Targeted albumin infusions in hospitalized patients with cirrhosis receiving terlipressin: A post-hoc analysis of ATTIRE.

IF 4.4 3区医学 Q2 GASTROENTEROLOGY & HEPATOLOGY

Annals of hepatology Pub Date : 2025-07-01 DOI:10.1016/j.aohep.2025.101941

Nikolaj Torp, Louise China, Mads Israelsen, Ewan Forrest, Nick Freemantle, Jonel Trebicka, Aleksander Krag, Alastair O'Brien

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Abstract

Introduction and objectives: The ATTIRE trial showed increased severe adverse events with targeted albumin therapy. Safety concerns exist regarding albumin-terlipressin use for hepatorenal syndrome-acute kidney injury (HRS-AKI), but terlipressin is also used for variceal bleeding and hypotension. We evaluated the safety of terlipressin and albumin for any indication using ATTIRE data.

Materials and methods: In ATTIRE, hospitalized decompensated cirrhosis patients were randomized to daily 20 % albumin (serum albumin ≥30 g/L) or standard care for up to 14 days post-randomization. Of 777 patients, 42 received terlipressin at randomization in the targeted albumin arm and 41 in standard care. We studied death and fluid-related complications from serious adverse event reporting during the 15-day trial period.

Results: Indications for terlipressin were variceal bleeding (73 %), HRS-AKI (23 %) and sepsis-induced hypotension (3 %). Median albumin dosing was higher with targeted albumin than standard care for variceal bleeding (200 g vs. 0 g) and sepsis-induced hypotension (180 g vs. 0 g), but similar for HRS-AKI (220 g vs. 230 g). A composite of death and fluid-related complications was more common with targeted albumin compared to standard care (log-rank: p = 0.011), where the increased risk persisted when adjusting for baseline MELD. This composite outcome occurred more often in variceal bleeding patients treated with targeted albumin (n = 7) compared to standard care (n = 2), although the difference was not statistically significant (p = 0.064).

Conclusions: In hospitalized cirrhosis patients, targeted albumin infusions with terlipressin may increase the risk of death and fluid-related complications, particularly in variceal bleeding. Caution is warranted when using albumin in this subgroup.

Clinical trial number: EudraCT number: 2014-002,300-24 and International Standard RCT Number: 14,174,793 Research Ethics Committee Number: 15/LO/0104.

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肝硬化住院患者接受特利加压素的靶向白蛋白输注：装束的事后分析。

介绍和目的：装束试验显示靶向白蛋白治疗增加了严重不良事件。白蛋白-特利加压素用于肝肾综合征-急性肾损伤（HRS-AKI）存在安全性问题，但特利加压素也用于静脉曲张出血和低血压。我们使用装束数据评估特利加压素和白蛋白在任何适应症中的安全性。材料和方法：在实验组中，住院失代偿期肝硬化患者随机分为每日20%白蛋白（血清白蛋白≥30 g/L）或标准治疗组，随机分组后14天。在777例患者中，42例在靶向白蛋白组随机接受特利加压素治疗，41例接受标准治疗。在15天的试验期间，我们研究了严重不良事件报告中的死亡和液体相关并发症。结果：特利加压素的适应症为静脉曲张出血（73%）、HRS-AKI（23%）和败血症性低血压（3%）。针对静脉曲张出血（200 g vs. 0 g）和败血症性低血压（180 g vs. 0 g），靶向白蛋白的中位白蛋白剂量高于标准治疗，但对于hr - aki （220 g vs. 230 g）相似。与标准治疗相比，靶向白蛋白治疗更常见死亡和液体相关并发症的复合（log-rank: p = 0.011），在调整基线MELD后，风险持续增加。与标准治疗（n=2）相比，靶向白蛋白治疗的静脉曲张出血患者（n=7）更常出现这种复合结果，尽管差异无统计学意义（p=0.064）。结论：在住院的肝硬化患者中，靶向白蛋白输注特利加压素可能会增加死亡和液体相关并发症的风险，尤其是静脉曲张出血。在这个亚组中使用白蛋白需要谨慎。临床试验号：edract号：2014-002300-24；国际标准RCT号：14174793；研究伦理委员会号：15/LO/0104。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Annals of hepatology 医学-胃肠肝病学

CiteScore

7.90

自引率

2.60%

发文量

183

审稿时长

4-8 weeks

期刊介绍： Annals of Hepatology publishes original research on the biology and diseases of the liver in both humans and experimental models. Contributions may be submitted as regular articles. The journal also publishes concise reviews of both basic and clinical topics.