Sequence variants of estrogen receptor β and risk of prostate cancer in the national cancer institute breast and prostate cancer cohort consortium

被引：25

作者：

Chen, Yen-Ching

Kraft, Peter

Bretsky, Philip

Ketkar, Shamika

Hunter, David J.

Albanes, Demetrius

Altshuler, David

Andriole, Gerald

Berg, Christine D.

Boeing, Heiner

Burtt, Noel

Bueno-de-Mesquita, Bas

Cann, Howard

Canzian, Federico

Chanock, Stephen

Dunning, Alison

Feigelson, Heather S.

Freedman, Matthew

Gaziano, J. Michael

Giovannucci, Edward

Sanchez, Maria-Jose

Haiman, Christopher A.

Hallmans, Goran

Hayes, Richard B.

Henderson, Brian E.

Hirschhorn, Joel

Kaaks, Rudolf

Key, Timothy J.

Kolonel, Laurence N.

LeMarchand, Loic

Ma, Jing

Overvad, Kim

Palli, Domenico

Pharaoh, Paul

Pike, Malcolm

Riboli, Eliot

Rodriguez, Carmen

Setiawan, V. Wendy

Stampfer, Meir

Stram, Daniel O.

Thomas, Gilles

Thun, Michael J.

Travis, Ruth C.

Virtamo, Jarmo

Trichopouiou, Antonia

Wacholder, Sholom

Weinstein, Stephanie J.

机构：

[1] Channing Labs, Boston, MA 02115 USA

[2] Brigham & Womens Hosp, Dept Med, Div Aging, Boston, MA 02115 USA

[3] Harvard Univ, Sch Med, Program Mol & Genet Epidemiol, Cambridge, MA 02138 USA

[4] Harvard Univ, Sch Publ Hlth, Dept Nutr, Boston, MA 02115 USA

[5] Harvard Univ, Sch Publ Hlth, Dept Epidemiol, Boston, MA 02115 USA

[6] Natl Taiwan Univ, Coll Publ Hlth, Grad Inst Epidemiol, Res Ctr Genes Environm & Human Hlth, Taipei 10764, Taiwan

[7] Cedars Sinai Med Ctr, Dept Internal Med, Los Angeles, CA 90048 USA

[8] Univ So Calif, Keck Sch Med, Dept Prevent Med, Los Angeles, CA USA

[9] Washington Univ, St Louis, MO USA

[10] Natl Canc Inst, Div Canc Epidemiol & Genet, Rockville, MD USA

[11] Broad Inst Harvard, Cambridge, MA 02139 USA

[12] MIT, Whitehead Inst Biomed Res, Cambridge, MA USA

[13] Natl Canc Inst, Div Canc Prevent, Bethesda, MD USA

[14] German Inst Human Nutr, Dept Epidemiol, Potsdam, Germany

[15] Natl Inst Publ Hlth & Environm, Ctr Nutr & Hlth, NL-3720 BA Bilthoven, Netherlands

[16] Ctr Etud Polymorphisme Humain, Fdn Jean Dausset, F-75010 Paris, France

[17] Genet Susceptibil Grp, Lyon, France

[18] IARC, Unit Nutr & Canc, Lyon, France

[19] Natl Canc Inst, Core Genotyping Facil, Gaithersburg, MD USA

[20] Univ Cambridge, Dept Oncol, Cambridge, England

[21] Amer Canc Soc, Natl Home Off, Dept Epidemiol & Surveillance Res, Atlanta, GA 30329 USA

[22] Andalusian Sch Publ Hlth, Granada, Spain

[23] Umea Univ, Dept Publ Hlth & Clin Med, Umea, Sweden

[24] German Canc Res Ctr, Div Canc Epidemiol, Heidelberg, Germany

[25] Canc Res, Epidemiol Unit, Oxford, England

[26] Univ Hawaii, Canc Res Ctr, Honolulu, HI 96813 USA

[27] Aarhus Univ Hosp, Aalborg Hosp, Dept Clin Epidemiol, Aalborg, Denmark

[28] CSPO Sci Inst Tuscany, Mol & Nutr Epidemiol Unit, Florence, Italy

[29] Natl Publ Hlth Inst, Canc Prevent Unit, Helsinki, Finland

[30] Univ Athens, Sch Med, Dept Hyg & Epidemiol, GR-11527 Athens, Greece

来源：

CANCER EPIDEMIOLOGY BIOMARKERS & PREVENTION | 2007年 / 16卷 / 10期

关键词：

D O I：

10.1158/1055-9965.EPI-07-0431

中图分类号：

R73 [肿瘤学];

学科分类号：

100214 ;

摘要：

Background: Estrogen receptor beta (ESR2) may play a role in modulating prostate carcirtogenesis through the regulation of genes related to cell proliferation and apoptosis. Methods: We conducted nested case-control studies in the Breast and Prostate Cancer Cohort Consortium (BPC3) that pooled 8,323 prostate cancer cases and 9,412 controls from seven cohorts. Whites were the predominant ethnic group. We characterized genetic variation in ESR2 by resequencing exons in 190 breast and prostate cancer cases and genotyping a dense set of single nucleotide polymorphisms (SNP) spanning the locus in a multiethnic panel of 349 cancer-free subjects. We selected four haplotype-tagging SNPs (htSNP) to capture common ESR2 variation in Whites; these htSNPs were then genotyped in all cohorts. Conditional logistic regression models were used to assess the association between sequence variants of ESR2 and the risk of prostate cancer. We also investigated the effect modification by age, body mass index, and family history, as well as the association between sequence variants of ESR2 and advanced-stage (>= T3b, N-1, or M-1) and high-grade (Gleason sum >= 8) prostate cancer, respectively. Results: The four tag SNPs in ESR2 were not significantly associated with prostate cancer risk, individually. The global test for the influence of any haplotype on the risk of prostate cancer was not significant (P = 0.31). However, we observed that men carrying two copies of one of the variant haplotypes (TACC) had a 1.46-fold increased risk of prostate cancer (99% confidence interval, 1.06-2.01) compared with men carrying zero copies of this variant haplotype. No SNPs or haplotypes were associated with advanced stage or high grade of prostate cancer. Conclusion: In our analysis focused on genetic variation common in Whites, we observed little evidence for any substantial association of inherited variation in ESR2 with risk of prostate cancer. A nominally significant (P < 0.01) association between the TACC haplotype and prostate cancer risk under the recessive model could be a chance finding and, in any event, would seem to contribute only slightly to the overall burden of prostate cancer.

引用

页码：1973 / 1981

页数：9

共 40 条

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