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Bladder cancer: translating molecular genetic insights into clinical practice.

机译:膀胱癌:将分子遗传学见解转化为临床实践。

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Transitional cell (urothelial) carcinoma of the bladder is the second most common urologic malignancy and is one of the best understood neoplasms, with relatively well-defined pathogenetic pathways, natural history, and tumor biology. Conventional clinical and pathologic parameters are widely used to grade and stage tumors and to predict clinical outcome of transitional cell carcinoma; but the predictive ability of these parameters is limited, and there is a lack of indices that could allow prospective assessment of risk for individual patients. In the last decade, a wide range of candidate biomarkers representing key pathways in carcinogenesis have been reported to be clinically relevant and potentially useful as diagnostic and prognostic molecular markers, and as potential therapeutic targets. The use of molecular markers has facilitated the development of novel and more accurate diagnostic, prognostic, and therapeutic strategies. FGFR3 and TP53 mutations have been recognized as key genetic pathways in the carcinogenesis of transitional cell carcinoma. FGFR3 appears to be the most frequently mutated oncogene in transitional cell carcinoma; its mutation is strongly associated with low tumor grade, early stage, and low recurrence rate, which confer a better overall prognosis. In contrast, TP53 mutations are associated with higher tumor grade, more advanced stage, and more frequent tumor recurrences. These molecular markers offer the potential to characterize individual urothelial neoplasms more completely than is possible by histologic evaluation alone. Areas in which molecular markers may prove valuable include prediction of tumor recurrence, molecular staging of transitional cell carcinoma, detection of lymph node metastasis and circulating cancer cells, identification of therapeutic targets, and prediction of response to therapy. With accumulating molecular knowledge of transitional cell carcinoma, we are closer to the goal of bridging the gap between molecular findings and clinical outcomes. Assessment of key genetic pathways and expression profiles could ultimately establish a set of molecular markers to predict the biological nature of tumors and to establish new standards for molecular tumor grading, classification, and prognostication. The main focus of this review is to discuss clinically relevant biomarkers that might be useful in the management of transitional cell carcinoma and to provide approaches in the analysis of molecular pathways that influence the clinical course of bladder cancer.
机译:膀胱移行细胞(尿路上皮)癌是第二常见的泌尿外科恶性肿瘤,是最易理解的肿瘤之一,具有相对明确的致病途径,自然病史和肿瘤生物学。常规的临床和病理学参数被广泛用于对肿瘤进行分级和分期,并预测移行细胞癌的临床结局。但是这些参数的预测能力是有限的,并且缺乏可以对每个患者进行前瞻性评估的指标。在过去的十年中,已报道了代表致癌关键途径的多种候选生物标志物与临床相关,并且有可能用作诊断和预后分子标志物以及潜在的治疗靶标。分子标记物的使用促进了新型和更准确的诊断,预后和治疗策略的发展。 FGFR3和TP53突变已被认为是移行细胞癌致癌的关键遗传途径。 FGFR3似乎是移行细胞癌中最常见的致癌基因。其突变与低肿瘤分级,早期和低复发率密切相关,从而赋予更好的总体预后。相反,TP53突变与更高的肿瘤等级,更晚期,更频繁的肿瘤复发相关。这些分子标记物提供了比单独通过组织学评估更完整地表征单个尿路上皮肿瘤的潜力。分子标记物可能被证明有价值的领域包括肿瘤复发的预测,过渡细胞癌的分子分期,淋巴结转移和循环癌细胞的检测,治疗靶标的确定以及对治疗反应的预测。随着对移行细胞癌分子知识的积累,我们更接近弥合分子发现与临床结果之间差距的目标。对关键遗传途径和表达谱的评估最终可以建立一套分子标记,以预测肿瘤的生物学特性,并为分子肿瘤的分级,分类和预后建立新的标准。这篇综述的主要重点是讨论可能在移行细胞癌管理中有用的临床相关生物标志物,并提供分析影响膀胱癌临床病程的分子途径的方法。

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