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首页> 外文期刊>Journal of Cancer Research and Clinical Oncology >Combined loss of TFF3 and PTEN is associated with lethal outcome and overall survival in men with prostate cancer
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Combined loss of TFF3 and PTEN is associated with lethal outcome and overall survival in men with prostate cancer

机译:TFF3和PTEN的联合丧失与致命结果和前列腺癌的男性的整体生存有关

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BackgroundTrefoil Factor 3 (TFF3) has been implicated in Prostate Cancer (PCa) progression. However, its prognostic value and association with other biomarkers have not been fully explored. We assessed the combined value of TFF3 and PTEN in two cohorts: one is managed surgically for localized PCa and the second is managed non-surgically by androgen deprivation therapy for advanced disease.Design228 radical prostatectomies (RP) and 318 transurethral resection of prostate (TURP) samples were assessed by immunohistochemistry (IHC) for TFF3 and by IHC and fluorescent in situ hybridization (FISH) for PTEN. Results of biomarkers expression were correlated with various pathological and clinical outcome parameters including biochemical recurrence (BCR) in the RP cohort and cancer-specific mortality (PCSM) and overall survival (OS) in the TURP cohort.ResultsTFF3 expression was detected in 131/226 (57.9%) RP samples and 148/318 (46.5%) of TURP cases. In general, TFF3 positivity was less frequently observed with advanced Gleason Groups. TFF3 expression was also assessed in relation to PTEN expression. Only 15-16% of TFF3-expressed cases were present in association with complete loss of PTEN expression in the TURP and localized cohorts, respectively. Loss of TFF3 expression was not related to BCR after RP, but was prognostic in the non-surgical cohort and associated with decrease OS and PCSM (HR 2.31, CI: 1.67-3.18, p<0.0001) and (HR 3.99, CI: 2.43-6.56; p<0.0001), respectively. Adjusting for Gleason score, combined loss of TFF3/PTEN was most associated with OS (HR 2.33, CI: 1.49-3.62; p<0.0001) and PCSM (HR=3.44, CI: 1.75-6.78, p<0.0001).ConclusionThe study documents for the first time significant association for combined status of TFF3 expression and PTEN loss in OS and PCSM in patients not managed by surgical intervention. Prospective assessment of PTEN and TFF3 may provide further insight into molecularly subtyping PCa and aid in stratifying patients at risk for lethal disease.
机译:背景图案系数3(TFF3)已涉及前列腺癌(PCA)进展。然而,它的预后价值和与其他生物标志物联合尚未得到充分探索。我们评估了TFF3和PTEN中的两个队列中的综合值:一个在手术上进行管理,用于局部PCA,第二个通过雄激素剥夺治疗进行治疗,用于晚期疾病。DESIGN228自由基前列腺切除术(RP)和318分尿液切除前列腺(TURP )通过免疫组织化学(IHC)对TFF3和IHC和荧光原位杂交(鱼类)进行分类的样品。生物标志物表达的结果与在RP群组中的生物化学复发(BCR)的各种病理和临床结果参数相关,并且在Turp Cohort.resultstff3表达中,在131/226中检测到Turp Cohort.resultstff3表达的整体存活(OS)。 (57.9%)RP样品和148/318(46.5%)的草图病例。通常,用先进的Gleason组频率观察到TFF3积极性。还关于PTEN表达评估了TFF3表达。只有15-16%的TFF3表达病例分别与土耳其人和局部队列中的PTEN表达完全丧失。 RP3表达的丧失与RP之后的BCR无关,但在非外科队列中预后并与降低OS和PCSM相关(HR 2.31,CI:1.67-3.18,P <0.0001)和(HR 3.99,CI:2.43分别为-6.56; p <0.0001)。调整Glason评分,TFF3 / PTEN的联合损失与OS最相关(HR 2.33,CI:1.49-3.62; P <0.0001)和PCSM(HR = 3.44,CI:1.75-6.78,P <0.0001)。结论研究第一次患者组合于TFF3表达和PTEM损耗的第一次综合关联的文献,在没有手术干预的患者中的OS和PCSM中。 PTEN和TFF3的前瞻性评估可以进一步了解分子亚型PCA,并有助于致命疾病风险的分层患者。

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