TFF3 和 PTEN 联合缺失与前列腺癌男性的致死结局和总生存期相关。
Combined loss of TFF3 and PTEN is associated with lethal outcome and overall survival in men with prostate cancer.
机构信息
Department of Pathology and Laboratory Medicine, University of Calgary Cumming School of Medicine and Calgary Laboratory Services, Calgary, AB, Canada.
Department of Medical Oncology, Faculty of Medicine and Dentistry, University of Alberta, Edmonton, AB, Canada.
出版信息
J Cancer Res Clin Oncol. 2019 Jul;145(7):1751-1759. doi: 10.1007/s00432-019-02933-z. Epub 2019 May 25.
BACKGROUND
Trefoil 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.
DESIGN
228 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.
RESULTS
TFF3 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).
CONCLUSION
The 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.
背景
三叶因子 3(TFF3)已被牵连到前列腺癌(PCa)的进展中。然而,其预后价值及其与其他生物标志物的关联尚未得到充分探索。我们评估了 TFF3 和 PTEN 在两个队列中的联合价值:一个队列接受了局部前列腺癌的手术治疗,另一个队列接受了雄激素剥夺治疗的晚期疾病的非手术治疗。
设计
通过免疫组织化学(IHC)对 226 例根治性前列腺切除术(RP)和 318 例经尿道前列腺切除术(TURP)样本进行了 TFF3 评估,通过 IHC 和荧光原位杂交(FISH)对 PTEN 进行了评估。生物标志物表达的结果与各种病理和临床结果参数相关联,包括 RP 队列中的生化复发(BCR)和 TURP 队列中的癌症特异性死亡率(PCSM)和总生存率(OS)。
结果
在 226 例 RP 样本中的 131/226(57.9%)和 318 例 TURP 病例中的 148/318(46.5%)中检测到 TFF3 表达。一般来说,TFF3 阳性的发生率随着 Gleason 分组的进展而降低。还评估了 TFF3 表达与 PTEN 表达之间的关系。在 TURP 和局限性队列中,只有 15-16%的 TFF3 表达病例与完全缺失 PTEN 表达相关。在 RP 后,TFF3 表达缺失与 BCR 无关,但在非手术队列中具有预后意义,与降低 OS 和 PCSM 相关(HR 2.31,CI:1.67-3.18,p<0.0001)和(HR 3.99,CI:2.43-6.56;p<0.0001)。调整 Gleason 评分后,TFF3/PTEN 联合缺失与 OS(HR 2.33,CI:1.49-3.62;p<0.0001)和 PCSM(HR=3.44,CI:1.75-6.78,p<0.0001)最相关。
结论
本研究首次记录了在不接受手术干预的患者中,TFF3 表达和 PTEN 缺失的联合状态与 OS 和 PCSM 之间存在显著关联。对 PTEN 和 TFF3 的前瞻性评估可能进一步深入了解前列腺癌的分子亚型,并有助于分层有致命疾病风险的患者。
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