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Noninvasive Evaluation of Liver Fibrosis and Portal Hypertension After Successful Portoenterostomy for Biliary Atresia

机译:胆道闭锁成功进行门肠造口术后肝纤维化和门脉高压的非侵入性评估

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摘要

We investigated noninvasive follow‐up markers for histologic liver fibrosis and portal hypertension (PH) in patients with biliary atresia after successful portoenterostomy (PE). Among children with bilirubin <20 µmol/L after PE (n = 39), Metavir fibrosis stage was evaluated at PE and in follow‐up protocol liver biopsies (n = 83). PH was defined as endoscopically confirmed esophageal varices or thrombocytopenia associated with splenomegaly. The accuracy of liver biochemistry and stiffness in detecting liver fibrosis and PH was analyzed by the area under the receiving operating characteristic curve (AUROC) and multiple regression models. During a median native liver survival of 8.3 years (interquartile range 2.5‐10.8 years), cirrhosis (Metavir F4) had developed in 51% of patients and PH in 54% of patients. Cirrhosis was equally common in all age tertiles of 1.2‐2.1 years (n = 10/27), 3.9‐5.8 years (n = 12/28), and 9.0‐14 years (n = 12/28). In the two oldest age tertiles, histologic liver fibrosis had progressed further in patients with PH than without PH (P < 0.001). PH was accurately predicted by the aspartate aminotransferase‐to‐platelet ratio index (APRI) (cutoff, 0.70; AUROC, 0.92), bile acids (cutoff, 49 µmol/L; AUROC, 0.91), and liver stiffness (cutoff, 16.9 kPa; AUROC, 0.89; P < 0.001 each) across all age tertiles. Liver stiffness was the most accurate predictor of cirrhosis overall (AUROC, 0.82; P < 0.001), whereas bilirubin was >11 µmol/L in the youngest tertile (AUROC, 0.91; P < 0.001), bile acids was >80 µmol/L in the middle tertile (AUROC, 0.81; P = 0.009), and liver stiffness was >24 kPa in the oldest age tertile (AUROC, 0.96; P = 0.002). Conclusion: After successful PE, development of PH associates with progression of liver fibrosis and can be accurately detected by APRI and stiffness. Liver stiffness most accurately identified cirrhosis in older children, whereas biochemical markers of cholestasis closely reflected histologic cirrhosis in younger children.
机译:我们研究了成功的门肠造口术(PE)后胆道闭锁患者的组织学肝纤维化和门脉高压(PH)的无创性随访指标。在PE后胆红素<20 µmol / L的儿童中(n = 39),在PE和随访方案的肝活检中评估了Metavir纤维化阶段(n = 83)。 PH被定义为经内镜证实的食管静脉曲张或与脾肿大相关的血小板减少症。通过接受手术特征曲线(AUROC)下的面积和多元回归模型分析了肝生化的准确性和刚度,以检测肝纤维化和PH。在中位自然肝脏生存期为8.3年(四分位间距2.5-10.8年)中,肝硬化(Metavir F4)在51%的患者中发生,PH在54%的患者中发生。肝硬化在1.2-2.1岁(n = 10/27),3.9-5.8岁(n = 12/28)和9.0-14岁(n = 12/28)的所有年龄三分位数中同样普遍。在两个年龄最大的三分位数中,有PH的患者的组织学肝纤维化进展较无PH的患者更为明显(P <0.001)。天冬氨酸氨基转移酶与血小板的比率指数(APRI)(临界值为0.70; AUROC为0.92),胆汁酸(临界值为49 µmol / L; AUROC为0.91)和肝硬度(临界值为16.9 kPa)可以准确预测PH ; AUROC,0.89;在所有年龄三分位数中均P <0.001)。肝硬度是最准确的整体肝硬化预测指标(AUROC,0.82; P <0.001),而最年轻的三分位数中胆红素> 11 µmol / L(AUROC,0.91; P <0.001),胆汁酸> 80 µmol / L在中三分位数(AUROC,0.81; P = 0.009)中,最老年龄的三分位数(AUROC,0.96; P = 0.002)的肝硬度大于24 kPa。结论:成功的PE后,PH的发展与肝纤维化的发展有关,并且可以通过APRI和僵硬度进行准确检测。肝硬度可以最准确地识别年龄较大的儿童的肝硬化,而胆汁淤积的生化指标则紧密反映了年龄较小的儿童的组织学性肝硬化。

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