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Expression of the Androgen-Regulated Fusion Gene TMPRSS2-ERG Does Not Predict Response to Endocrine Treatment in Hormone-Naive, Node-Positive Prostate Cancer

机译:雄激素调节的融合基因TMPRSS2-ERG的表达不能预测激素原发性,淋巴结阳性的前列腺癌对内分泌治疗的反应。

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Background: Fusion of the androgen-regulated gene transmembrane protease, serine 2, TMPRSS2, to the v-ets erythroblastosis virus E26 oncogene homolog (avian), ERG, of the erythroblast transformation-specific (ETS) family is the most common genetic alteration in prostate cancer (PCa). Objective: To determine whether expression of androgen-regulated TMPRSS2-ERG predicts response to endocrine treatment in hormone-naive, node-positive PCa. Design, setting, and participants: Eighty-five patients with histologically confirmed, node-positive PCa who were without treatment at the moment of lymph node dissection were analysed. RNA was isolated from the paraffin-embedded lymph node metastases and complementary DNA (cDNA) was made. The quality of cDNA was tested by polymerase chain reaction (PCR) analysis of the expression of the housekeeping gene hydroxymethylbilane synthase, HMBS (formerly PBGD). TMPRSS2-ERG expression was analysed by PCR using a forward primer in TMPRSS2 exon 1 and a reverse primer in ERG exon 4. Measurements: The primary end point was time from start of endocrine therapy to the occurrence of three consecutive rises in prostate-specific antigen (PSA) that were at least 2 wk apart and resulted in two 50% increases over the PSA nadir. Secondary end points were time to PSA nadir after start of endocrine treatment and cancer-specific and overall survival. Results and limitations: TMPRSS2-ERG was expressed in 59% of the 71 patients who could be analysed. Median duration of response to endocrine therapy was 20.9 mo versus 24.1 mo for gene fusion-positive versus gene fusion-negative patients (95% confidence intervals: 18.6-23.1 vs 18.9-29.4, p = 0.70). Furthermore, no significant differences were seen between the two groups for the secondary end points. Conclusions: Expression of TMPRSS2-ERG is frequent in lymph node metastases of patients with untreated PCa; however, expression of this androgen-regulated fusion gene did not correspond with duration of response to endocrine therapy. Our results suggest that expression of TMPRSS2-ERG is not a candidate marker to select for metastatic PCa patients who will benefit more from endocrine treatment.
机译:背景:雄激素调节基因跨膜蛋白酶丝氨酸2,TMPRSS2与成红细胞转化特异性(ETS)家族的v-ets成红细胞病病毒E26癌基因同源物(禽)ERG的融合前列腺癌(PCa)。目的:确定雄激素调节型TMPRSS2-ERG的表达是否可预测未接受过激素的淋巴结阳性的PCa对内分泌治疗的反应。设计,设置和参与者:分析了在淋巴结清扫时未经治疗的经组织学证实的85例淋巴结阳性的PCa患者。从石蜡包埋的淋巴结转移中分离出RNA,并制备了互补DNA(cDNA)。通过看家基因羟甲基胆烷合酶HMBS(以前称为PBGD)的表达的聚合酶链反应(PCR)分析来测试cDNA的质量。通过使用TMPRSS2外显子1中的正向引物和ERG外显子4中的反向引物,通过PCR分析TMPRSS2-ERG的表达。测量:主要终点是从开始内分泌治疗到前列腺特异性抗原连续三次升高的时间。 (PSA)至少相隔2周,并且比PSA最低点增加了两个50%。次要终点是开始内分泌治疗以及癌症特异性和总体生存后达到PSA最低点的时间。结果与局限性:在可以分析的71例患者中,有59%表达了TMPRSS2-ERG。基因融合阳性和基因融合阴性的患者对内分泌治疗的反应时间中位数为20.9 mo,而基因融合阴性患者的中位响应时间为24.1 mo(95%置信区间:18.6-23.1 vs 18.9-29.4,p = 0.70)。此外,两组在次要终点方面无明显差异。结论:未经治疗的PCa患者的淋巴结转移中TMPRSS2-ERG的表达频繁。然而,这种雄激素调节的融合基因的表达与内分泌治疗的反应持续时间不符。我们的结果表明,TMPRSS2-ERG的表达不是选择转移性PCa患者的候选标记,后者将从内分泌治疗中受益更多。

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