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  • 标题:Inhibition of Antiestrogen-Promoted Pro-Survival Autophagy and Tamoxifen Resistance in Breast Cancer through Vitamin D Receptor
  • 本地全文:下载
  • 作者:Ye Li ; Katherine L Cook ; Wei Yu
  • 期刊名称:Nutrients
  • 电子版ISSN:2072-6643
  • 出版年度:2021
  • 卷号:13
  • 期号:5
  • 页码:1715
  • DOI:10.3390/nu13051715
  • 出版社:MDPI Publishing
  • 摘要:We determined how vitamin D receptor (VDR) is linked to disease outcome in estrogen receptor-positive (ER ) breast cancer patients treated with tamoxifen (TAM). Breast cancer patients (n = 581) in four different datasets were divided into those expressing higher (above median) and lower levels of VDR in pretreatment ER tumors. Across all datasets, TAM-treated patients with higher pretreatment tumor VDR expression exhibited significantly longer recurrence-free survival. Ingenuity pathway analysis identified autophagy and unfolded protein response (UPR) as top differentially expressed pathways between high and low VDR-expressing ER cancers. Activation of VDR with vitamin D (VitD), either calcitriol or its synthetic analog EB1089, sensitized MCF-7-derived, antiestrogen-resistant LCC9 human breast cancer cells to TAM, and attenuated increased UPR and pro-survival autophagy. Silencing of VDR blocked these effects through the IRE1α-JNK pathway. Further, silencing of VDR impaired sensitivity to TAM in antiestrogen-responsive LCC1 cells, and prevented the effects of calcitriol and EB1089 on UPR and autophagy. In a preclinical mouse model, dietary VitD supplementation induced VDR activation and reduced carcinogen-induced ER mammary tumor incidence. In addition, IRE1α-JNK signaling was downregulated and survival autophagy was inhibited in mammary tumors of VitD-supplemented mice. Thus, activation of VDR is predictive of reduced risk of breast cancer recurrence in ER patients, possibly by inhibiting antiestrogen-promoted pro-survival autophagy.
  • 关键词:breast cancer; recurrence-free survival; tamoxifen; vitamin D receptor; vitamin D analogs; autophagy breast cancer ; recurrence-free survival ; tamoxifen ; vitamin D receptor ; vitamin D analogs ; autophagy
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