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癌症中的核受体共抑制复合物:机制、功能与调控

Nuclear receptor corepressor complexes in cancer: mechanism, function and regulation.

作者信息

Wong Madeline M, Guo Chun, Zhang Jinsong

机构信息

Department of Pharmacological & Physiological Science, Saint Louis University School of Medicine St. Louis, Missouri 63104.

出版信息

Am J Clin Exp Urol. 2014 Oct 2;2(3):169-87. eCollection 2014.

PMID:25374920
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4219314/
Abstract

Nuclear receptor corepressor (NCoR) and silencing mediator for retinoid and thyroid hormone receptors (SMRT) function as corepressors for diverse transcription factors including nuclear receptors such as estrogen receptors and androgen receptors. Deregulated functions of NCoR and SMRT have been observed in many types of cancers and leukemias. NCoR and SMRT directly bind to transcription factors and nucleate the formation of stable complexes that include histone deacetylase 3, transducin b-like protein 1/TBL1-related protein 1, and G-protein pathway suppressor 2. These NCoR/SMRT-interacting proteins also show deregulated functions in cancers. In this review, we summarize the literature on the mechanism, regulation, and function of the core components of NCoR/SMRT complexes in the context of their involvement in cancers and leukemias. While the current studies support the view that the corepressors are promising targets for cancer treatment, elucidation of the mechanisms of corepressors involved in individual types of cancers is likely required for effective therapy.

摘要

核受体共抑制因子(NCoR)和维甲酸及甲状腺激素受体沉默介质(SMRT)作为多种转录因子的共抑制因子发挥作用,这些转录因子包括雌激素受体和雄激素受体等核受体。在许多类型的癌症和白血病中都观察到了NCoR和SMRT的功能失调。NCoR和SMRT直接与转录因子结合,并促使形成稳定的复合物,该复合物包括组蛋白去乙酰化酶3、转导素β样蛋白1/TBL1相关蛋白1和G蛋白途径抑制因子2。这些与NCoR/SMRT相互作用的蛋白在癌症中也表现出功能失调。在本综述中,我们总结了关于NCoR/SMRT复合物核心成分在癌症和白血病中的作用机制、调控及功能的文献。虽然目前的研究支持共抑制因子是癌症治疗有前景的靶点这一观点,但可能需要阐明共抑制因子在个体癌症类型中的作用机制才能实现有效治疗。

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