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Molecular Pathways: Targeting Steroid Receptor Coactivators in Cancer

机译:分子途径:靶向癌症中的类固醇受体共觉器

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Coactivators represent a large class of proteins that partner with nuclear receptors and other transcription factors to regulate gene expression. Given their pleiotropic roles in the control of transcription, coactivators have been implicated in a broad range of human disease states, including cancer. This is best typified by the three members of the steroid receptor coacti-vator (SRC) family, each of which integrates steroid hormone signaling and growth factor pathways to drive oncogenic gene expression programs in breast, endometrial, ovarian, prostate, and other cancers. Because of this, coactivators represent emerging targets for cancer therapeutics, and efforts are now being made to develop SRC-targeting agents, such as the SI-2 inhibitor and the novel SRC stimulator, MCB-613, that are able to block cancer growth in cell culture and animal model systems. Here, we will discuss the mechanisms through which coactivators drive cancer progression and how targeting coactivators represent a novel conceptual approach to combat tumor growth that is distinct from the use of other targeted therapeutic agents. We also will describe efforts to develop next-generation SRC inhibitors and stimulators that can be taken into the clinic for the treatment of recurrent, drug-resistant cancers.
机译:共激活子是一大类与核受体和其他转录因子共同调节基因表达的蛋白质。鉴于辅激活子在转录控制中的多效性作用,它们与包括癌症在内的多种人类疾病状态有关。类固醇受体协同激活因子(SRC)家族的三个成员最能体现这一点,每个家族都整合了类固醇激素信号和生长因子途径,以驱动乳腺癌、子宫内膜癌、卵巢癌、前列腺癌和其他癌症中的致癌基因表达程序。正因为如此,共激活剂代表了癌症治疗学的新兴靶点,目前正在努力开发SRC靶向剂,如SI-2抑制剂和新型SRC刺激剂MCB-613,它们能够在细胞培养和动物模型系统中阻止癌症生长。在这里,我们将讨论共激活因子驱动癌症进展的机制,以及靶向共激活因子如何代表一种新的概念性方法来对抗肿瘤生长,这与使用其他靶向治疗剂不同。我们还将介绍开发新一代SRC抑制剂和刺激剂的努力,这些抑制剂和刺激剂可用于临床治疗复发性耐药癌症。

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