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通过白蛋白透析改善慢性肝衰竭急性发作时受损的白蛋白结合能力。

Improvement of impaired albumin binding capacity in acute-on-chronic liver failure by albumin dialysis.

作者信息

Klammt Sebastian, Mitzner Steffen R, Stange Jan, Loock Jan, Heemann Uwe, Emmrich Jörg, Reisinger Emil C, Schmidt Reinhard

机构信息

Department of Internal Medicine, Division of Nephrology, University Rostock, Rostock, Germany.

出版信息

Liver Transpl. 2008 Sep;14(9):1333-9. doi: 10.1002/lt.21504.

Abstract

Extracorporeal albumin dialysis (ECAD) enables the elimination of albumin bound substances and is used as artificial liver support system. Albumin binding function for the benzodiazepine binding site specific marker Dansylsarcosine was estimated in plasma samples of 22 patients with cirrhosis and hyperbilirubinaemia (ECAD: n = 12; control: n = 10) during a period of 30 days in a randomized controlled clinical ECAD trial. Albumin Binding Capacity (ABiC) at baseline was reduced to 31.8% (median; range 24%-74%) and correlated to the severity of liver disease. Within two weeks a significant improvement of ABiC and a reduction of the albumin bound markers bilirubin and bile acids were observed in the ECAD group. During single treatments a significant decrease of albumin bound substances (bilirubin and bile acids) as well as an increase in ABiC was observed. In the control group, baseline ABiC was significantly lower in patients who died during study period (34.2% vs. 41.7%; P < 0.028), whereas no significant differences were observed for CHILD, coagulation factors, albumin, bile acids nor bilirubin. At baseline 13 patients had a severely impaired ABiC (<40%), improvement of ABiC was more frequent in the ECAD group (5/6) than in the SMT group (2/7). Reduced albumin binding function is present in decompensated liver failure and is related to severity and 30 day survival. ABiC can be improved by ECAD. The beneficial effect of this treatment may be related to the improvement of albumin binding function more than to the elimination of specific substances. Characterization of albumin function by the ABiC test may help to evaluate different liver support systems and other therapeutic measures.

摘要

体外白蛋白透析(ECAD)能够清除与白蛋白结合的物质,可用作人工肝支持系统。在一项随机对照临床ECAD试验中,对22例肝硬化合并高胆红素血症患者(ECAD组:n = 12;对照组:n = 10)的血浆样本进行了为期30天的检测,评估了白蛋白对苯二氮䓬结合位点特异性标志物丹磺酰肌氨酸的结合功能。基线时白蛋白结合能力(ABiC)降至31.8%(中位数;范围24%-74%),并与肝病严重程度相关。在两周内,ECAD组的ABiC显著改善,与白蛋白结合的标志物胆红素和胆汁酸减少。在单次治疗期间,观察到与白蛋白结合的物质(胆红素和胆汁酸)显著减少以及ABiC增加。在对照组中,研究期间死亡的患者基线ABiC显著较低(34.2%对41.7%;P < 0.028),而在儿童、凝血因子、白蛋白、胆汁酸和胆红素方面未观察到显著差异。基线时13例患者的ABiC严重受损(<40%),ECAD组ABiC改善的频率(5/6)高于标准治疗组(SMT组,2/7)。失代偿性肝衰竭存在白蛋白结合功能降低,且与严重程度和30天生存率相关。ECAD可改善ABiC。这种治疗的有益效果可能更多地与白蛋白结合功能的改善有关,而不是与特定物质的清除有关。通过ABiC试验对白蛋白功能进行表征可能有助于评估不同的肝支持系统和其他治疗措施。

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