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循环染色体构象特征显著提高前列腺癌检测的PSA阳性预测价值和总体准确率。

Circulating Chromosome Conformation Signatures Significantly Enhance PSA Positive Predicting Value and Overall Accuracy for Prostate Cancer Detection.

作者信息

Pchejetski Dmitri, Hunter Ewan, Dezfouli Mehrnoush, Salter Matthew, Powell Ryan, Green Jayne, Naithani Tarun, Koutsothanasi Christina, Alshaker Heba, Jaipuria Jiten, Connor Martin J, Eldred-Evans David, Fiorentino Francesca, Ahmed Hashim, Akoulitchev Alexandre, Winkler Mathias

机构信息

School of Medicine, University of East Anglia, Norwich NR4 7TJ, UK.

Oxford BioDynamics Limited, Oxford OX4 2WB, UK.

出版信息

Cancers (Basel). 2023 Jan 29;15(3):821. doi: 10.3390/cancers15030821.

Abstract

BACKGROUND

Prostate cancer (PCa) has a high lifetime prevalence (one out of six men), but currently there is no widely accepted screening programme. Widely used prostate specific antigen (PSA) test at cut-off of 3.0 ng/mL does not have sufficient accuracy for detection of any prostate cancer, resulting in numerous unnecessary prostate biopsies in men with benign disease and false reassurance in some men with PCa. We have recently identified circulating chromosome conformation signatures (CCSs, Episwitch PCa test) allowing PCa detection and risk stratification in line with standards of clinical PCa staging. The purpose of this study was to determine whether combining the Episwitch PCa test with the PSA test will increase its diagnostic accuracy.

METHODS

= 109 whole blood samples of men enrolled in the PROSTAGRAM screening pilot study and = 38 samples of patients with established PCa diagnosis and cancer-negative controls from Imperial College NHS Trust were used. Samples were tested for PSA, and the presence of CCSs in the loci encoding for of , , , , and associated with high-risk PCa identified in our previous work.

RESULTS

PSA > 3 ng/mL alone showed a low positive predicted value (PPV) of 0.14 and a high negative predicted value (NPV) of 0.93. EpiSwitch alone showed a PPV of 0.91 and a NPV of 0.32. Combining PSA and Episwitch tests has significantly increased the PPV to 0.81 although reducing the NPV to 0.78. Furthermore, integrating PSA, as a continuous variable (rather than a dichotomised 3 ng/mL cut-off), with EpiSwitch in a new multivariant stratification model, Prostate Screening EpiSwitch (PSE) test, has yielded a remarkable combined PPV of 0.92 and NPV of 0.94 when tested on the independent prospective cohort.

CONCLUSIONS

Our results demonstrate that combining the standard PSA readout with circulating chromosome conformations (PSE test) allows for significantly enhanced PSA PPV and overall accuracy for PCa detection. The PSE test is accurate, rapid, minimally invasive, and inexpensive, suggesting significant screening diagnostic potential to minimise unnecessary referrals for expensive and invasive MRI and/or biopsy testing. Further extended prospective blinded validation of the new combined signature in a screening cohort with low cancer prevalence would be the recommended step for PSE adoption in PCa screening.

摘要

背景

前列腺癌(PCa)终生患病率较高(六分之一男性),但目前尚无广泛接受的筛查方案。广泛使用的前列腺特异性抗原(PSA)检测,其临界值为3.0 ng/mL,对于检测所有前列腺癌的准确性不足,导致许多患有良性疾病的男性接受了不必要的前列腺活检,而一些患有PCa的男性则得到了错误的安心结果。我们最近发现了循环染色体构象特征(CCSs,Episwitch PCa检测),可根据临床PCa分期标准进行PCa检测和风险分层。本研究的目的是确定将Episwitch PCa检测与PSA检测相结合是否会提高其诊断准确性。

方法

使用了参加PROSTAGRAM筛查试点研究的109名男性的全血样本,以及来自帝国理工学院国民保健服务信托基金的38例已确诊PCa患者和癌症阴性对照的样本。对样本进行PSA检测,并检测我们之前工作中确定的与高危PCa相关的、、、、和基因座中CCSs的存在情况。

结果

单独PSA>3 ng/mL显示出较低的阳性预测值(PPV)为0.14和较高的阴性预测值(NPV)为0.93。单独的EpiSwitch显示PPV为0.91,NPV为0.32。将PSA和EpiSwitch检测相结合,显著提高了PPV至0.81,尽管NPV降至0.78。此外,在新的多变量分层模型前列腺筛查EpiSwitch(PSE)检测中,将PSA作为连续变量(而非二分的3 ng/mL临界值)与EpiSwitch整合,在独立的前瞻性队列中进行测试时,产生了显著的联合PPV为0.92和NPV为0.94。

结论

我们的结果表明,将标准PSA读数与循环染色体构象(PSE检测)相结合,可显著提高PSA的PPV和PCa检测的总体准确性。PSE检测准确、快速、微创且廉价,表明其具有显著的筛查诊断潜力,可将昂贵且侵入性的MRI和/或活检检测的不必要转诊降至最低。在癌症患病率较低的筛查队列中对新的联合特征进行进一步扩展的前瞻性盲法验证,将是PSE应用于PCa筛查的推荐步骤。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7f5a/9913359/67a3f732668e/cancers-15-00821-g001.jpg

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