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非肌层浸润性膀胱癌进展的分子生物标志物——超越传统风险分层

Molecular biomarkers of progression in non-muscle-invasive bladder cancer - beyond conventional risk stratification.

作者信息

Olislagers Mitchell, de Jong Florus C, Rutten Vera C, Boormans Joost L, Mahmoudi Tokameh, Zuiverloon Tahlita C M

机构信息

Department of Urology, Erasmus University Medical Center, Erasmus MC Cancer Institute, Rotterdam, the Netherlands.

Department of Pathology, Erasmus University Medical Center, Rotterdam, the Netherlands.

出版信息

Nat Rev Urol. 2025 Feb;22(2):75-91. doi: 10.1038/s41585-024-00914-7. Epub 2024 Aug 2.

Abstract

The global incidence of bladder cancer is more than half a million diagnoses each year. Bladder cancer can be categorized into non-muscle-invasive bladder cancer (NMIBC), which accounts for ~75% of diagnoses, and muscle-invasive bladder cancer (MIBC). Up to 45% of patients with NMIBC develop disease progression to MIBC, which is associated with a poor outcome, highlighting a clinical need to identify these patients. Current risk stratification has a prognostic value, but relies solely on clinicopathological parameters that might not fully capture the complexity of disease progression. Molecular research has led to identification of multiple crucial players involved in NMIBC progression. Identified biomarkers of progression are related to cell cycle, MAPK pathways, apoptosis, tumour microenvironment, chromatin stability and DNA-damage response. However, none of these biomarkers has been prospectively validated. Reported gene signatures of progression do not improve NMIBC risk stratification. Molecular subtypes of NMIBC have improved our understanding of NMIBC progression, but these subtypes are currently unsuitable for clinical implementation owing to a lack of prospective validation, limited predictive value as a result of intratumour subtype heterogeneity, technical challenges, costs and turnaround time. Future steps include the development of consensus molecular NMIBC subtypes that might improve conventional clinicopathological risk stratification. Prospective implementation studies of biomarkers and the design of biomarker-guided clinical trials are required for the integration of molecular biomarkers into clinical practice.

摘要

全球每年膀胱癌的确诊病例超过50万例。膀胱癌可分为非肌层浸润性膀胱癌(NMIBC)和肌层浸润性膀胱癌(MIBC),其中NMIBC约占确诊病例的75%。高达45%的NMIBC患者会进展为MIBC,这与不良预后相关,凸显了识别这些患者的临床需求。目前的风险分层具有预后价值,但仅依赖于可能无法完全反映疾病进展复杂性的临床病理参数。分子研究已导致识别出多个参与NMIBC进展的关键因素。已确定的进展生物标志物与细胞周期、丝裂原活化蛋白激酶(MAPK)通路、细胞凋亡、肿瘤微环境、染色质稳定性和DNA损伤反应有关。然而,这些生物标志物均未经过前瞻性验证。报道的进展基因特征并不能改善NMIBC的风险分层。NMIBC的分子亚型增进了我们对NMIBC进展的理解,但由于缺乏前瞻性验证、肿瘤内亚型异质性导致的预测价值有限、技术挑战、成本和周转时间等原因,这些亚型目前不适合临床应用。未来的步骤包括开发可能改善传统临床病理风险分层的共识分子NMIBC亚型。将分子生物标志物整合到临床实践中需要进行生物标志物的前瞻性实施研究以及设计生物标志物指导的临床试验。

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