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首页> 外文期刊>The Prostate >The anterior gradient 2 (AGR2) gene is overexpressed in prostate cancer and may be useful as a urine sediment marker for prostate cancer detection.
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The anterior gradient 2 (AGR2) gene is overexpressed in prostate cancer and may be useful as a urine sediment marker for prostate cancer detection.

机译:前梯度2(AGR2)基因在前列腺癌中过表达,可能可用作前列腺癌检测的尿沉渣标记。

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BACKGROUND: AGR2 is a member of the endoplasmatic reticulum protein disulphide isomerase gene family implicated in tumor metastasis. Its expression pattern, function, and utility as a marker remains to be further investigated. METHODS: Using real-time RT-PCR and immunohistochemistry, changes of expression in different tumor stages were explored in microdissected tumor samples. AGR2 transcript level in urine sediments was scrutinized for suitability as a tumor marker. AGR2 androgen regulation and function were analyzed in cellular prostate cancer models. RESULTS: AGR2 is highly expressed in prostate cancer compared to benign tissue in particular also in low-grade tumors and PIN lesions. AGR2 transcripts were detected in urine sediments of patients undergoing prostate biopsy with significantly higher levels in tumor patients. The urine AGR2/PSA transcript ratio allowed much better discrimination between cancer and benign patients than serum total PSA or %freePSA. Prostate tumor cells express and secrete variable amounts of AGR2 protein, the highest level was found in PC3 cells. In androgen receptor-positive cell lines AGR2 is upregulated by androgens. Increased expression enhanced the migratory and invasive potential but decreased growth and proliferation in vitro and in vivo. CONCLUSION: AGR2 enhances the invasion phenotype of prostate cancer cells while at the same time attenuating cell-cycle progression. This function, its expression pattern and the increased level of AGR transcripts in urine sediments of prostate cancer patients call for further exploration as a prostate cancer marker and a modulator of tumor growth and invasion.
机译:背景:AGR2是内质网蛋白二硫键异构酶基因家族成员,与肿瘤转移有关。其表达模式,功能和作为标志物的用途仍有待进一步研究。方法:利用实时RT-PCR和免疫组化技术,在显微解剖的肿瘤样品中探讨不同肿瘤阶段表达的变化。仔细检查尿沉渣中的AGR2转录水平是否适合作为肿瘤标志物。在细胞前列腺癌模型中分析了AGR2雄激素的调节和功能。结果:与良性组织相比,AGR2在前列腺癌中高表达,特别是在低度肿瘤和PIN病变中。在进行前列腺穿刺活检的患者的尿沉渣中检测到了AGR2转录本,而在肿瘤患者中其水平明显升高。尿液AGR2 / PSA的转录比例比血清总PSA或%freePSA更好地区分了癌症患者和良性患者。前列腺肿瘤细胞表达和分泌不同量的AGR2蛋白,在PC3细胞中发现最高水平。在雄激素受体阳性细胞系中,AGR2被雄激素上调。表达的增加增强了迁移和侵袭的潜力,但在体外和体内降低了生长和增殖。结论:AGR2增强了前列腺癌细胞的侵袭表型,同时减弱了细胞周期进程。前列腺癌患者尿沉渣中的这种功能,其表达模式和AGR转录物水平的提高,需要进一步探索作为前列腺癌的标志物以及肿瘤生长和侵袭的调节剂。

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