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首页> 外文期刊>BMC Cancer >A competing risk nomogram predicting cause-specific mortality in patients with lung adenosquamous carcinoma
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A competing risk nomogram predicting cause-specific mortality in patients with lung adenosquamous carcinoma

机译:一种竞争风险载体预测肺腺瘤癌患者患者的原因特异性死亡率

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BACKGROUND:Adenosquamous carcinoma (ASC) is an uncommon histological subtype of lung cancer. The purpose of this study was to assess the cumulative incidences of lung cancer-specific mortality (LC-SM) and other cause-specific mortality (OCSM) in lung ASC patients, and construct a corresponding competing risk nomogram for LC-SM.METHODS:Data on 2705 patients with first primary lung ASC histologically diagnosed between 2004 and 2015 were extracted from the Surveillance, Epidemiology, and End Results (SEER) database. The cumulative incidence function (CIF) was utilized to calculate the 3-year and 5-year probabilities of LC-SM and OCSM, and a competing risk model was built. Based on the model, we developed a competing risk nomogram to predict the 3-year and 5-year cumulative probabilities of LC-SM and the corresponding concordance indexes (C-indexes) and calibration curves were derived to assess the model performance. To evaluate the clinical usefulness of the nomogram, decision curve analysis (DCA) was conducted. Furthermore, patients were categorized into three groups according to the tertile values of the nomogram-based scores, and their survival differences were assessed using CIF curves.RESULTS:The 3-year and 5-year cumulative mortalities were 49.6 and 55.8% for LC-SM and 8.2 and 11.8% for OCSM, respectively. In multivariate analysis, increasing age, male sex, no surgery, and advanced T, N and M stages were related to a significantly higher likelihood of LC-SM. The nomogram showed good calibration, and the 3-year and 5-year C-indexes for predicting the probabilities of LC-SM in the validation cohort were both 0.79, which were almost equal to those of the ten-fold cross validation. DCA demonstrated that using the nomogram gained more benefit when the threshold probabilities were set within the ranges of 0.24-0.89 and 0.25-0.91 for 3-year and 5-year LCSM, respectively. In both the training and validation cohorts, the high-risk group had the highest probabilities of LC-SM, followed by the medium-risk and low-risk groups (both P??0.0001).CONCLUSIONS:The competing risk nomogram displayed excellent discrimination and calibration for predicting LC-SM. With the aid of this individualized predictive tool, clinicians can more expediently devise appropriate treatment protocols and follow-up schedules.
机译:背景:腺癌癌(ASC)是肺癌的罕见组织学亚型。本研究的目的是评估肺癌患者肺癌特异性死亡率(LC-SM)和其他原因特异性死亡率(OCSM)的累积发病率,并为LC-SM构建相应的竞争风险载体。从监测,流行病学和最终结果(SEER)数据库中提取2705名初级肺部ASC组织学诊断的数据。利用累积发生率(CIF)来计算LC-SM和OCSM的3年和5年的概率,并建立了竞争风险模型。基于该模型,我们开发了一种竞争风险NOM图,以预测LC-SM的3年和5年的累积概率和相应的一致性指数(C-INDEXES)和校准曲线以评估模型性能。为了评估NOM图的临床有用性,进行了决策曲线分析(DCA)。此外,根据基于墨迹的评分的三分比,患者分为三组,使用CIF曲线评估它们的存活差异。结果:3年和5年累计死亡率为49.6和55.8% SM和8.2和11.8%分别用于OCSM。在多变量分析中,增加年龄,男性性别,无手术和先进的T,N和M阶段与LC-SM的显着较高的可能性有关。 NOM图显示出良好的校准,3年和5年的C索引用于预测验证队列中LC-SM的概率均为0.79,几乎等于十倍交叉验证的索引。 DCA分别证明,使用阈值概率分别在为3年和5年LCSM的范围内设定阈值概率时,使用墨顶图获得了更多的好处。在培训和验证队列中,高风险组具有LC-SM的最高概率,其次是中风险和低风险群体(P?<?0.0001).Conclusions:竞争风险NOM图显示出优秀预测LC-SM的辨别和校准。借助于这种个性化的预测工具,临床医生可以更有利地设计适当的治疗方案和后续时间表。

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