U.S. Department of Health & Human Services | National Institutes of Health (NIH)Abstract: Mammographic density (MD) phenotypes are strongly associated with breast cancer risk and highly heritable. In this GWAS meta-analysis of 24,192 women, we identify 31 MD loci at P < 5 × 10−8, tripling the number known to 46. Seventeen identified MD loci also are associated with breast cancer risk in an independent meta-analysis (P < 0.05). Mendelian randomization analyses show that genetic estimates of dense area (DA), nondense area (NDA), and percent density (PD) are all significantly associated with breast cancer risk (P < 0.05). Pathway analyses reveal distinct biological processes involving DA, NDA and PD loci. These findings provide additional insights into the genetic basis of MD phenotypes and their associations with breast cancer risk