Tanshinones inhibit the growth of breast cancer cells through epigenetic modification of Aurora A expression and function.

Tanshinones inhibit the growth of breast cancer cells through epigenetic modification of Aurora A expression and function.

The objectives of this study were to evaluate the effects of tanshinones from a Chinese herb Salvia Miltiorrhiza on the growth of breast cancer cells, and to elucidate cellular and molecular mechanisms of action. Tanshinones showed the dose-dependent effect on the growth inhibition of breast cancer...

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Main Authors: Yi Gong, Yanli Li, Hamid M Abdolmaleky, Linglin Li, Jin-Rong Zhou
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2012-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3317444?pdf=render
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spelling doaj-7ee4a84abab54e4397a6961f8df581372020-11-25T02:08:05ZengPublic Library of Science (PLoS)PLoS ONE1932-62032012-01-0174e3365610.1371/journal.pone.0033656Tanshinones inhibit the growth of breast cancer cells through epigenetic modification of Aurora A expression and function.Yi GongYanli LiHamid M AbdolmalekyLinglin LiJin-Rong ZhouThe objectives of this study were to evaluate the effects of tanshinones from a Chinese herb Salvia Miltiorrhiza on the growth of breast cancer cells, and to elucidate cellular and molecular mechanisms of action. Tanshinones showed the dose-dependent effect on the growth inhibition of breast cancer cells in vitro, with tanshinone I (T1) the most potent agent. T1 was also the only tanshinone to have potent activity in inhibiting the growth of the triple-negative breast cancer cell line MDA-MB231. T1 caused cell cycle arrests of both estrogen-dependent and estrogen-independent cell lines associated with alterations of cyclinD, CDK4 and cyclinB, and induced breast cancer cell apoptosis associated with upregulation of c-PARP and downregulation of survivin and Aurora A. Among these associated biomarkers, Aurora A showed the most consistent pattern with the anti-growth activity of tanshinones. Overexpression of Aurora A was also verified in breast tumors. The gene function assay showed that knockdown of Aurora A by siRNA dramatically reduced the growth-inhibition and apoptosis-induction activities of T1, suggesting Aurora A as an important functional target of T1 action. On the other hand, tanshinones had much less adverse effects on normal mammary epithelial cells. Epigenetic mechanism studies showed that overexpression of Aurora A gene in breast cancer cells was not regulated by gene promoter DNA methylation, but by histone acetylation. T1 treatment significantly reduced acetylation levels of histone H3 associated with Aurora A gene. Our results supported the potent activity of T1 in inhibiting the growth of breast cancer cells in vitro in part by downregulation of Aurora A gene function. Our previous studies also demonstrated that T1 had potent anti-angiogenesis activity and minimal side effects in vivo. Altogether, this study warrants further investigation to develop T1 as an effective and safe agent for the therapy and prevention of breast cancer.http://europepmc.org/articles/PMC3317444?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Yi Gong
Yanli Li
Hamid M Abdolmaleky
Linglin Li
Jin-Rong Zhou
spellingShingle Yi Gong
Yanli Li
Hamid M Abdolmaleky
Linglin Li
Jin-Rong Zhou
Tanshinones inhibit the growth of breast cancer cells through epigenetic modification of Aurora A expression and function.
PLoS ONE
author_facet Yi Gong
Yanli Li
Hamid M Abdolmaleky
Linglin Li
Jin-Rong Zhou
author_sort Yi Gong
title Tanshinones inhibit the growth of breast cancer cells through epigenetic modification of Aurora A expression and function.
title_short Tanshinones inhibit the growth of breast cancer cells through epigenetic modification of Aurora A expression and function.
title_full Tanshinones inhibit the growth of breast cancer cells through epigenetic modification of Aurora A expression and function.
title_fullStr Tanshinones inhibit the growth of breast cancer cells through epigenetic modification of Aurora A expression and function.
title_full_unstemmed Tanshinones inhibit the growth of breast cancer cells through epigenetic modification of Aurora A expression and function.
title_sort tanshinones inhibit the growth of breast cancer cells through epigenetic modification of aurora a expression and function.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2012-01-01
description The objectives of this study were to evaluate the effects of tanshinones from a Chinese herb Salvia Miltiorrhiza on the growth of breast cancer cells, and to elucidate cellular and molecular mechanisms of action. Tanshinones showed the dose-dependent effect on the growth inhibition of breast cancer cells in vitro, with tanshinone I (T1) the most potent agent. T1 was also the only tanshinone to have potent activity in inhibiting the growth of the triple-negative breast cancer cell line MDA-MB231. T1 caused cell cycle arrests of both estrogen-dependent and estrogen-independent cell lines associated with alterations of cyclinD, CDK4 and cyclinB, and induced breast cancer cell apoptosis associated with upregulation of c-PARP and downregulation of survivin and Aurora A. Among these associated biomarkers, Aurora A showed the most consistent pattern with the anti-growth activity of tanshinones. Overexpression of Aurora A was also verified in breast tumors. The gene function assay showed that knockdown of Aurora A by siRNA dramatically reduced the growth-inhibition and apoptosis-induction activities of T1, suggesting Aurora A as an important functional target of T1 action. On the other hand, tanshinones had much less adverse effects on normal mammary epithelial cells. Epigenetic mechanism studies showed that overexpression of Aurora A gene in breast cancer cells was not regulated by gene promoter DNA methylation, but by histone acetylation. T1 treatment significantly reduced acetylation levels of histone H3 associated with Aurora A gene. Our results supported the potent activity of T1 in inhibiting the growth of breast cancer cells in vitro in part by downregulation of Aurora A gene function. Our previous studies also demonstrated that T1 had potent anti-angiogenesis activity and minimal side effects in vivo. Altogether, this study warrants further investigation to develop T1 as an effective and safe agent for the therapy and prevention of breast cancer.
url http://europepmc.org/articles/PMC3317444?pdf=render
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AT hamidmabdolmaleky tanshinonesinhibitthegrowthofbreastcancercellsthroughepigeneticmodificationofauroraaexpressionandfunction
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