分子吸附再循环系统在治疗肝硬化伴腹水且血管收缩剂治疗失败的 1 型肝肾综合征患者方面无效。

Molecular adsorbent recirculating system is ineffective in the management of type 1 hepatorenal syndrome in patients with cirrhosis with ascites who have failed vasoconstrictor treatment.

机构信息

Division of Gastroenterology, Department of Medicine, University of Toronto, 9N/983 Toronto General Hospital, 200 Elizabeth Street, Toronto M5G 2C4, Ontario, Canada.

出版信息

Gut. 2010 Mar;59(3):381-6. doi: 10.1136/gut.2008.174615. Epub 2009 Aug 25.

DOI:10.1136/gut.2008.174615

PMID:19710033

Abstract

BACKGROUND

The pathogenetic mechanism of hepatorenal syndrome (HRS) is paradoxical renal vasoconstriction consequent upon systemic and splanchnic arterial vasodilatation. Molecular adsorbent recirculating system (MARS) is a specialised form of dialysis that clears albumin-bound substances, including vasodilators, and therefore can potentially reduce systemic vasodilatation in cirrhosis.

OBJECTIVE

To assess the efficacy of MARS in improving systemic and renal haemodynamics in patients with cirrhosis with refractory ascites and type 1 HRS not responding to vasoconstrictor therapy.

METHODS

A pilot study was carried out in an academic teaching hospital. The study group comprised six patients with cirrhosis, refractory ascites and type 1 HRS not responding to vasoconstrictor treatment. All patients received 5 days of 6-8 h of MARS dialysis. The main outcome measures were pre-MARS and post-MARS measurements of glomerular filtration rate, renal blood flow, neurohormones, cytokines and nitric oxide (NO), as well as daily biochemistry, haematology and urinary volume.

RESULTS

There were no significant changes in systemic haemodynamics and GFR following MARS treatments, despite a significant reduction in NO concentrations (111.5+/-18.8 micromol/l pre-MARS, to 65.1+/-8.2 micromol/l post-MARS, p=0.05). There was a transient reduction in serum creatinine (p<0.05), Child-Pugh and MELD (Model End-Stage Liver Disease) scores with MARS, but no significant difference was observed in neurohormone and cytokine levels. Four of six patients died following MARS treatments.

CONCLUSIONS

In patients with cirrhosis, refractory ascites and type 1 HRS not responding to vasoconstrictor treatment, MARS is ineffective in improving systemic haemodynamics and renal function despite reduction in NO levels, suggesting that vasodilatation in advanced cirrhosis is not due to excess systemic vasodilators alone. Transient reduction in serum creatinine indicates direct removal by MARS, and may not represent improved renal function.

摘要

背景

肝肾综合征（HRS）的发病机制是矛盾的肾血管收缩继发于全身和内脏动脉血管舒张。分子吸附再循环系统（MARS）是一种特殊形式的透析，可以清除白蛋白结合的物质，包括血管扩张剂，因此可能会降低肝硬化患者的全身血管舒张。

目的

评估 MARS 在改善肝硬化伴难治性腹水和对血管收缩剂治疗无反应的 1 型 HRS 患者的全身和肾脏血液动力学方面的疗效。

方法

在一所学术教学医院进行了一项试点研究。研究组包括 6 例肝硬化、难治性腹水和对血管收缩剂治疗无反应的 1 型 HRS 患者。所有患者均接受 5 天 6-8 小时的 MARS 透析。主要观察指标为 MARS 治疗前后肾小球滤过率、肾血流量、神经激素、细胞因子和一氧化氮（NO）的测量值，以及每日生化、血液学和尿量。

结果

尽管 NO 浓度显著降低（MARS 治疗前 111.5+/-18.8 μmol/L，治疗后 65.1+/-8.2 μmol/L，p=0.05），但全身血液动力学和 GFR 无明显变化。MARS 治疗后血清肌酐（p<0.05）、Child-Pugh 和 MELD（终末期肝病模型）评分短暂降低，但神经激素和细胞因子水平无显著差异。MARS 治疗后，6 例患者中有 4 例死亡。