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Expression patterns of candidate susceptibility genes HNF1β and CtBP2 in prostate cancer: Association with tumor progression

机译:候选易感基因HNF1β和CtBP2在前列腺癌中的表达模式:与肿瘤进展的关系

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Objectives: Genome-wide association studies have identified variants at multiple loci associated with prostate cancer (PCa) risk. Some of these loci include candidate susceptibility genes, such as MSMB, HNF1β, and C-terminal-binding protein (CtBP2). Except for MSMB, the clinicopathological significance of these genes has not been investigated. We therefore aimed to analyze their expression in PCa tissues, in relation with tumor progression and aggressiveness. Methods and materials: Protein expression was evaluated by immunohistochemistry on tissue microarrays containing samples from normal prostate (NL, n = 91), high-grade prostatic intraepithelial neoplasia (PIN, n = 61), clinically localized PCa (CLC, n = 434), PCa metastases (M, n = 28), and castration-resistant PCa (CRC, n = 49). Moreover, mRNA expression for each marker was assessed by quantitative real-time polymerase chain reaction, on 53 frozen samples of NL, CLC, and CRC. Results: These genes were differentially expressed at the different stages of PCa natural history. MSMB expression decreased with disease development and progression. In contrast, nuclear HNF1β and CtBP2 staining significantly increased in the CRC and M groups when compared with CLC, together with the transcripts levels. In patients with CLC, HNF1β and CtBP2 nuclear expressions were strongly associated with cancer cell proliferation. After adjusting for the Gleason score and the pathological stage, none of the candidate genes was significantly predictive of recurrence after radical prostatectomy. In patients with CRC, CtBP2 nuclear staining was associated with shorter overall survival. Conclusions: The decrease of MSMB expression during tumor progression strongly supports its role as a tumor-suppressor gene. Although its functions remain to be clarified in PCa cells, HNF1β and CtBP2 are associated with cancer cell proliferation, tumor progression, and castration-resistant disease.
机译:目的:全基因组关联研究已确定与前列腺癌(PCa)风险相关的多个基因座的变异。这些基因座中的一些包括候选易感基因,例如MSMB,HNF1β和C末端结合蛋白(CtBP2)。除了MSMB,尚未研究这些基因的临床病理意义。因此,我们旨在分析其在PCa组织中与肿瘤进展和侵袭性相关的表达。方法和材料:通过免疫组织化学在组织微阵列上评估蛋白质表达,该组织微阵列包含来自正常前列腺(NL,n = 91),高度前列腺上皮内瘤变(PIN,n = 61),临床定位的PCa(CLC,n = 434)的样品,PCa转移(M,n = 28)和去势抵抗性PCa(CRC,n = 49)。此外,在53个冷冻的NL,CLC和CRC样品上,通过定量实时聚合酶链反应评估了每种标记物的mRNA表达。结果:这些基因在PCa自然史的不同阶段差异表达。 MSMB表达随着疾病的发展和进展而降低。相反,与CLC相比,CRC和M组的核HNF1β和CtBP2染色显着增加。在CLC患者中,HNF1β和CtBP2的核表达与癌细胞增殖密切相关。调整格里森评分和病理分期后,所有候选基因均不能显着预测前列腺癌根治术后复发。在CRC患者中,CtBP2核染色与总体生存期缩短有关。结论:肿瘤进展过程中MSMB表达的降低强烈支持其作为肿瘤抑制基因的作用。尽管其功能在PCa细胞中仍有待阐明,但HNF1β和CtBP2与癌细胞增殖,肿瘤进展和去势抵抗性疾病有关。

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