Mechanistic Progress of Estrogen-induced Apoptosis in Estrogen-deprivedBreast Cancer Cells

Journal of Cell Science and Therapy Pub Date : 2015-07-31 DOI:10.4172/2157-7013.1000218

S. Chai, P. Fan

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引用次数: 6

Abstract

The laboratory discovery of estrogen-induced apoptosis has been translated to treat antihormone resistant patients and to reduce the incidence of breast cancer in postmenopausal hysterectomized women with estrogen replacement therapy (ERT). The key step is the selection pressure exerted by long-term antiestrogen therapy or over 5 years of menopause to specific breast cancer cell populations that will be vulnerable to estrogen-induced apoptosis. However, the mechanisms underlying estrogen-induced apoptosis are currently unclear. At the cellular level, estrogen-induced apoptosis is dependent upon the estrogen receptor (ER), which can be completely blocked by antiestrogen ICI 182,780 or 4-hydroxytamoxifen (4-OHT). Knockdown of ER alpha, but not ER beta, through specific small interfering RNAs effectively blocks estrogen-induced apoptosis, indicating that the ER alpha subtype participates in apoptosis. Further examinations demonstrate that estrogen-induced apoptosis is due to accumulation of endoplasmic reticulum stress, inflammatory responses, and oxidative stress, which, in turn, activate the intrinsic mitochondrial pathway and the extrinsic death receptor pathway to complete the process. This contrasts with paclitaxel, which causes G2 arrest with immediate apoptosis. These stress responses are modulated by glucocorticoids and the c-Src inhibitor to block estrogen-induced apoptosis, but the mechanism for estrogen action is through a genomic pathway rather than a non-genomic pathway. In the nucleus, estrogen activates classic ERE-regulated endogenous genes, but the ERE transcriptional pathway does not directly participate in the estrogen-induced apoptosis in vitro or in vivo. Simultaneously, estrogen activates a non-classic transcriptional pathway involving the interaction of ER with transcription factors such as activator protein-1 (AP-1), which may regulate proliferation, stress responses, or apoptosis. Investigation of how AP-1 modulates the stress responses to trigger estrogen-induced apoptosis will ultimately uncover the mechanisms underlying estrogen-induced apoptosis.

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雌激素缺失乳腺癌细胞中雌激素诱导凋亡的机制研究进展

雌激素诱导的细胞凋亡的实验室发现已经转化为治疗抗激素抵抗患者，并减少绝经后子宫切除术妇女雌激素替代疗法(ERT)的乳腺癌发病率。关键的一步是长期抗雌激素治疗或超过5年的更年期对特定的乳腺癌细胞群施加的选择压力，这些细胞群将容易受到雌激素诱导的凋亡。然而，雌激素诱导细胞凋亡的机制目前尚不清楚。在细胞水平上，雌激素诱导的细胞凋亡依赖于雌激素受体(ER)，雌激素受体可被抗雌激素ICI 182780或4-羟基他莫昔芬(4-OHT)完全阻断。通过特异性小干扰rna敲低ER α，而不敲低ER β，可有效阻断雌激素诱导的细胞凋亡，表明ER α亚型参与细胞凋亡。进一步的研究表明，雌激素诱导的细胞凋亡是由于内质网应激、炎症反应和氧化应激的积累，这反过来又激活了内在线粒体途径和外在死亡受体途径来完成这一过程。这与紫杉醇相反，后者引起G2阻滞并立即凋亡。这些应激反应由糖皮质激素和c-Src抑制剂调节，以阻断雌激素诱导的细胞凋亡，但雌激素的作用机制是通过基因组途径而不是非基因组途径。在细胞核内，雌激素激活经典的ERE调控内源基因，但在体内体外，ERE转录途径并不直接参与雌激素诱导的细胞凋亡。同时，雌激素激活了一条非经典的转录途径，包括内质网与转录因子如激活蛋白-1 (AP-1)的相互作用，这可能调节增殖、应激反应或细胞凋亡。研究AP-1如何调节应激反应触发雌激素诱导的细胞凋亡，将最终揭示雌激素诱导细胞凋亡的机制。

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Journal of Cell Science and Therapy

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