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Diabetes impacts prediction of cirrhosis and prognosis by non‐invasive fibrosis models in non‐alcoholic fatty liver disease

机译:非酒精性脂肪肝疾病中非侵入性纤维化模型对肝硬化和预后的糖尿病影响预测

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Abstract Background & Aims Non‐alcoholic fatty liver disease ( NAFLD ) patients with diabetes are at increased risk of cirrhosis and liver‐related death, and thus accurate fibrosis assessment in these patients is important. We examined the ability of non‐invasive fibrosis models to determine cirrhosis and outcomes in NAFLD patients with and without diabetes. Methods Non‐alcoholic fatty liver disease patients diagnosed between 2006 and 2015 had Hepascore, NAFLD fibrosis score ( NFS ), APRI and FIB ‐4 scores calculated at baseline and were followed up for outcomes of overall and liver‐related mortality/liver transplantation, hepatic decompensation and hepatocellular carcinoma ( HCC ). Model accuracy was determined by Harrell's C‐index and by Kaplan‐Meier analysis. Results A total of 284 patients (53% diabetic, 15% cirrhotic) were followed up for a median of 51.4?months, (range 6.1‐146). During follow‐up, diabetic patients had a greater risk of liver‐related death/transplantation, HR 3.4 (95% CI 1.2‐9.1) decompensation, HR 4.7 (95% CI 2.0‐11.3) and HCC , HR 2.9 (95% CI 1.2‐7.3). Among 241 subjects with a baseline liver biopsy, the accuracy of Hepascore, APRI and FIB ‐4 for predicting cirrhosis was lower amongst diabetics compared to non‐diabetics ( P ??.005 for all). Model accuracy apart from Hepascore, was also significantly lower for predicting liver death/transplantation in patients with diabetes. No patient with a low fibrosis score and without diabetes developed liver decompensation or HCC , whereas up to 21% of diabetic patients with a low fibrosis score developed liver decompensation and up to 27% developed HCC at 5?years. Conclusions Non‐invasive scoring systems are less accurate at predicting cirrhosis and liver‐related outcomes in patients with NAFLD and diabetes.
机译:抽象背景&目的是非酒精性脂肪肝病(NAFLD)糖尿病患者患肝硬化和肝脏相关死亡的风险增加,因此这些患者的准确纤维化评估很重要。我们检查了非侵入性纤维化模型的能力,以确定NAFLD患者患有糖尿病患者的肝硬化和结果。方法,2006年至2015年间诊断的非酒精脂肪肝病患者患有肝脏,NAFLD纤维化评分(NFS),APRI和FIB -4分数在基线计算,并随访总体和肝脏相关死亡率/肝移植的结果,肝脏失代偿和肝细胞癌(HCC)。模型准确性由Harrell的C-Index和Kaplan-Meier分析确定。结果总共284名患者(53%糖尿病,15%的肝硬化)随访,中位数为51.4个月,(范围为6.1-146)。在随访期间,糖尿病患者风险更大的肝相关的死亡/移植风险,HR 3.4(95%CI 1.2-9.1)失代偿,HR 4.7(95%CI 2.0-11.3)和HCC,HR 2.9(95%CI 1.2-7.3)。在241名受试者中,与非糖尿病患者相比,糖莽,APRI和FIB -4预测肝硬化的精度降低了糖尿病患者(P 1。005)。除了赫斯克斯堡外,模型精度也显着降低,用于预测糖尿病患者的肝死/移植。没有患有低纤维化分数和没有糖尿病的患者发育肝脏失代偿或HCC,而高达21%的糖尿病患者患有低纤维化症的患者发育肝脏失代偿,最高可达27%的HCC在5岁时发育了57%。结论无侵入性评分系统在预测NAFLD和糖尿病患者的肝硬化和肝脏相关结果方面不太准确。

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