分子改变与吸烟强度联合预测膀胱癌预后:洛杉矶癌症监测计划的报告。
Combination of molecular alterations and smoking intensity predicts bladder cancer outcome: a report from the Los Angeles Cancer Surveillance Program.
机构信息
Department of Pathology, University of Southern California, Los Angeles, California, USA.
出版信息
Cancer. 2013 Feb 15;119(4):756-65. doi: 10.1002/cncr.27763. Epub 2013 Jan 14.
BACKGROUND
Traditional single-marker and multimarker molecular profiling approaches in bladder cancer do not account for major risk factors and their influence on clinical outcome. This study examined the prognostic value of molecular alterations across all disease stages after accounting for clinicopathological factors and smoking, the most common risk factor for bladder cancer in the developed world, in a population-based cohort.
METHODS
Primary bladder tumors from 212 cancer registry patients (median follow-up, 13.2 years) were immunohistochemically profiled for Bax, caspase-3, apoptotic protease-activating factor 1 (Apaf-1), Bcl-2, p53, p21, cyclooxygenase-2, vascular endothelial growth factor, and E-cadherin alterations. "Smoking intensity" quantified the impact of duration and daily frequency of smoking.
RESULTS
Age, pathological stage, surgical modality, and adjuvant therapy administration were significantly associated with survival. Increasing smoking intensity was independently associated with worse outcome (P < .001). Apaf-1, E-cadherin, and p53 were prognostic for outcome (P = .005, .014, and .032, respectively); E-cadherin remained prognostic following multivariable analysis (P = .040). Combined alterations in all 9 biomarkers were prognostic by univariable (P < .001) and multivariable (P = .006) analysis. A multivariable model that included all 9 biomarkers and smoking intensity had greater accuracy in predicting prognosis than models composed of standard clinicopathological covariates without or with smoking intensity (P < .001 and P = .018, respectively).
CONCLUSIONS
Apaf-1, E-cadherin, and p53 alterations individually predicted survival in bladder cancer patients. Increasing number of biomarker alterations was significantly associated with worsening survival, although markers comprising the panel were not necessarily prognostic individually. Predictive value of the 9-biomarker panel with smoking intensity was significantly higher than that of routine clinicopathological parameters alone.
背景
传统的膀胱癌单标记物和多标记物分子分析方法并未考虑主要风险因素及其对临床结局的影响。本研究在一个基于人群的队列中,在考虑临床病理因素和吸烟(发达国家膀胱癌最常见的风险因素)的情况下,检测了所有疾病阶段的分子改变对预后的影响。
方法
对 212 名癌症登记患者的原发性膀胱癌肿瘤进行 Bax、caspase-3、凋亡蛋白酶激活因子 1(Apaf-1)、Bcl-2、p53、p21、环氧化酶-2、血管内皮生长因子和 E-钙黏蛋白改变的免疫组织化学分析。“吸烟强度”量化了吸烟持续时间和每日吸烟频率的影响。
结果
年龄、病理分期、手术方式和辅助治疗的应用与生存显著相关。吸烟强度增加与预后不良独立相关(P<0.001)。Apaf-1、E-钙黏蛋白和 p53 对结局有预后意义(P=0.005、0.014 和 0.032);在多变量分析后,E-钙黏蛋白仍然具有预后意义(P=0.040)。9 种生物标志物的联合改变通过单变量(P<0.001)和多变量(P=0.006)分析均具有预后意义。包括所有 9 种生物标志物和吸烟强度的多变量模型比不包括或包括吸烟强度的标准临床病理协变量组成的模型更准确地预测预后(P<0.001 和 P=0.018)。
结论
Apaf-1、E-钙黏蛋白和 p53 改变单独预测膀胱癌患者的生存。标志物改变数量的增加与生存恶化显著相关,尽管构成该标志物的改变不一定具有预后意义。包含吸烟强度的 9 种生物标志物面板的预测价值明显高于单独的常规临床病理参数。
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