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雄激素在人前列腺癌细胞系LNCaP中通过转录后调控增殖细胞核抗原的表达。

Androgens regulate the expression of proliferating cell nuclear antigen posttranscriptionally in the human prostate cancer cell line, LNCaP.

作者信息

Perry J E, Tindall D J

机构信息

Department of Urology Research, Mayo Clinic Foundation, Rochester, Minnesota 55905, USA.

出版信息

Cancer Res. 1996 Apr 1;56(7):1539-44.

PMID:8603399
Abstract

Proliferating cell nuclear antigen (PCNA) expression is required for DNA replication. Because androgens are critical for prostate cell proliferation, we investigated the effects of androgen on PCNA expression in the prostatic cancer cell line LNCaP. Flow cytometric analysis was used to measure cellular DNA content with dual labeling of PCNA. Semiconfluent LNCaP cells were grown in serum-free medium containing varying concentrations of the synthetic androgen mibolerone and processed for either fluorescence-activated cell sorting or Western analysis. Supplementation of serum-free medium with androgens resulted in dose-dependent changes in PCNA immunoreactivity, with maximum stimulation (2-fold) being achieved at 48 h with 10(-9)M mibolerone. Non-androgenic steroids did not change PCNA immunoreactivity compared with untreated controls, and the antiandrogen, casodex, inhibited the mibolerone-stimulated increase in PCNA immunoreactivity, suggesting that the androgenic induction of PCNA is mediated through the androgen receptor. The presence of a non-consensus androgen response element in the promoter region of the PCNA gene led us to investigate wether androgen responsiveness of the PCNA gene in LNCaP cells might be mediated at the transcriptional level. No change in steady-state mRNA for PCNA with androgen administration was observed. However, an investigation of the androgenic regulation of PCNA protein stability indicated that androgen treatment increased the half-life of 35S-labeled PCNA protein. In addition, polysome run-off translation assays demonstrated an increase in PCNA protein after a 6-h stimulation of LNCaP cells with 10(-9)M mibolerone. These data suggest that androgen induction of prostate cell proliferation may be mediated, at least in part, through PCNA at the posttranscriptional level.

摘要

增殖细胞核抗原(PCNA)的表达是DNA复制所必需的。由于雄激素对前列腺细胞增殖至关重要,我们研究了雄激素对前列腺癌细胞系LNCaP中PCNA表达的影响。采用流式细胞术分析并通过PCNA双重标记来测量细胞DNA含量。将接近汇合的LNCaP细胞在含有不同浓度合成雄激素米勃酮的无血清培养基中培养,然后进行荧光激活细胞分选或蛋白质免疫印迹分析。在无血清培养基中添加雄激素导致PCNA免疫反应性呈剂量依赖性变化,在48小时时,10^(-9)M米勃酮可实现最大刺激(2倍)。与未处理的对照相比,非雄激素类类固醇不会改变PCNA免疫反应性,而抗雄激素药物比卡鲁胺可抑制米勃酮刺激的PCNA免疫反应性增加,这表明PCNA的雄激素诱导作用是通过雄激素受体介导的。PCNA基因启动子区域存在一个非一致性雄激素反应元件,这促使我们研究LNCaP细胞中PCNA基因的雄激素反应性是否可能在转录水平上介导。未观察到给予雄激素后PCNA稳态mRNA有变化。然而,对PCNA蛋白稳定性的雄激素调节研究表明,雄激素处理增加了35S标记的PCNA蛋白的半衰期。此外,多核糖体释放翻译分析表明,用10^(-9)M米勃酮刺激LNCaP细胞6小时后,PCNA蛋白增加。这些数据表明,雄激素诱导前列腺细胞增殖可能至少部分是在转录后水平通过PCNA介导的。

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