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首页> 外文期刊>Journal of Molecular Endocrinology >Going off the grid: ERα breast cancer beyond estradiol
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Going off the grid: ERα breast cancer beyond estradiol

机译:脱离电网:雌二醇以外的ERα乳腺癌

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摘要

Novel studies have linked cholesterol biosynthesis to drug resistance in luminal breast cancer. Structural data suggest that cholesterol metabolites, including 27-hydroxycholesterol (27HC), can act as ERα ligands in these cells. Additionally, hypercholesterolemia has now been linked to breast cancer progression. The focus of this review is to briefly summarize these recent findings and discuss how epigenetic reprogramming is definitively connected to endogenous cholesterol biosynthesis. We elaborate on how these data support a working model in which cholesterol biosynthesis promotes autocrine, pro-invasive signaling via activation of a series of closely related transcription factors. Importantly, we discuss how this mechanism of resistance is specifically associated with aromatase inhibitors. Finally, we examine how the field is now considering the development of anticholesterol therapeutics and companion biomarkers to stratify and treat ERα breast cancer patients. In particular, we review recent progress in pharmaceutical strategies targeting the cholesterol molecular machinery in primary and secondary breast cancers.
机译:新的研究已将胆固醇的生物合成与管腔型乳腺癌的耐药性联系起来。结构数据表明胆固醇代谢物,包括27-羟基胆固醇(27HC),可以在这些细胞中充当ERα配体。此外,高胆固醇血症现已与乳腺癌的进展相关。这篇综述的重点是简要总结这些最新发现,并讨论表观遗传重编程如何与内源性胆固醇生物合成绝对相关。我们将详细说明这些数据如何支持一种工作模型,其中胆固醇生物合成通过激活一系列紧密相关的转录因子来促进自分泌,促侵入性信号传导。重要的是,我们讨论了这种抗药性机制如何与芳香化酶抑制剂特别相关。最后,我们检查该领域现在如何考虑开发抗胆固醇治疗药物和伴随生物标志物以对ERα乳腺癌患者进行分层和治疗。特别是,我们回顾了针对原发性和继发性乳腺癌中胆固醇分子机制的药物策略的最新进展。

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