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The Early Effects of Rapid Androgen Deprivation on Human Prostate Cancer

机译:快速雄激素剥夺对人类前列腺癌的早期影响

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摘要

The androgen receptor (AR) is the dominant growth factor in prostate cancer (PCa). Therefore, understanding how ARs regulate the human transcriptome is of paramount importance. The early effects of castration on human PCa have not previously been studied 27 patients medically castrated with degarelix 7 d before radical prostatectomy. We used mass spectrometry, immunohistochemistry, and gene expression array (validated by reverse transcription-polymerase chain reaction) to compare resected tumour with matched, controlled, untreated PCa tissue. All patients had levels of serum androgen, with reduced levels of intraprostatic androgen at prostatectomy. We observed differential expression of known androgen-regulated genes (TMPRSS2, KLK3, CAMKK2, FKBP5). We identified 749 genes downregulated and 908 genes upregulated following castration. AR regulation of α-methylacyl-CoA racemase expression and three other genes (FAM129A, RAB27A, and KIAA0101) was confirmed. Upregulation of oestrogen receptor 1 (ESR1) expression was observed in malignant epithelia and was associated with differential expression of ESR1-regulated genes and correlated with proliferation (Ki-67 expression).
机译:雄激素受体(AR)是前列腺癌(PCa)中的主要生长因子。因此,了解AR如何调节人类转录组至关重要。先前尚未研究去势对人类PCa的早期影响27例患者在前列腺癌根治术前7 d用地加瑞克7药物去势。我们使用质谱,免疫组织化学和基因表达阵列(通过逆转录-聚合酶链反应验证)来比较切除的肿瘤与匹配,受控,未经治疗的PCa组织。所有患者的血清雄激素水平均降低,前列腺切除术中前列腺内雄激素水平降低。我们观察到了已知雄激素调节基因(TMPRSS2,KLK3,CAMKK2,FKBP5)的差异表达。我们鉴定了去势后的749个基因下调和908个基因上调。证实了对α-甲基酰基辅酶A消旋酶表达和其他三个基因(FAM129A,RAB27A和KIAA0101)的AR调节。在恶性上皮中观察到雌激素受体1(ESR1)表达上调,并且与ESR1调控基因的差异表达相关,并与增殖相关(Ki-67表达)。

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