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Diagnostic molecular markers predicting aggressive potential in low-grade prostate cancer

机译:预测低级前列腺癌的攻击性潜力的诊断分子标记

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Currently, clinicians rely on clinical nomograms to stratify progression risk at the time of diagnosis in patients with prostate cancer (CaP). However, these tools may not accurately distinguish aggressive potential in low-grade CaP. The current study determined the diagnostic potential of 3 molecular markers (ROCK1, RUNX3, and miR-301a) in terms of their ability to identify which low-grade tumors are likely to progress. Real-time PCR and immunohistochemical analysis were used to assess ROCK1, RUNX3, and miR-301a expression profiles in 118 serum and needle biopsy specimens. Expressions of ROCK1 and miR-301a were found to be significantly higher in Gleason 6 and 7 CaP as compared to BPH, while an inverse trend was observed with RUNX3. Further, incorporation of all 3 molecular markers significantly improved clinical nomograms? diagnostic accuracy and correlated with disease progression. Hence, in conclusion, the inclusion of these 3 molecular markers identified aggressive phenotype and predicted disease progression in low-grade CaP tumors at the time of diagnosis.
机译:目前,临床医生依靠临床列线图对前列腺癌(CaP)患者诊断时的进展风险进行分层。然而,这些工具可能无法准确区分低级CaP中的攻击性潜力。目前的研究确定了3种分子标记物(ROCK1、RUNX3和miR-301a)在识别哪些低度恶性肿瘤可能进展方面的诊断潜力。实时PCR和免疫组织化学分析用于评估118份血清和穿刺活检标本中ROCK1、RUNX3和miR-301a的表达谱。与BPH相比,Gleason 6和7 CaP中ROCK1和miR-301a的表达显著高于BPH,而RUNX3中观察到相反的趋势。此外,所有3种分子标记物的加入显著改善了临床列线图?诊断准确率和死亡率与疾病进展相关。因此,综上所述,纳入这3种分子标记物可在诊断时确定低级别CaP肿瘤的侵袭性表型并预测疾病进展。

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