非肌肉浸润性尿路上皮癌预后的新标志物和当代标志物。

Korean Journal of Urology Pub Date : 2015-08-01 Epub Date: 2015-07-31 DOI:10.4111/kju.2015.56.8.553
M Hammad Ather, Syed M Nazim
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引用次数: 9

摘要

非肌肉侵袭性(NMI)尿路上皮癌(UC)与多种生物潜能相关。它的特点是经常复发和进展,从而使肿瘤预后恶化。近四分之三的NMI uc在5年内复发,而一半在随访期间可以进展。进展尤其见于T1和原位癌(CIS)。毫无疑问,NMI UC是治疗成本最高的癌症之一。欧洲癌症研究和治疗组织(EORTC)风险计算器是评估新诊断癌症复发和进展潜力的常用工具。用于评估的参数是肿瘤的大小和数量,肿瘤的病理分期和分级,是否存在CIS和既往复发率。EORTC工具的主要优点是易于使用和不需要运行昂贵的分子测试。然而,病理分期和分级的可重复性是适度的,这是临床医生关注的问题。鉴于临床病理变量不足以预测个体的预后,分子标记物有可能预测NMI UC的临床结果。在过去的20年里,在理解膀胱癌的分子生物学方面做了大量的工作;然而,这些知识的翻译价值仍然很差。分子标记在预测复发方面的作用似乎有限,因为多灶性疾病和不完全治疗可能比切除肿瘤的分子特征对复发更重要。尿液标志物在膀胱癌预后中的价值非常有限,并且(主要作为细胞学的辅助)用于检测和监测尿路上皮细胞癌复发。用分子标记物预测进展具有相当大的前景。然而,分子标志物在临床病理指标上的当代价值是有限的。
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New and contemporary markers of prognosis in nonmuscle invasive urothelial cancer.

Nonmuscle invasive (NMI) urothelial cancer (UC) is associated with varied biological potential. It is characterized by frequent recurrence and progression, which thus worsens the oncological outcome. Nearly three-quarters of NMI UCs recur within 5 years, whereas half can progress during follow-up. Progression is particularly seen in T1 and carcinoma in situ (CIS). Undoubtedly, NMI UC is one of the most expensive cancers to manage. The European Organisation for Research and Treatment of Cancer (EORTC) risk calculator is a commonly used tool for assessing the recurrence and progression potential of a newly diagnosed cancer. The parameters used in the assessment are tumor size and number, pathological stage and grade of the cancer, presence of CIS, and prior recurrence rate. The main advantages of the EORTC tool are its ease of use and the lack of need to run expensive molecular tests. However, reproducibility of pathologic stage and grade is modest, which is a concern to clinicians. Molecular markers have potential for predicting the clinical outcome of NMI UC, given that clinico-pathologic variables are not sufficient for prediction of prognosis in an individual. Significant work has been done in the past 2 decades in understanding the molecular biology of bladder cancer; however, the translational value of this knowledge remains poor. The role for molecular markers in predicting recurrence seems limited because multifocal disease and incomplete treatment are probably more important for recurrence than the molecular features of a resected tumor. Urinary markers have very limited value in prognostication of bladder cancer and are used (mainly as an adjunct to cytology) for detection and surveillance of urothelial cell cancer recurrence. Prediction of progression with molecular markers holds considerable promise. Nevertheless, the contemporary value of molecular markers over clinico-pathologic indexes is limited.

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