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PCA3 测量在主动监测方案中预测短期活检进展的准确性。

Accuracy of PCA3 measurement in predicting short-term biopsy progression in an active surveillance program.

机构信息

Department of Urology, Johns Hopkins Medical Institutions, Baltimore, Maryland 21287, USA.

出版信息

J Urol. 2010 Feb;183(2):534-8. doi: 10.1016/j.juro.2009.10.003. Epub 2009 Dec 14.

DOI:10.1016/j.juro.2009.10.003
PMID:20006883
Abstract

PURPOSE

PCA3 is a prostate specific noncoding mRNA that is significantly over expressed in prostate cancer tissue. Urinary PCA3 levels have been associated with prostate cancer grade and extent, suggesting a possible role in monitoring patients on active surveillance. We assessed the relationship between PCA3 and prostate biopsy results in men in a surveillance program.

MATERIALS AND METHODS

Urine specimens were obtained from 294 men with prostate cancer enrolled in the Johns Hopkins surveillance program. The followup protocol included semiannual free and total prostate specific antigen measurements, digital rectal examination and annual surveillance prostate biopsy. Cox proportional hazards regression was used to evaluate the association between PCA3 results and progression on surveillance biopsy (defined as Gleason pattern 4 or 5, more than 2 positive biopsy cores or more than 50% involvement of any core with cancer).

RESULTS

Patients with progression on biopsy (12.9%) had a mean PCA3 score similar to that of those without progression (60.0 vs 50.8, p = 0.131). ROC analysis suggested that PCA3 alone could not be used to identify men with progression on biopsy (AUC 0.589, 95% CI 0.496-0.683, p = 0.076). After adjustment for age and date of diagnosis PCA3 was not significantly associated with progression on biopsy (p = 0.15).

CONCLUSIONS

In men with low risk prostate cancer who were carefully selected for surveillance the PCA3 score was not significantly associated with short-term biopsy progression. Further analysis is necessary to assess the usefulness of PCA3 in combination with other biomarkers or in selected subsets of patients undergoing surveillance.

摘要

目的

PCA3 是一种前列腺特异性非编码 mRNA,在前列腺癌组织中表达显著上调。尿 PCA3 水平与前列腺癌的分级和范围有关,提示其在监测主动监测患者方面可能具有一定作用。我们评估了 PCA3 与监测项目中男性前列腺活检结果之间的关系。

材料与方法

从参加约翰霍普金斯监测项目的 294 名前列腺癌男性患者中获得尿标本。随访方案包括每半年进行游离前列腺特异性抗原和总前列腺特异性抗原测量、直肠指检和每年进行监测性前列腺活检。采用 Cox 比例风险回归评估 PCA3 结果与监测性活检进展之间的关系(定义为 Gleason 模式 4 或 5、2 个以上阳性活检核心或任何核心的癌症浸润超过 50%)。

结果

活检进展的患者(12.9%)的平均 PCA3 评分与无进展患者相似(60.0 与 50.8,p=0.131)。ROC 分析表明,单独使用 PCA3 无法识别活检进展的男性(AUC 0.589,95%CI 0.496-0.683,p=0.076)。校正年龄和诊断日期后,PCA3 与活检进展无显著相关性(p=0.15)。

结论

在精心选择进行监测的低危前列腺癌男性中,PCA3 评分与短期活检进展无显著相关性。需要进一步分析以评估 PCA3 与其他生物标志物联合使用或在接受监测的特定患者亚组中的有用性。

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