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首页> 外文期刊>Cancer: A Journal of the American Cancer Society >Impact of recent screening on predicting the outcome of prostate cancer biopsy in men with elevated prostate-specific antigen: data from the European Randomized Study of Prostate Cancer Screening in Gothenburg, Sweden.
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Impact of recent screening on predicting the outcome of prostate cancer biopsy in men with elevated prostate-specific antigen: data from the European Randomized Study of Prostate Cancer Screening in Gothenburg, Sweden.

机译:最近筛查对预测前列腺特异性抗原升高的男性前列腺癌活检结果的影响:来自瑞典哥德堡前列腺癌筛查欧洲随机研究的数据。

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BACKGROUND: Risk models to predict prostate cancer on biopsy, whether they include only prostate-specific antigen (PSA) or other markers, are intended for use in all men of screening age. However, the association between PSA and cancer probably depends on a man's recent screening history. METHODS: The authors examined the effect of prior screening on the ability to predict the risk of prostate cancer by using a previously reported, 4-kallikrein panel that included total PSA, free PSA, intact PSA, and human kallikrein-related peptidase 2 (hK2). The study cohort comprised 1241 men in Gothenburg, Sweden who underwent biopsy for elevated PSA during their second or later visit for the European Randomized Study of Screening for Prostate Cancer. The predictive accuracy of the 4-kallikrein panel was calculated. RESULTS: Total PSA was not predictive of prostate cancer. The previously published 4-kallikrein model increased predictive accuracy compared with total PSA and age alone (area under the curve [AUC], 0.66 vs 0.51; P < .001) but was poorly calibrated and missed many cancers. A model that was developed with recently screened men provided important improvements in discrimination (AUC, 0.67 vs 0.56; P < .001). Using this model reduced the number of biopsies by 413 per 1000 men with elevated PSA, missed 60 of 216 low-grade cancers (Gleason score < or =6), but missed only 1 of 43 high-grade cancers. CONCLUSIONS: Previous participation in PSA screening dramatically changed the performance of statistical models that were designed to predict biopsy outcome. A 4-kallikrein panel was able to predict prostate cancer in men who had a recent screening history and provided independent confirmation that multiple kallikrein forms contribute important diagnostic information for men with elevated PSA. Cancer
机译:背景:风险模型预测活组织检查的前列腺癌,无论它们是否仅包括前列腺特异性抗原(PSA)或其他标记,旨在用于筛查年龄的所有人。然而,PSA和癌症之间的关联可能取决于男人最近的筛查历史。方法:作者检测了先前筛选对预测前列腺癌风险的效果,通过使用先前报道的4-kallikrein面板,包括总PSA,免费的PSA,完整PSA和人Kallikrein相关的肽酶2(HK2 )。研究队列包括瑞典哥德堡1241名男子,在欧洲筛查前列腺癌的欧洲随机研究中接受了升高的PSA活组织检查。计算了4-Kallikrein面板的预测精度。结果:总PSA未预测前列腺癌。此前发表的4-kallikrein模型与单独的总PSA和年龄相比(曲线[AUC]下的面积,0.66 Vs 0.51; p <.001)相比,预测精度增加了预测性准确度,但校准不良并错过了许多癌症。使用最近筛选的人开发的模型提供了重要的识别改进(AUC,0.67 Vs 0.56; P <.001)。使用该模型将活检数量减少413个具有升高的PSA的男性,错过了216个低级癌症的60名(Gleason得分<或= 6),但只错过了43种高级癌症中的1个。结论:以前参与PSA筛查显着改变了统计模型的性能,旨在预测活检结果。一个4-kallikrein小组能够预测具有最近筛选历史的男性的前列腺癌,并提供独立的确认,即多个Kallikrein形式为PSA升高的男性提供了重要的诊断信息。癌症

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