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首页> 外文期刊>The Journal of Urology >Clinical usefulness of serum prostate specific antigen for the detection of prostate cancer is preserved in men receiving the dual 5alpha-reductase inhibitor dutasteride.
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Clinical usefulness of serum prostate specific antigen for the detection of prostate cancer is preserved in men receiving the dual 5alpha-reductase inhibitor dutasteride.

机译:接受双重5α-还原酶抑制剂度他雄胺的男性保留了血清前列腺特异性抗原在检测前列腺癌中的临床实用性。

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PURPOSE: We determined whether the decrease in serum PSA seen with 5alpha-reductase inhibitors affects the clinical usefulness of PSA for prostate cancer screening using data from 2 dutasteride benign prostatic hyperplasia studies. MATERIALS AND METHODS: A total of 2,802 men 50 years or older with a clinical diagnosis of benign prostatic hyperplasia, no history of prostate cancer, PSA 1.5 to 10 ng/ml, prostate volume 30 cc or greater, an American Urological Association symptom score of 12 or greater and peak urinary flow rate 15 ml per second or less were randomized to 0.5 mg dutasteride daily or matching placebo for 24 months. Increases in PSA from baseline and the maximum increase from nadir to month 24 were compared between the groups and analyzed by prostate cancer status, as determined by PSA driven biopsy and an advised cutoff of more than 4 ng/ml after doubling to correct for dutasteride treatment with sensitivity and specificity calculated for each. RESULTS: In placebo treated men without prostate cancer there was an 8.3% median increase in PSA at month 24 compared with -59.5% in those who received dutasteride, using doubled values to correct for dutasteride treatment. In those with prostate cancer these changes were 23.8% and -37.2%, respectively. Using the upper PSA limit of 4 ng/ml sensitivity for prostate cancer in men receiving dutasteride vs placebo was 0.737 vs 0.804, while specificity was 0.671 vs 0.578. Using a PSA increase from nadir of 0.8 ng/ml the sensitivity of dutasteride was 0.548 and its specificity was 0.795. CONCLUSIONS: A doubling factor is effective for maintaining the sensitivity and specificity of PSA for prostate cancer detection in men on dutasteride. Increases in serum PSA in men receiving dutasteride should be considered suspicious and serial PSA measurements should be used to evaluate changes from nadir.
机译:目的:我们使用来自2个dutasteride良性前列腺增生研究的数据,确定了5α-还原酶抑制剂引起的血清PSA降低是否影响PSA对前列腺癌筛查的临床有效性。材料与方法:共有2,802名50岁以上的男性,临床诊断为良性前列腺增生,无前列腺癌病史,PSA 1.5至10 ng / ml,前列腺体积30 cc或更高,美国泌尿外科协会症状评分为12个月或以上,峰值尿流率15毫升/秒或更少,随机分配至0.5毫克度他雄胺每天或24个月匹配安慰剂。比较两组之间从基线的PSA升高和从最低点到第24个月的最大升高,并通过PSA驱动的活检和加倍校正度他雄胺治疗后建议的大于4 ng / ml的临界值,通过前列腺癌状态进行分析。并计算出每种药物的敏感性和特异性。结果:在接受安慰剂治疗的无前列腺癌的男性中,PSA的中位值在24个月时增加了8.3%,而接受dutasteride的患者则为-59.5%,使用双倍值校正dutasteride的治疗。在前列腺癌患者中,这些变化分别为23.8%和-37.2%。使用接受度他雄胺和安慰剂治疗的男性的前列腺癌敏感性PSA上限为4 ng / ml,特异性为0.737 vs 0.804,特异性为0.671 vs 0.578。使用从最低点0.8 ng / ml增加的PSA,度他雄胺的敏感性为0.548,其特异性为0.795。结论:倍增因子可有效维持PSA对度他雄胺男性前列腺癌检测的敏感性和特异性。接受度他雄胺治疗的男性血清PSA升高应被认为是可疑的,并且应使用一系列PSA测量来评估最低点的变化。

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