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1rarebird · 05-24-2010, 02:54 PM

http://www.surgjournal.com/article/S...392-8/abstract

The reason I decided forego vitamin E for my HFs.
bird

Volume 140, Issue 4, Pages 607-615 (October 2006)

Effect of vitamin E on tamoxifen-treated breast cancer cells

Presented at the 63rd Annual Meeting of the Central Surgical Association, Louisville, Kentucky, March 9-11, 2006.
Elizabeth A. Peralta, MD

, Melita L. Viegas, MD, Somaja Louis, MS, Deborah L. Engle, MS, Gary L. Dunnington, MDReceived 10 February 2006; accepted 10 July 2006. published online 04 September 2006.
Background

Induction of apoptosis by tamoxifen has been postulated to involve oxidative stress. Tamoxifen (TAM) may act on estrogen receptors (ER) located in the plasma membrane. Our hypothesis that supplemental antioxidant vitamin E (α-tocopherol) acts at the plasma membrane to alter the effectiveness of tamoxifen was tested in ER-positive breast cancer cell lines, MCF-7 and T47D.

Methods

Cells were treated in vitro with 20-μM TAM alone and in combination with 10-μM α-tocopherol (AT). Estrogen growth signals were quantified by immunohistochemical staining for the mitogen-activated protein kinase p-ERK. Rapid changes in intracellular calcium were detected in TAM-treated MCF-7 and T-47D cells by fluorescence microscopy of cells loaded with the calcium-sensitive dye Fluo 4AM. Apoptosis was assayed by flow cytometry.

Results

Proliferating cells in normal medium exhibited strong p-ERK staining. Addition of TAM abolished p-ERK staining and caused cell rounding and death. The addition of AT led to the restoration of cell proliferation and p-ERK expression even in the presence of high-dose TAM. Intracellular calcium rapidly increased in MCF-7 and T47D cells upon exposure to TAM, followed by an increase in caspase activation and eventual apoptosis. The increase in intracellular calcium was abolished by the addition of 10μM AT to TAM, and pan-caspase staining decreased at 5 hours from 72% to 41%.

Conclusions

These studies suggest that supplemental vitamin E decreases the inhibitory effect of TAM on the proliferation of ER+ breast cancer cells and eliminates the rapid rise in intracellular calcium that leads to apoptosis stimulated by TAM. The use of vitamin E acetate supplements may be inadvisable for women taking tamoxifen.

05-24-2010, 02:54 PM	#9
1rarebird Senior Member Join Date: Feb 2010 Location: TN Posts: 175	Re: Vitamin E, hot flashes and Tamoxifen http://www.surgjournal.com/article/S...392-8/abstract The reason I decided forego vitamin E for my HFs. bird Volume 140, Issue 4, Pages 607-615 (October 2006) Effect of vitamin E on tamoxifen-treated breast cancer cells Presented at the 63rd Annual Meeting of the Central Surgical Association, Louisville, Kentucky, March 9-11, 2006. Elizabeth A. Peralta, MD , Melita L. Viegas, MD, Somaja Louis, MS, Deborah L. Engle, MS, Gary L. Dunnington, MDReceived 10 February 2006; accepted 10 July 2006. published online 04 September 2006. Background Induction of apoptosis by tamoxifen has been postulated to involve oxidative stress. Tamoxifen (TAM) may act on estrogen receptors (ER) located in the plasma membrane. Our hypothesis that supplemental antioxidant vitamin E (α-tocopherol) acts at the plasma membrane to alter the effectiveness of tamoxifen was tested in ER-positive breast cancer cell lines, MCF-7 and T47D. Methods Cells were treated in vitro with 20-μM TAM alone and in combination with 10-μM α-tocopherol (AT). Estrogen growth signals were quantified by immunohistochemical staining for the mitogen-activated protein kinase p-ERK. Rapid changes in intracellular calcium were detected in TAM-treated MCF-7 and T-47D cells by fluorescence microscopy of cells loaded with the calcium-sensitive dye Fluo 4AM. Apoptosis was assayed by flow cytometry. Results Proliferating cells in normal medium exhibited strong p-ERK staining. Addition of TAM abolished p-ERK staining and caused cell rounding and death. The addition of AT led to the restoration of cell proliferation and p-ERK expression even in the presence of high-dose TAM. Intracellular calcium rapidly increased in MCF-7 and T47D cells upon exposure to TAM, followed by an increase in caspase activation and eventual apoptosis. The increase in intracellular calcium was abolished by the addition of 10μM AT to TAM, and pan-caspase staining decreased at 5 hours from 72% to 41%. Conclusions These studies suggest that supplemental vitamin E decreases the inhibitory effect of TAM on the proliferation of ER+ breast cancer cells and eliminates the rapid rise in intracellular calcium that leads to apoptosis stimulated by TAM. The use of vitamin E acetate supplements may be inadvisable for women taking tamoxifen. __________________ Male Breast Cancer, DX 5/15/09, IDC, STAGE 1, 1.7 cm, HER2+++, ER+(95%)/PR+(75%), Ki67 40%, grade 3, 0/5 nodes, TX: mastectomy, TCH finished 7/19/10, radiation 6 wks., Tamoxifen on going, bisphosphonate 24 mos.