首页> 外文期刊>Journal of Clinical Oncology >Novel staging system for predicting disease-specific survival in patients with breast cancer treated with surgery as the first intervention: time to modify the current American Joint Committee on Cancer staging system.
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Novel staging system for predicting disease-specific survival in patients with breast cancer treated with surgery as the first intervention: time to modify the current American Joint Committee on Cancer staging system.

机译:新型分期系统可预测以手术治疗的乳腺癌患者的疾病特异性存活率,这是第一种干预措施:现在​​是时候修改目前的美国癌症联合委员会分期系统。

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PURPOSE: American Joint Committee on Cancer (AJCC) staging is used to determine breast cancer prognosis, yet patient survival within each stage shows wide variation. We hypothesized that differences in biology influence this variation and that addition of biologic markers to AJCC staging improves determination of prognosis. PATIENTS AND METHODS: We identified a cohort of 3,728 patients who underwent surgery as the first intervention between 1997 and 2006. A Cox proportional hazards model, with backward stepwise exclusion of factors and stratification on pathologic stage (PS), was used to test the significance of adding grade (G), lymphovascular invasion (L), estrogen receptor (ER) status (E), progesterone receptor (PR) status, combined ER and PR status (EP), or combined ER, PR, and human epidermal growth factor receptor 2 status (M). We assigned values of 0 to 2 to these disease-specific survival (DSS) -associated factors and assessed six different staging systems: PS, PS + G, PS + G L, PS + G E, PS + G EP, and PS + G M. We compared 5-year DSS rates, Akaike's information criterion (AIC), and Harrell's concordance index (C-index) between systems. Surveillance, Epidemiology, and End Results data were used as the external validation cohort (n = 26,711). RESULTS: Median follow-up was 6.5 years, and 5-year DSS rate was 97.4%. The PS + G E status staging system was most precise, with a low AIC (1,931.9) and the highest C-index (0.80). PS + G E status was confirmed to stratify outcomes in internal bootstrapping samples and the external validation cohort. CONCLUSION: Our results validate an improved breast cancer staging system that incorporates grade and ER status. We recommend that biologic markers be incorporated into revised versions of the AJCC staging system.
机译:目的:美国癌症联合委员会(AJCC)分期用于确定乳腺癌的预后,但每个阶段的患者生存率差异很大。我们假设生物学差异会影响这种变异,并且向AJCC分期添加生物标志物可改善对预后的确定。患者与方法:我们确定了1997年至2006年的3728例接受手术治疗的患者作为首次干预。采用Cox比例风险模型,将因素逐步后移并按病理分期(PS)进行分层,以检验其重要性。增加等级(G),淋巴管浸润(L),雌激素受体(ER)状态,孕激素受体(PR)状态,ER和PR合并状态(EP)或ER,PR和人表皮生长因子的合并受体2状态(M)。我们为这些疾病特异性生存(DSS)相关因素分配了0到2的值,并评估了六个不同的分期系统:PS,PS + G,PS + GL,PS + GE,PS + G EP和PS + G M我们比较了系统之间的5年DSS费率,Akaike的信息标准(AIC)和Harrell的一致性指数(C-index)。监测,流行病学和最终结果数据用作外部验证队列(n = 26,711)。结果:中位随访时间为6.5年,5年DSS率为97.4%。 PS + G E状态分期系统最为精确,AIC低(1,931.9),C指数最高(0.80)。确认PS + G E状态可对内部自举样本和外部验证队列的结果进行分层。结论:我们的结果验证了结合了等级和ER状态的改进的乳腺癌分期系统。我们建议将生物标志物纳入AJCC分期系统的修订版中。

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