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雄激素受体水平的调控:对前列腺癌进展和治疗的影响

Regulation of androgen receptor levels: implications for prostate cancer progression and therapy.

作者信息

Burnstein Kerry L

机构信息

Department of Molecular and Cellular Pharmacology, University of Miami Miller School of Medicine, Miami, Florida, USA.

出版信息

J Cell Biochem. 2005 Jul 1;95(4):657-69. doi: 10.1002/jcb.20460.

Abstract

Androgen deprivation has been the standard therapy for advanced and metastatic prostate cancer for over half a century, as prostate tumors are initially dependent on androgens for growth and survival. Unfortunately, in most patients undergoing androgen ablation, relapse (recurrent tumor growth) eventually occurs. The actions of the principal androgens, testosterone and dihydrotestosterone (DHT), are mediated via androgen receptors (ARs), ligand-activated transcription factors that belong to the nuclear receptor superfamily. Because of the presence of transcriptionally active ARs in tumors from recurrent or androgen-independent disease, there is a heightened interest in new therapeutic paradigms that target the AR and its regulatory pathways. The regulation of AR levels is highly complex with control exerted by several pathways and in a cell-, tissue-, and developmental-stage specific manner. Androgens are important regulators of AR mRNA and protein through transcriptional and post-transcriptional mechanisms. This article reviews the evidence implicating the AR in recurrent prostate cancer and discusses the multiple mechanisms that regulate AR levels in normal and neoplastic cells. The complexity of AR regulation suggests that there will be an ample array of potential new drug targets for modulating levels of this receptor, a key signaling molecule in prostate cancer.

摘要

半个多世纪以来,雄激素剥夺一直是晚期和转移性前列腺癌的标准治疗方法,因为前列腺肿瘤最初依赖雄激素生长和存活。不幸的是,在大多数接受雄激素消融治疗的患者中,最终会出现复发(肿瘤复发生长)。主要雄激素睾酮和双氢睾酮(DHT)的作用是通过雄激素受体(ARs)介导的,ARs是属于核受体超家族的配体激活转录因子。由于复发或雄激素非依赖性疾病的肿瘤中存在转录活性ARs,因此人们对靶向AR及其调节途径的新治疗模式越来越感兴趣。AR水平的调节非常复杂,由多种途径控制,并且具有细胞、组织和发育阶段特异性。雄激素通过转录和转录后机制是AR mRNA和蛋白质的重要调节因子。本文综述了AR与复发性前列腺癌相关的证据,并讨论了调节正常细胞和肿瘤细胞中AR水平的多种机制。AR调节的复杂性表明,将有大量潜在的新药物靶点来调节该受体的水平,该受体是前列腺癌中的关键信号分子。

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