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关于肝硬化患者白蛋白治疗的争议。

Controversies regarding albumin therapy in cirrhosis.

作者信息

Trebicka Jonel, Garcia-Tsao Guadalupe

机构信息

Department of Internal Medicine B, University of Münster, Münster, Germany.

European Foundation for Study of Chronic Liver Failure, EASL-CLIF-Consortium, Barcelona, Spain.

出版信息

Hepatology. 2025 Jan 1;81(1):288-303. doi: 10.1097/HEP.0000000000000521. Epub 2023 Aug 7.

Abstract

Albumin is the most abundant protein in the human body and is synthetized exclusively by the liver. Therefore, serum albumin levels are reduced in acute and/or chronic liver disease. In cirrhosis, low levels of albumin predict the outcome. In advanced cirrhosis, the quality of albumin is decreased due to high oxidative stress and a proinflammatory state. Therefore, the administration of i.v. albumin would seem to be of pathophysiological relevance and benefit. Yet, the questions that remain are who, when, how much, and how often. While albumin infusion is recommended after large-volume paracentesis, at diagnosis of spontaneous bacterial peritonitis, in acute kidney injury, and in hepatorenal syndrome, the amount and schedule of albumin to be administered require refinement, particularly given complications related to volume overload that have become increasingly apparent. Other indications for albumin such as infections other than spontaneous bacterial peritonitis, hyponatremia, HE, prevention of poor outcomes in hospitalized, and in outpatients with cirrhosis are still debated. The results of studies in these settings are either negative, controversial, or inconclusive. This sheds some doubts regarding the use of albumin as a "one size fits all" strategy. The indication and patient selection are crucial and not always intuitive. The amount and frequency also seem to play a role in the success or failure of albumin. This review will critically discuss the evidence and underline areas where there are indications for albumin use and others where evidence is still insufficient and will have to await the development/results of randomized controlled trials.

摘要

白蛋白是人体中含量最丰富的蛋白质,且仅由肝脏合成。因此,急性和/或慢性肝病时血清白蛋白水平会降低。在肝硬化中,低水平白蛋白可预测病情转归。在晚期肝硬化中,由于高氧化应激和促炎状态,白蛋白质量下降。因此,静脉输注白蛋白似乎具有病理生理学意义且有益处。然而,仍存在的问题是哪些人、何时、输注多少以及多久输注一次。虽然推荐在大量腹腔穿刺放液后、诊断自发性细菌性腹膜炎时、急性肾损伤以及肝肾综合征时输注白蛋白,但白蛋白的输注量和给药方案仍需优化,尤其是考虑到与容量超负荷相关的并发症日益明显。白蛋白的其他适应证,如除自发性细菌性腹膜炎之外的感染、低钠血症、肝性脑病、预防住院患者及肝硬化门诊患者不良结局等,仍存在争议。这些情况下的研究结果要么为阴性,要么存在争议,要么尚无定论。这让人对将白蛋白作为“一刀切”的策略产生了一些怀疑。适应证和患者选择至关重要,且并非总是直观明了。输注量和频率似乎也对白蛋白治疗的成败有影响。本综述将批判性地讨论相关证据,并强调白蛋白有使用指征的领域以及证据仍不足、有待随机对照试验开展/得出结果的其他领域。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4b25/11643133/d1df975830e8/hep-81-288-g002.jpg

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