首页> 外文期刊>The Journal of Urology >Androgen receptor gene amplification at primary progression predicts response to combined androgen blockade as second line therapy for advanced prostate cancer.
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Androgen receptor gene amplification at primary progression predicts response to combined androgen blockade as second line therapy for advanced prostate cancer.

机译:雄激素受体基因在主要进程中的扩增可预测对联合雄激素阻断的反应,作为晚期前列腺癌的二线治疗。

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PURPOSE: Amplification of the androgen receptor gene has been found in a third of hormone refractory prostate carcinomas. It is possible that amplification facilitates cell growth ability in low concentrations of androgens remaining in the serum after androgen deprivation therapy. We evaluate whether androgen receptor gene amplification at primary progression is associated with response to second line combined androgen blockade for prostate cancer. MATERIALS AND METHODS: A total of 77 patients with prostate cancer were treated initially with androgen deprivation monotherapy followed by combined androgen blockade after the first progression. After initiation of second line combined androgen blockade patients were followed every 3 months to evaluate treatment responses. Biopsies were taken from the prostate at the first progression under endocrine monotherapy. Androgen receptor gene copy number was determined by fluorescence in situ hybridization. RESULTS: Androgen receptor gene amplification was found in 10 of the 77 cases (13%) at the primary disease progression, and was associated with a favorable response to second line combined androgen blockade. Only 1 of 34 (3%) patients classified as nonresponders had androgen receptor gene amplification, whereas 9 of 41 (21%) classified as having either stable disease or response had amplification (p = 0.016). Patients with androgen receptor gene amplification also had a decrease in prostate specific antigen more often after combined androgen blockade than those with no amplification (p = 0.079). However, androgen receptor gene amplification was not associated with patient survival after the first progression. CONCLUSIONS: Androgen receptor gene amplification detected in tumors progressing during androgen deprivation monotherapy is associated with favorable treatment response to second line combined androgen blockade. This finding suggests that at least some androgen receptor amplified tumors retain a high degree of dependency on residual androgens remaining in serum after monotherapy.
机译:目的:在三分之一的激素难治性前列腺癌中发现了雄激素受体基因的扩增。雄激素剥夺治疗后,扩增可能会促进血清中残留的低浓度雄激素的细胞生长能力。我们评估雄激素受体基因扩增在主要进展是否与对前列腺癌的二线联合雄激素阻断反应有关。材料与方法:总共77例前列腺癌患者最初接受雄激素剥夺单药治疗,然后在首次进展后进行联合雄激素阻断治疗。在开始二线联合雄激素阻断治疗后,每3个月随访患者以评估治疗反应。在内分泌单一疗法的第一个进展中从前列腺取活检。通过荧光原位杂交确定雄激素受体基因拷贝数。结果:在原发疾病进展的77例病例中,有10例(13%)发现了雄激素受体基因扩增,并且与二线联合雄激素阻断的良好反应相关。被分类为无反应的34名患者中只有1名(3%)具有雄激素受体基因扩增,而被分类为疾病稳定或有响应的41名中有9名(21%)具有扩增(p = 0.016)。雄激素受体基因扩增的患者与未扩增的男性相比,联合雄激素阻断后前列腺特异性抗原的减少也更多(p = 0.079)。然而,雄激素受体基因的扩增与患者在首次进展后的存活率无关。结论:在雄激素剥夺单药治疗期间进展中的肿瘤中检测到的雄激素受体基因扩增与对二线联合雄激素阻断的良好治疗反应相关。这一发现表明,至少一些雄激素受体扩增的肿瘤在单药治疗后仍然对血清中残留的雄激素有高度依赖性。

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