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膀胱癌M-VAC新辅助化疗临床反应预测系统的研究

Study of the prediction system for clinical response to M-VAC neoadjuvant chemotherapy for bladder cancer.

作者信息

Takata R, Obara W, Fujioka T

机构信息

Department of Urology, Iwate Medical University, Iwate, Japan.

出版信息

Aktuelle Urol. 2010 Jan;41 Suppl 1:S41-5. doi: 10.1055/s-0029-1224655. Epub 2010 Jan 21.

Abstract

Neoadjuvant chemotherapy for invasive bladder cancer, involving a regimen of M-VAC, can manage micrometastasis and improve the prognosis. However, some patients suffer from severe adverse drug reactions without any effect, and no method yet exists for predicting the response of an individual patient to chemotherapy. Our purpose in this study is to establish a method for predicting the response to the M-VAC therapy. We analyzed gene-expression profiles of biopsy materials from 40 invasive bladder cancers using a cDNA microarray consisting of 27 648 genes, after populations of cancer cells had been purified by laser-microbeam microdissection. We identified 14 predictive genes that were expressed differently between nine responder and nine non-responder tumors and devised a prediction-scoring system that clearly separated the responder group from the non-responder group. This system accurately predicted the clinical response for 19 of the 22 additional test cases. The group of patients with positive predictive scores had significantly longer survival times than that with negative scores. As real-time RT-PCR data were highly concordant with the cDNA microarray data for those 14 genes, we developed a quantitative RT-PCR-based prediction system that could be feasible for routine clinical use. Taken together, our results suggest that the sensitivity of an invasive bladder cancer to the M-VAC neoadjuvant chemotherapy can be predicted by expression patterns in this set of genes, a step toward achievement of "personalized therapy" for treatment of this disease.

摘要

侵袭性膀胱癌的新辅助化疗,采用M-VAC方案,可控制微转移并改善预后。然而,一些患者出现严重药物不良反应却毫无效果,且尚无预测个体患者化疗反应的方法。本研究的目的是建立一种预测对M-VAC疗法反应的方法。在通过激光微束显微切割纯化癌细胞群体后,我们使用包含27648个基因的cDNA微阵列分析了40例侵袭性膀胱癌活检材料的基因表达谱。我们鉴定出14个预测基因,它们在9例反应者和9例无反应者肿瘤之间表达不同,并设计了一个预测评分系统,该系统能清晰地将反应者组与无反应者组区分开来。该系统准确预测了另外22个测试病例中19例的临床反应。预测评分阳性的患者组生存时间明显长于评分阴性的患者组。由于这14个基因的实时RT-PCR数据与cDNA微阵列数据高度一致,我们开发了一种基于定量RT-PCR的预测系统,该系统在常规临床应用中可能是可行的。综上所述,我们的结果表明,侵袭性膀胱癌对M-VAC新辅助化疗的敏感性可通过这组基因的表达模式来预测,这是朝着实现该疾病“个性化治疗”迈出的一步。

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