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Androgen receptor down regulation by small interference RNA induces cell growth inhibition in androgen sensitive as well as in androgen independent prostate cancer cells.小分子干扰RNA介导的雄激素受体下调可抑制雄激素敏感及雄激素非依赖型前列腺癌细胞的生长。
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Small-interfering RNA-induced androgen receptor silencing leads to apoptotic cell death in prostate cancer.小干扰RNA诱导的雄激素受体沉默导致前列腺癌细胞凋亡。
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HER2/neu kinase-dependent modulation of androgen receptor function through effects on DNA binding and stability.HER2/neu激酶通过影响DNA结合和稳定性对雄激素受体功能进行依赖性调节。
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Rapid signalling pathway activation by androgens in epithelial and stromal cells.雄激素在上皮细胞和基质细胞中快速激活信号通路。
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Antiandrogen withdrawal alone or in combination with ketoconazole in androgen-independent prostate cancer patients: a phase III trial (CALGB 9583).单独使用抗雄激素药物或与酮康唑联合用于雄激素非依赖性前列腺癌患者:一项III期试验(CALGB 9583)。
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Short interfering RNAs can induce unexpected and divergent changes in the levels of untargeted proteins in mammalian cells.短干扰RNA可在哺乳动物细胞中诱导非靶向蛋白质水平发生意想不到的不同变化。
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Molecular determinants of resistance to antiandrogen therapy.抗雄激素治疗耐药性的分子决定因素。
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Androgen receptor mediates non-genomic activation of phosphatidylinositol 3-OH kinase in androgen-sensitive epithelial cells.雄激素受体介导雄激素敏感性上皮细胞中磷脂酰肌醇3-羟基激酶的非基因组激活。
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Epidermal growth factor increases coactivation of the androgen receptor in recurrent prostate cancer.表皮生长因子增加复发性前列腺癌中雄激素受体的共激活。
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Steroids and oocyte maturation--a new look at an old story.类固醇与卵母细胞成熟——对一个老故事的新审视。
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雄激素受体对雄激素非依赖性CWR22前列腺癌细胞的细胞周期进程仍然至关重要。

Androgen receptor remains critical for cell-cycle progression in androgen-independent CWR22 prostate cancer cells.

作者信息

Yuan Xin, Li Tong, Wang Hongyun, Zhang Tao, Barua Moumita, Borgesi Robert A, Bubley Glenn J, Lu Michael L, Balk Steven P

机构信息

Hematology/Oncology Division, Beth Israel Deaconess Medical Center, 330 Brookline Ave., Boston, MA 02215, USA.

出版信息

Am J Pathol. 2006 Aug;169(2):682-96. doi: 10.2353/ajpath.2006.051047.

DOI:10.2353/ajpath.2006.051047
PMID:16877366
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1698802/
Abstract

The majority of prostate cancers (PCa) that relapse after androgen deprivation therapy (androgen-independent PCa) continue to express androgen receptor (AR). To study the functional importance of AR in these tumors, we derived androgen-independent CWR22 PCa xenografts in castrated mice and generated a cell line from one of these xenografts (CWR22R3). Similarly to androgen-independent PCa in patients, the relapsed xenografts and cell line expressed AR and were resistant to treatment with bicalutamide. However, expression of the AR-regulated PSA gene in the CWR22R3 cell line was markedly decreased compared to the relapsed xenografts in vivo. Transfections with androgen-regulated reporter genes further indicated that the cells lacked androgen-independent AR transcriptional activity and were not hypersensitive to low androgen concentrations despite constitutive activation of the Erk/MAP kinases. Nonetheless, AR remained essential for androgen-independent growth because retroviral shRNA-mediated AR down-regulation resulted in marked long-term growth suppression. This was associated with increased levels of p27(kip1) and hypophosphorylation of retinoblastoma protein but not with decreases in D-type cyclin levels or MAP kinase activation. These results reveal a potentially critical function of AR in androgen-independent PCa that is distinct from its previously described transcriptional or nontranscriptional functions.

摘要

大多数在雄激素剥夺治疗后复发的前列腺癌(去势抵抗性前列腺癌)仍继续表达雄激素受体(AR)。为了研究AR在这些肿瘤中的功能重要性,我们在去势小鼠中培育出去势抵抗性CWR22前列腺癌异种移植瘤,并从其中一个异种移植瘤中建立了一个细胞系(CWR22R3)。与患者的去势抵抗性前列腺癌相似,复发的异种移植瘤和细胞系表达AR,并且对比卡鲁胺治疗具有抗性。然而,与体内复发的异种移植瘤相比,CWR22R3细胞系中AR调控的PSA基因的表达明显降低。用雄激素调控的报告基因进行转染进一步表明,尽管Erk/MAP激酶组成性激活,但这些细胞缺乏雄激素非依赖性AR转录活性,并且对低浓度雄激素不敏感。尽管如此,AR对于雄激素非依赖性生长仍然至关重要,因为逆转录病毒shRNA介导的AR下调导致明显的长期生长抑制。这与p27(kip1)水平升高和成视网膜细胞瘤蛋白的低磷酸化有关,但与D型细胞周期蛋白水平降低或MAP激酶激活无关。这些结果揭示了AR在去势抵抗性前列腺癌中一种潜在的关键功能,该功能与其先前描述的转录或非转录功能不同。