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Risk Stratification after Biochemical Failure following Curative Treatment of Locally Advanced Prostate Cancer: Data from the TROG 96.01 Trial

机译:局部晚期前列腺癌的治疗后生化失败后的风险分层:TROG 96.01试验数据

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Purpose. Survival following biochemical failure is highly variable. Using a randomized trial dataset, we sought to define a risk stratification scheme in men with locally advanced prostate cancer (LAPC).Methods. The TROG 96.01 trial randomized 802 men with LAPC to radiation ± neoadjuvant androgen suppression therapy (AST) between 1996 and 2000. Ten-year follow-up data was used to develop three-tier post-biochemical failure risk stratification schemes based on cutpoints of time to biochemical failure (TTBF) and PSA doubling time (PSADT). Schemes were evaluated in univariable, competing risk models for prostate cancer-specific mortality. The performance was assessed by c-indices and internally validated by the simple bootstrap method. Performance rankings were compared in sensitivity analyses using multivariable models and variations in PSADT calculation.Results. 485 men developed biochemical failure. c-indices ranged between 0.630 and 0.730. The most discriminatory scheme had a high risk category defined by PSADT < 4 months or TTBF < 1 year and low risk category by PSADT > 9 months or TTBF > 3 years.Conclusion. TTBF and PSADT can be combined to define risk stratification schemes after biochemical failure in men with LAPC treated with short-term AST and radiotherapy. External validation, particularly in long-term AST and radiotherapy datasets, is necessary.
机译:目的。生化失败后的生存率差异很大。使用随机试验数据集,我们试图定义局部晚期前列腺癌(LAPC)男性的风险分层方案。 TROG 96.01试验在1996年至2000年之间将802例LAPC患者随机分配接受放射±新辅助雄激素抑制疗法(AST)。十年的随访数据用于根据时间点制定三级生化失败后风险分层方案生化衰竭(TTBF)和PSA加倍时间(PSADT)。在针对前列腺癌特异性死亡率的单变量,竞争性风险模型中评估了方案。性能由c-indices评估,并通过简单的bootstrap方法进行内部验证。使用多变量模型和PSADT计算中的变量在敏感性分析中比较了性能排名。 485名男子发生了生化衰竭。 c指数介于0.630和0.730之间。最具歧视性的方案是由PSADT <4个月或TTBF <1年定义的高风险类别,由PSADT> 9个月或TTBF> 3年定义的低风险类别。可以将TTBF和PSADT结合起来,以定义经短期AST和放疗治疗的LAPC男性生化失败后的风险分层方案。必须进行外部验证,尤其是在长期AST和放射治疗数据集中。

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