ESR1 promoter hypermethylation does not predict atypia in RPFNA nor persistent atypia after 12 months tamoxifen chemoprevention

Julie H. Ostrander; Joseph C. Baker; Siya Lem; Gloria Broadwater; Gregory R. Bean; Nicholas C. D'Amato; Vanessa K. Goldenberg; Craig Rowell; Catherine Ibarra-Drendall; Tracey Grant; Patrick G. Pilie; Shauna N. Vasilatos; Michelle M. Troch; Victoria Scott; Lee G. Wilke; Carolyn Paisie; Sarah M. Rabiner; Alejandro Torres-Hernandez; Carola M. Zalles; Victoria L. Seewaldt

doi:10.1158/1055-9965.EPI-07-2696

ESR1 promoter hypermethylation does not predict atypia in RPFNA nor persistent atypia after 12 months tamoxifen chemoprevention

Julie H. Ostrander, Joseph C. Baker, Siya Lem, Gloria Broadwater, Gregory R. Bean, Nicholas C. D'Amato, Vanessa K. Goldenberg, Craig Rowell, Catherine Ibarra-Drendall, Tracey Grant, Patrick G. Pilie, Shauna N. Vasilatos, Michelle M. Troch, Victoria Scott, Lee G. Wilke, Carolyn Paisie, Sarah M. Rabiner, Alejandro Torres-Hernandez, Carola M. Zalles, Victoria L. Seewaldt

Medicine - Hematology, Oncology, Transplant

Research output: Contribution to journal › Article › peer-review

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Abstract

Purpose: Currently, we lack biomarkers to predict whether high-risk women with mammary atypia will respond to tamoxifen chemoprevention. Experimental Design: Thirty-four women with cytologic mammary atypia from the Duke University High-Risk clinic were offered tamoxifen chemoprevention. We tested whether ESR1 promoter hypermethylation and/or estrogen receptor (ER) protein expression by immunohistochemistry predicted persistent atypia in 18 women who were treated with tamoxifen for 12 months and in 16 untreated controls. Results: We observed a statistically significant decrease in the Masood score of women on tamoxifen chemoprevention for 12 months compared with controlwomen. This was a significant interaction effect of time (0, 6, and 12 months) and treatment group (tamoxifen versus control) P = 0.0007. However, neither ESR1 promoter hypermethylation nor low ER expression predicted persistent atypia in Random Periareolar Fine Needle Aspiration after 12 months tamoxifen prevention. Conclusions: Results from this single institution pilot study provide evidence that, unlike for invasive breast cancer, ESR1 promoter hypermethylation and/or low ER expression is not a reliable marker of tamoxifen-resistant atypia.

Original language	English (US)
Pages (from-to)	1884-1890
Number of pages	7
Journal	Cancer Epidemiology Biomarkers and Prevention
Volume	17
Issue number	8
DOIs	https://doi.org/10.1158/1055-9965.EPI-07-2696
State	Published - Aug 2008

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Ostrander, J. H., Baker, J. C., Lem, S., Broadwater, G., Bean, G. R., D'Amato, N. C., Goldenberg, V. K., Rowell, C., Ibarra-Drendall, C., Grant, T., Pilie, P. G., Vasilatos, S. N., Troch, M. M., Scott, V., Wilke, L. G., Paisie, C., Rabiner, S. M., Torres-Hernandez, A., Zalles, C. M., & Seewaldt, V. L. (2008). ESR1 promoter hypermethylation does not predict atypia in RPFNA nor persistent atypia after 12 months tamoxifen chemoprevention. Cancer Epidemiology Biomarkers and Prevention, 17(8), 1884-1890. https://doi.org/10.1158/1055-9965.EPI-07-2696

Ostrander, JH, Baker, JC, Lem, S, Broadwater, G, Bean, GR, D'Amato, NC, Goldenberg, VK, Rowell, C, Ibarra-Drendall, C, Grant, T, Pilie, PG, Vasilatos, SN, Troch, MM, Scott, V, Wilke, LG, Paisie, C, Rabiner, SM, Torres-Hernandez, A, Zalles, CM & Seewaldt, VL 2008, 'ESR1 promoter hypermethylation does not predict atypia in RPFNA nor persistent atypia after 12 months tamoxifen chemoprevention', Cancer Epidemiology Biomarkers and Prevention, vol. 17, no. 8, pp. 1884-1890. https://doi.org/10.1158/1055-9965.EPI-07-2696

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title = "ESR1 promoter hypermethylation does not predict atypia in RPFNA nor persistent atypia after 12 months tamoxifen chemoprevention",

abstract = "Purpose: Currently, we lack biomarkers to predict whether high-risk women with mammary atypia will respond to tamoxifen chemoprevention. Experimental Design: Thirty-four women with cytologic mammary atypia from the Duke University High-Risk clinic were offered tamoxifen chemoprevention. We tested whether ESR1 promoter hypermethylation and/or estrogen receptor (ER) protein expression by immunohistochemistry predicted persistent atypia in 18 women who were treated with tamoxifen for 12 months and in 16 untreated controls. Results: We observed a statistically significant decrease in the Masood score of women on tamoxifen chemoprevention for 12 months compared with controlwomen. This was a significant interaction effect of time (0, 6, and 12 months) and treatment group (tamoxifen versus control) P = 0.0007. However, neither ESR1 promoter hypermethylation nor low ER expression predicted persistent atypia in Random Periareolar Fine Needle Aspiration after 12 months tamoxifen prevention. Conclusions: Results from this single institution pilot study provide evidence that, unlike for invasive breast cancer, ESR1 promoter hypermethylation and/or low ER expression is not a reliable marker of tamoxifen-resistant atypia.",

author = "Ostrander, {Julie H.} and Baker, {Joseph C.} and Siya Lem and Gloria Broadwater and Bean, {Gregory R.} and D'Amato, {Nicholas C.} and Goldenberg, {Vanessa K.} and Craig Rowell and Catherine Ibarra-Drendall and Tracey Grant and Pilie, {Patrick G.} and Vasilatos, {Shauna N.} and Troch, {Michelle M.} and Victoria Scott and Wilke, {Lee G.} and Carolyn Paisie and Rabiner, {Sarah M.} and Alejandro Torres-Hernandez and Zalles, {Carola M.} and Seewaldt, {Victoria L.}",

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doi = "10.1158/1055-9965.EPI-07-2696",

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T1 - ESR1 promoter hypermethylation does not predict atypia in RPFNA nor persistent atypia after 12 months tamoxifen chemoprevention

AU - Ostrander, Julie H.

AU - Baker, Joseph C.

AU - Lem, Siya

AU - Broadwater, Gloria

AU - Bean, Gregory R.

AU - D'Amato, Nicholas C.

AU - Goldenberg, Vanessa K.

AU - Rowell, Craig

AU - Ibarra-Drendall, Catherine

AU - Grant, Tracey

AU - Pilie, Patrick G.

AU - Vasilatos, Shauna N.

AU - Troch, Michelle M.

AU - Scott, Victoria

AU - Wilke, Lee G.

AU - Paisie, Carolyn

AU - Rabiner, Sarah M.

AU - Torres-Hernandez, Alejandro

AU - Zalles, Carola M.

AU - Seewaldt, Victoria L.

PY - 2008/8

Y1 - 2008/8

N2 - Purpose: Currently, we lack biomarkers to predict whether high-risk women with mammary atypia will respond to tamoxifen chemoprevention. Experimental Design: Thirty-four women with cytologic mammary atypia from the Duke University High-Risk clinic were offered tamoxifen chemoprevention. We tested whether ESR1 promoter hypermethylation and/or estrogen receptor (ER) protein expression by immunohistochemistry predicted persistent atypia in 18 women who were treated with tamoxifen for 12 months and in 16 untreated controls. Results: We observed a statistically significant decrease in the Masood score of women on tamoxifen chemoprevention for 12 months compared with controlwomen. This was a significant interaction effect of time (0, 6, and 12 months) and treatment group (tamoxifen versus control) P = 0.0007. However, neither ESR1 promoter hypermethylation nor low ER expression predicted persistent atypia in Random Periareolar Fine Needle Aspiration after 12 months tamoxifen prevention. Conclusions: Results from this single institution pilot study provide evidence that, unlike for invasive breast cancer, ESR1 promoter hypermethylation and/or low ER expression is not a reliable marker of tamoxifen-resistant atypia.

AB - Purpose: Currently, we lack biomarkers to predict whether high-risk women with mammary atypia will respond to tamoxifen chemoprevention. Experimental Design: Thirty-four women with cytologic mammary atypia from the Duke University High-Risk clinic were offered tamoxifen chemoprevention. We tested whether ESR1 promoter hypermethylation and/or estrogen receptor (ER) protein expression by immunohistochemistry predicted persistent atypia in 18 women who were treated with tamoxifen for 12 months and in 16 untreated controls. Results: We observed a statistically significant decrease in the Masood score of women on tamoxifen chemoprevention for 12 months compared with controlwomen. This was a significant interaction effect of time (0, 6, and 12 months) and treatment group (tamoxifen versus control) P = 0.0007. However, neither ESR1 promoter hypermethylation nor low ER expression predicted persistent atypia in Random Periareolar Fine Needle Aspiration after 12 months tamoxifen prevention. Conclusions: Results from this single institution pilot study provide evidence that, unlike for invasive breast cancer, ESR1 promoter hypermethylation and/or low ER expression is not a reliable marker of tamoxifen-resistant atypia.

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ESR1 promoter hypermethylation does not predict atypia in RPFNA nor persistent atypia after 12 months tamoxifen chemoprevention

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