The Association of the Long Prostate Cancer Expressed PDE4D Transcripts to Poor Patient Outcome Depends on the Tumour's TMPRSS2-ERG Fusion Status.

IF 2.3 Q3 ONCOLOGY
Prostate Cancer Pub Date : 2019-06-02 eCollection Date: 2019-01-01 DOI:10.1155/2019/8107807
Dianne van Strijp, Christiane de Witz, Birthe Heitkötter, Sebastian Huss, Martin Bögemann, George S Baillie, Miles D Houslay, Chris Bangma, Axel Semjonow, Ralf Hoffmann
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引用次数: 6

Abstract

Objectives: To investigate the added value of assessing transcripts for the long cAMP phosphodiesterase-4D (PDE4D) isoforms, PDE4D5 and PDE4D9, regarding the prognostic power of the 'CAPRA & PDE4D7' combination risk model to predict longitudinal postsurgical biological outcomes in prostate cancer.

Patients and methods: RNA was extracted from both biopsy punches of resected tumours (606 patients; RP cohort) and diagnostic needle biopsies (168 patients; DB cohort). RT-qPCR was performed in order to determine PDE4D5, PDE4D7, and PDE4D9 transcript scores in both study cohorts. By RNA sequencing, we determined the TMPRSS2-ERG fusion status of each tumour sample in the RP cohort. Kaplan-Meier survival analyses were then applied to correlate the PDE4D5, PDE4D7 and PDE4D9 scores with postsurgical patient outcomes. Logistic regression was then used to combine the clinical CAPRA score with PDE4D5, PDE4D7, and PDE4D9 scores in order to build a 'CAPRA & PDE4D5/7/9' regression model. ROC and decision curve analysis was used to estimate the net benefit of the 'CAPRA & PDE4D5/7/9' risk model.

Results: Kaplan-Meier survival analysis, on the RP cohort, revealed a significant association of the PDE4D7 score with postsurgical biochemical recurrence (BCR) in the presence of the TMPRSS2-ERG gene rearrangement (logrank p<0.0001), compared to the absence of this gene fusion event (logrank p=0.08). In contrast, the PDE4D5 score was only significantly associated with BCR in TMPRSS2-ERG fusion negative tumours (logrank p<0.0001 vs. logrank p=0.4 for TMPRSS2-ERG+ tumours). This was similar for the PDE4D9 score although less pronounced compared to that of the PDE4D5 score (TMPRSS2ERG- logrank p<0.0001 vs. TMPRSS2ERG+ logrank p<0.005). In order to predict BCR after primary treatment, we undertook ROC analysis of the logistic regression combination model of the CAPRA score with the PDE4D5, PDE4D7, and PDE4D9 scores. For the DB cohort, this demonstrated significant differences in the AUC between the CAPRA and the PDE4D5/7/9 regression model vs. the CAPRA and PDE4D7 risk model (AUC 0.87 vs. 0.82; p=0.049) vs. the CAPRA score alone (AUC 0.87 vs. 0.77; p=0.005). The CAPRA and PDE4D5/7/9 risk model stratified 19.2% patients of the DB cohort to either 'no risk of biochemical relapse' (NPV 100%) or the 'start of any secondary treatment (NPV 100%)', over a follow-up period of up to 15 years. Decision curve analysis presented a clear, net benefit for the use of the novel CAPRA & PDE4D5/7/9 risk model compared to the clinical CAPRA score alone or the CAPRA and PDE4D7 model across all decision thresholds.

Conclusion: Association of the long PDE4D5, PDE4D7, and PDE4D9 transcript scores to prostate cancer patient outcome, after primary intervention, varies in opposite directions depending on the TMPRSS2-ERG genomic fusion background of the tumour. Adding transcript scores for the long PDE4D isoforms, PDE4D5 and PDE4D9, to our previously presented combination risk model of the combined 'CAPRA & PDE4D7' score, in order to generate the CAPRA and PDE4D5/7/9 score, significantly improves the prognostic power of the model in predicting postsurgical biological outcomes in prostate cancer patients.

Abstract Image

Abstract Image

Abstract Image

长前列腺癌表达PDE4D转录物与不良患者预后的关系取决于肿瘤的TMPRSS2-ERG融合状态。
目的:探讨评估长链cAMP磷酸二酯酶- 4d (PDE4D)亚型、PDE4D5和PDE4D9转录本的附加价值,以及“CAPRA & PDE4D7”联合风险模型在预测前列腺癌纵向术后生物学预后方面的预后能力。患者和方法:从切除肿瘤的两个活检孔中提取RNA(606例;RP队列)和诊断性针活检(168例患者;DB队列)。采用RT-qPCR测定两个研究队列中PDE4D5、PDE4D7和PDE4D9转录物得分。通过RNA测序,我们确定了RP队列中每个肿瘤样本的TMPRSS2-ERG融合状态。然后应用Kaplan-Meier生存分析将PDE4D5、PDE4D7和PDE4D9评分与术后患者预后相关联。然后采用Logistic回归将临床CAPRA评分与PDE4D5、PDE4D7、PDE4D9评分结合,构建“CAPRA & PDE4D5/7/9”回归模型。采用ROC和决策曲线分析对“CAPRA & PDE4D5/7/9”风险模型的净收益进行估计。结果:在RP队列中,Kaplan-Meier生存分析显示,在存在TMPRSS2-ERG基因重排的情况下,PDE4D7评分与术后生化复发(BCR)存在显著相关性(logrank p)。结论:经初步干预后,PDE4D5、PDE4D7和PDE4D9长转录本评分与前列腺癌患者预后的相关性,取决于肿瘤的TMPRSS2-ERG基因组融合背景,呈相反方向变化。将PDE4D长亚型PDE4D5和PDE4D9的转录本评分加入到我们之前提出的CAPRA & PDE4D7评分联合风险模型中,以生成CAPRA和PDE4D5/7/9评分,显著提高了该模型预测前列腺癌患者术后生物学预后的能力。
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来源期刊
Prostate Cancer
Prostate Cancer ONCOLOGY-
CiteScore
2.70
自引率
0.00%
发文量
9
审稿时长
13 weeks
期刊介绍: Prostate Cancer is a peer-reviewed, Open Access journal that provides a multidisciplinary platform for scientists, surgeons, oncologists and clinicians working on prostate cancer. The journal publishes original research articles, review articles, and clinical studies related to the diagnosis, surgery, radiotherapy, drug discovery and medical management of the disease.
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