Downregulation of BAGâ1 in T47D cells promotes resistance to tamoxifen via activation of the PI3K/Akt/mTOR signaling pathway.
[No authors listed]
摘要
Tamoxifen, a selective estrogen receptor (ER) modulator, is the most widely used endocrine therapy for patients with ERâpositive breast cancer. However, ~30% of tamoxifenâtreated breast cancers do not initially respond to tamoxifen, and neither do they eventually develop tamoxifen resistance. Bclâ2âassociated athanogene 1 (BAGâ1) is a multifunctional protein that interacts with a wide range of molecules to protect cells from apoptosis otherwise induced by cytotoxic drugs, growth factor withdrawal, radiation and stress. The aim of the present study was to investigate the function of BAGâ1 in tamoxifen resistance. Immunohistochemistry techniques were used to determine BAGâ1 expression in 119 stage IâIII primary breast cancer tissues and it was identified that BAGâ1 was significantly overexpressed in ERâpositive breast cancer (P=0.001). Knockdown of BAGâ1 by short interfering RNA was revealed to downregulate ER, and upregulate phospho (p)âprotein kinase B (Akt) and pâmammalian target of rapamycin (mTOR) levels. Furthermore, significantly decreased tamoxifenâinduced apoptosis (41.70±1.93 vs. 55.03±2.39%; P=0.012) was observed in T47D cells following the silencing of BAGâ1. In contrast, overexpression of BAGâ1 long enhanced apoptosis (65.10±2.35 vs. 55.03±2.39%; P=0.039) in T47D cells treated with tamoxifen. Combination treatment of tamoxifen and an mTOR inhibitor restored the inhibitory effects of tamoxifen in T47D cells exhibiting low BAGâ1 expression levels (66.87±2.27 vs. 57.07±2.46%; P=0.037). In conclusion, there results of the present study indicated that suppression of BAGâ1 expression may activate the phosphoinositide 3âkinase/Akt/mTOR pathway and protect ERâpositive breast cancer cells from tamoxifenâinduced inhibition of proliferation. ERâpositive breast cancer cells exhibiting low BAGâ1 expression appeared to be more sensitive to treatment with the mTOR inhibitor rapamycin. Furthermore, the results indicated that combination treatment targeting ER with tamoxifen and targeting mTOR with rapamycin may significantly potentiate the inhibitory effect in BAGâ1âsilenced cells.
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