Mitra Anirban P, Pagliarulo Vincenzo, Yang Dongyun, Waldman Frederic M, Datar Ram H, Skinner Donald G, Groshen Susan, Cote Richard J
Department of Pathology, Norris Comprehensive Cancer Center, Keck School of Medicine, University of Southern California, Los Angeles, CA, USA.
J Clin Oncol. 2009 Aug 20;27(24):3929-37. doi: 10.1200/JCO.2008.18.5744. Epub 2009 Jul 20.
This study sought to determine if alterations in molecular pathways could supplement TNM staging to more accurately predict clinical outcome in patients with urothelial carcinoma (UC).
Expressions of 69 genes involved in known cancer pathways were quantified on bladder specimens from 58 patients with UC (stages Ta-T4) and five normal urothelium controls. All tumor transcript values beyond two standard deviations from the normal mean expression were designated as over- or underexpressed. Univariate and multivariable analyses were conducted to obtain a predictive expression signature. A published external data set was used to confirm the potential of the prognostic gene panels.
In univariate analysis, six genes were significantly associated with time to recurrence, and 10 with overall survival. Recursive partitioning identified three genes as significant determinants for recurrence, and three for overall survival. Of all genes identified by either univariate or partitioning analysis, four were found to significantly predict both recurrence and survival (JUN, MAP2K6, STAT3, and ICAM1); overexpression was associated with worse outcome. Comparing the favorable (low or normal) expression of > or = three of four versus < or = two of four of these oncogenes showed 5-year recurrence probability of 41% versus 88%, respectively (P < .001), and 5-year overall survival probability of 61% versus 5%, respectively (P < .001). The prognostic potential of this four-gene panel was confirmed in a large independent external cohort (disease-specific survival, P = .039).
We have documented the generation of a concise, biologically relevant four-gene panel that significantly predicts recurrence and survival and may also identify potential therapeutic targets for UC.
本研究旨在确定分子通路的改变是否可以补充TNM分期,以更准确地预测尿路上皮癌(UC)患者的临床结局。
对58例UC患者(Ta - T4期)的膀胱标本和5例正常尿路上皮对照样本中参与已知癌症通路的69个基因的表达进行定量分析。所有肿瘤转录本值超过正常平均表达两个标准差以上的被定义为过表达或低表达。进行单变量和多变量分析以获得预测性表达特征。使用已发表的外部数据集来确认预后基因panel的潜力。
在单变量分析中,6个基因与复发时间显著相关,10个基因与总生存期显著相关。递归划分确定3个基因是复发的显著决定因素,3个基因是总生存期的显著决定因素。在单变量分析或划分分析确定的所有基因中,发现4个基因显著预测复发和生存期(JUN、MAP2K6、STAT3和ICAM1);过表达与更差的结局相关。比较这4个癌基因中≥3个与≤2个的有利(低或正常)表达情况,5年复发概率分别为41%和88%(P < .001),5年总生存概率分别为61%和5%(P < .001)。这个四基因panel的预后潜力在一个大型独立外部队列中得到证实(疾病特异性生存,P = .039)。
我们已经证明生成了一个简洁的、具有生物学相关性的四基因panel,该panel能显著预测复发和生存期,还可能识别UC的潜在治疗靶点。
