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Application of a biochemical and clinical model to predict individual survival in patients with end-stage liver disease

机译:生化和临床模型在预测终末期肝病患者个体存活中的应用

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摘要

AIM: To investigate the capability of a biochemical and clinical model, BioCliM, in predicting the survival of cirrhotic patients.METHODS: We prospectively evaluated the survival of 172 cirrhotic patients. The model was constructed using clinical (ascites, encephalopathy and variceal bleeding) and biochemical (serum creatinine and serum total bilirubin) variables that were selected from a Cox proportional hazards model. It was applied to estimate 12-, 52- and 104-wk survival. The model’s calibration using the Hosmer-Lemeshow statistic was computed at 104 wk in a validation dataset. Finally, the model’s validity was tested among an independent set of 85 patients who were stratified into 2 risk groups (low risk ≤ 8 and high risk > 8).RESULTS: In the validation cohort, all measures of fit, discrimination and calibration were improved when the biochemical and clinical model was used. The proposed model had better predictive values (c-statistic: 0.90, 0.91, 0.91) than the Model for End-stage Liver Disease (MELD) and Child-Pugh (CP) scores for 12-, 52- and 104-wk mortality, respectively. In addition, the Hosmer-Lemeshow (H-L) statistic revealed that the biochemical and clinical model (H-L, 4.69) is better calibrated than MELD (H-L, 17.06) and CP (H-L, 14.23). There were no significant differences between the observed and expected survival curves in the stratified risk groups (low risk, P = 0.61; high risk, P = 0.77).CONCLUSION: Our data suggest that the proposed model is able to accurately predict survival in cirrhotic patients.
机译:目的:探讨生化和临床模型BioCliM预测肝硬化患者生存的能力。方法:我们前瞻性评估了172例肝硬化患者的生存率。使用从Cox比例风险模型中选择的临床(腹水,脑病和静脉曲张出血)和生化(血清肌酐和血清总胆红素)变量构建模型。它被用于估计12周,52周和104周的存活率。该模型使用Hosmer-Lemeshow统计信息的校准是在验证数据集中以104周计算的。最后,该模型的有效性在独立的85位患者中进行了检验,这些患者分为2个风险组(低风险≤8和高风险> 8)。结果:在验证队列中,改善了所有拟合度,区分度和校正度的量度当使用生化和临床模型时。与12周龄,52周龄和104周龄死亡率的终末期肝病(MELD)和Child-Pugh(CP)评分模型相比,拟议的模型具有更好的预测值(c统计量:0.90、0.91、0.91),分别。此外,Hosmer-Lemeshow(H-L)统计数据显示,生化和临床模型(H-L,4.69)的校准比MELD(H-L,17.06)和CP(H-L,14.23)更好。在分层风险组中观察到的和预期的生存曲线之间没有显着差异(低风险,P = 0.61;高风险,P = 0.77)。结论:我们的数据表明,所提出的模型能够准确预测肝硬化患者的生存率耐心。

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