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前列腺癌预防试验中检测到的癌症的病理特征:对前列腺癌检测和化学预防的意义。

Pathologic characteristics of cancers detected in The Prostate Cancer Prevention Trial: implications for prostate cancer detection and chemoprevention.

作者信息

Lucia M Scott, Darke Amy K, Goodman Phyllis J, La Rosa Francisco G, Parnes Howard L, Ford Leslie G, Coltman Charles A, Thompson Ian M

机构信息

University of Colorado Denver School of Medicine, Aurora, Colorado 80045, USA.

出版信息

Cancer Prev Res (Phila). 2008 Aug;1(3):167-73. doi: 10.1158/1940-6207.CAPR-08-0078. Epub 2008 May 18.

Abstract

The Prostate Cancer Prevention Trial (PCPT) showed a risk of prostate cancer at prostate-specific antigen (PSA) <4.0 ng/mL and that prostate cancer risk is reduced by finasteride. A major concern about early detection by PSA and prevention by finasteride is that they may involve biologically inconsequential tumors. We reviewed the pathologic characteristics of prostate biopsies from men in the placebo and finasteride groups of the PCPT. We examined tumor pathology characteristics stratified by level of PSA for men in the placebo group who underwent radical prostatectomy. Seventy-five percent of all cancers and 62% of Gleason score <or=6 cancers in the PCPT met the biopsy criteria for clinically significant tumors. Surrogate measures for tumor volume (number of cores positive, percent cores positive, linear extent, and bilaterality) and risk of perineural invasion were lower in men who received finasteride. The PSA-associated risks of insignificant cancer were 51.7% (PSA, 0-1.0 ng/mL), 33.7% (1.1-2.5 ng/mL), 17.8% (2.6-4.0 ng/mL), and 11.7% (4.1-10 ng/mL). Conversely, the risks of high-grade (Gleason score >or=7) tumors for the same PSA strata were 15.6%, 37.9%, 49.1%, and 52.4%, respectively. These data highlight the dilemma of PSA when used for screening: Lower cutoff levels increase detection of insignificant disease, but cure is more likely, whereas higher cutoff levels make detection of significant cancer more likely, but cure is less likely. Therefore, the effectiveness of finasteride in preventing prostate cancer, including Gleason score <or=6 cancer, with meaningful rates of significant disease in the PCPT suggests that cutoff values for PSA screening should be individualized and that men undergoing screening should be informed of the opportunity to reduce their risk of disease with finasteride.

摘要

前列腺癌预防试验(PCPT)表明,在前列腺特异性抗原(PSA)<4.0 ng/mL时存在前列腺癌风险,且非那雄胺可降低前列腺癌风险。对通过PSA进行早期检测以及通过非那雄胺进行预防的一个主要担忧是,它们可能涉及生物学上无关紧要的肿瘤。我们回顾了PCPT安慰剂组和非那雄胺组男性前列腺活检的病理特征。我们检查了接受根治性前列腺切除术的安慰剂组男性按PSA水平分层的肿瘤病理特征。PCPT中所有癌症的75%以及Gleason评分≤6分的癌症的62%符合临床显著肿瘤的活检标准。接受非那雄胺治疗的男性肿瘤体积的替代指标(阳性芯数量、阳性芯百分比、线性范围和双侧性)以及神经周围侵犯风险较低。PSA相关的无意义癌症风险分别为51.7%(PSA,0 - 1.0 ng/mL)、33.7%(1.1 - 2.5 ng/mL)、17.8%(2.6 - 4.0 ng/mL)和11.7%(4.1 - 10 ng/mL)。相反,相同PSA分层的高级别(Gleason评分≥7分)肿瘤风险分别为15.6%、37.9%、49.1%和52.4%。这些数据凸显了PSA用于筛查时的困境:较低的临界值增加了对无意义疾病的检测,但治愈的可能性更大;而较高的临界值使检测到显著癌症的可能性更大,但治愈的可能性更小。因此,非那雄胺在预防前列腺癌(包括Gleason评分≤6分癌症)方面的有效性,以及PCPT中有意义的显著疾病发生率表明,PSA筛查的临界值应个体化,并且接受筛查的男性应被告知有机会通过非那雄胺降低疾病风险。

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本文引用的文献

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What to do with an abnormal PSA test.PSA检测结果异常该怎么办。
Oncologist. 2008 Mar;13(3):299-305. doi: 10.1634/theoncologist.2007-0139.
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Cancer statistics, 2008.2008年癌症统计数据。
CA Cancer J Clin. 2008 Mar-Apr;58(2):71-96. doi: 10.3322/CA.2007.0010. Epub 2008 Feb 20.

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