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线粒体 DNA 缺失检测可准确预测前列腺重复活检结果。

Accurate prediction of repeat prostate biopsy outcomes by a mitochondrial DNA deletion assay.

机构信息

Genesis Genomics, Thunder Bay, ON, Canada.

出版信息

Prostate Cancer Prostatic Dis. 2010 Jun;13(2):126-31. doi: 10.1038/pcan.2009.64. Epub 2010 Jan 19.

DOI:10.1038/pcan.2009.64
PMID:20084081
Abstract

Several cancers are characterized by large-scale mtDNA deletions. We previously provided evidence that one of these deletions has potential utility in resolving false from true-negative prostate needle biopsies. This study was to assess the clinical value of this deletion in predicting re-biopsy outcomes. We used a quantitative polymerase chain reaction assay to measure the levels of the deletion in individual negative needle biopsies from 101 patients who had a repeat biopsy within a year with known outcomes. Using an empirically established cycle threshold (Ct) cutoff of 31, and the lowest Ct for each patient as diagnostic of prostate cancer, as well as the histopathologic diagnosis on second biopsy, we calculated the clinical performance of the deletion. The Ct cutoff at 31 gave a sensitivity and specificity of 84 and 54%, respectively, with the area under a receiver-operating characteristics curve of 0.749. The negative predictive value was 91%. The assay was able to predict the presence of a missed tumor in 17 out of 20 men a year before diagnosis. This ancillary test appears to identify men who do not require a repeat biopsy with a high degree of certainty. The results suggest that the majority of men with atypical small acinar proliferation have a concurrent missed tumor and therefore require close monitoring for early detection.

摘要

几种癌症的特点是大规模的 mtDNA 缺失。我们之前提供的证据表明,这些缺失之一在确定前列腺针吸活检的假阴性和真阴性方面具有潜在的应用价值。本研究旨在评估该缺失在预测再次活检结果中的临床价值。我们使用定量聚合酶链反应(PCR)测定法,测量了 101 例患者的个别阴性针吸活检中该缺失的水平,这些患者在一年内有已知结果的重复活检。使用经验建立的循环阈值(Ct)截止值 31,并将每个患者的最低 Ct 值诊断为前列腺癌,以及第二次活检的组织病理学诊断,我们计算了缺失的临床性能。Ct 截止值为 31 时,敏感性和特异性分别为 84%和 54%,接收者操作特性曲线下的面积为 0.749。阴性预测值为 91%。该检测能够在诊断前一年预测出 20 名男性中有 17 名存在漏诊肿瘤。该辅助检测似乎能够非常确定地识别出不需要重复活检的男性。结果表明,大多数具有非典型小腺泡增生的男性都存在同时漏诊的肿瘤,因此需要密切监测以早期发现。

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