肝硬化患者显性肝性脑病发展预测模型。
A Model for Predicting Development of Overt Hepatic Encephalopathy in Patients With Cirrhosis.
机构信息
Department of Clinical Medicine, Center for the Diagnosis and Treatment of Portal Hypertension, "Sapienza" University of Rome, Rome, Italy.
Department of Medicine, University of Padua, Padua, Italy.
出版信息
Clin Gastroenterol Hepatol. 2015 Jul;13(7):1346-52. doi: 10.1016/j.cgh.2014.12.025. Epub 2015 Jan 5.
BACKGROUND & AIMS: Overt hepatic encephalopathy (HE) affects patients' quantity and quality of life and places a burden on families. There is evidence that overt HE might be prevented pharmacologically, but prophylaxis would be justified and cost effective only for patients at risk. We aimed to identify patients with cirrhosis at risk for overt HE.
METHODS
We collected data from October 2009 through December 2012 for 216 consecutive patients with cirrhosis (based on liver biopsy, 96 patients with minimal HE), admitted to the Gastroenterology Unit at the University of Rome. Patients were followed up and evaluated for an average of 14.7 ± 11.6 months; development of overt HE was recorded. We analyzed end-stage liver disease scores, shunt placement, previous overt or minimal HE, psychometric hepatic encephalopathy score (PHES), and levels of albumin, bilirubin, creatinine, and sodium to develop a prediction model. We validated the model in 112 patients with cirrhosis seen at the University of Padua and followed up for 12 ± 9.5 months.
RESULTS
During the follow-up period, 68 patients (32%) developed at least 1 episode of overt HE. Based on multivariate analysis, the development of overt HE was associated with previous HE, minimal HE (based on PHES), and level of albumin less than 3.5 g/dL (area under curve [AUC], 0.74). A model that excluded minimal HE but included albumin level and previous HE also identified patients who would develop overt HE (AUC, 0.71); this difference in AUC values was not statistically significant (P = .104). Both models were validated in the independent group of patients (3 variables: AUC, 0.74; 95% confidence interval, 0.66-0.83; and 2 variables: AUC, 0.71; 95% confidence interval, 0.63-0.78).
CONCLUSIONS
We developed and validated a model to identify patients with cirrhosis at risk for overt HE based on previous HE, albumin levels, and PHES. If PHES was not available, previous HE and albumin levels still can identify patients at risk. Psychometric evaluation is essential for patients with no history of HE. These findings should aid in planning studies of pharmacologic prevention of overt HE.
背景与目的
显性肝性脑病(HE)会影响患者的生活质量和数量,并给家庭带来负担。有证据表明,显性 HE 可以通过药物预防,但只有对有风险的患者进行预防才合理且具有成本效益。我们旨在确定有显性 HE 风险的肝硬化患者。
方法
我们从 2009 年 10 月至 2012 年 12 月收集了 216 例连续的肝硬化患者的数据(基于肝活检,96 例有轻微 HE),这些患者被收入罗马大学胃肠病科。对患者进行了平均 14.7±11.6 个月的随访和评估;记录显性 HE 的发展情况。我们分析了终末期肝病评分、分流术、既往显性或轻微 HE、心理测量性肝性脑病评分(PHES)以及白蛋白、胆红素、肌酐和钠水平,以建立预测模型。我们在 112 例在帕多瓦大学就诊并随访 12±9.5 个月的肝硬化患者中验证了该模型。
结果
在随访期间,68 例(32%)患者至少发生了 1 次显性 HE 发作。基于多变量分析,显性 HE 的发展与既往 HE、轻微 HE(基于 PHES)和白蛋白水平<3.5 g/dL 有关(曲线下面积[AUC],0.74)。排除轻微 HE 但纳入白蛋白水平和既往 HE 的模型也能识别出会发生显性 HE 的患者(AUC,0.71);这两种 AUC 值的差异无统计学意义(P=0.104)。两个模型在独立患者组中均得到验证(3 个变量:AUC,0.74;95%置信区间,0.66-0.83;2 个变量:AUC,0.71;95%置信区间,0.63-0.78)。
结论
我们基于既往 HE、白蛋白水平和 PHES 制定并验证了一种用于识别显性 HE 风险的肝硬化患者的模型。如果无法获得 PHES,则既往 HE 和白蛋白水平仍可识别出有风险的患者。心理测量评估对无 HE 病史的患者至关重要。这些发现应有助于规划显性 HE 的药物预防研究。
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