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Evaluation of the Hepa Wash® treatment in pigs with acute liver failure

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BORIS DOI
10.7892/boris.45144
Date of Publication
2013
Publication Type
Article
Division/Institute

Institut für Patholog...

Author
Al-Chalabi, Ahmed
Matevossian, Edouard
v. Thaden, Anne-K.
Luppa, Peter
Neiss, Albrecht
Schuster, Tibor
Yang, Zejian
Schreiber, Catherine
Schimmel, Patrick
Nairz, Ewald
Radermacher, Peter
Huber, Wolfgang
Schmid, Roland M.
Kreymann, Bernhard
Perren, Aurelorcid-logo
Institut für Pathologie
Subject(s)

500 - Science::570 - ...

600 - Technology::610...

Series
BMC gastroenterology
ISSN or ISBN (if monograph)
1471-230X
Publisher
BioMed Central
Language
English
Publisher DOI
10.1186/1471-230X-13-83
PubMed ID
23668774
Uncontrolled Keywords

Artificial liver

Acute liver failure

Albumin dialysis

Animal model

Swine

Renal dialysis

Multiple organ failur...

Capillary leak syndro...

Cardiovascular failur...

Renal failure

Description
BACKGROUND

Mortality of patients with acute liver failure (ALF) is still unacceptably high. Available liver support systems are still of limited success at improving survival. A new type of albumin dialysis, the Hepa Wash® system, was newly introduced. We evaluated the new liver support system as well as the Molecular Adsorbent Recycling System (MARS) in an ischemic porcine model of ALF.

METHODS

In the first study animals were randomly allocated to control (n=5) and Hepa Wash (n=6) groups. In a further pilot study, two animals were treated with the MARS-system. All animals received the same medical and surgical procedures. An intraparenchymal intracranial pressure was inserted. Hemodynamic monitoring and goal-directed fluid therapy using the PiCCO system was done. Animals underwent functional end-to-side portacaval shunt and ligation of hepatic arteries. Treatment with albumin dialysis was started after fall of cerebral perfusion pressure to 45 mmHg and continued for 8 h.

RESULTS

All animals in the Hepa Wash group survived the 13-hour observation period, except for one that died after stopping treatment. Four of the control animals died within this period (p=0.03). Hepa Wash significantly reduced impairment of cerebral perfusion pressure (23±2 vs. 10±3 mmHg, p=0.006) and mean arterial pressure (37±1 vs. 24±2 mmHg, p=0.006) but had no effect on intracranial pressure (14±1 vs. 15±1 mmHg, p=0.72). Hepa Wash also enhanced cardiac index (4.94±0.32 vs. 3.36±0.25 l/min/m2, p=0.006) and renal function (urine production, 1850 ± 570 vs. 420 ± 180 ml, p=0.045) and eliminated water soluble (creatinine, 1.3±0.2 vs. 3.2±0.3 mg/dl, p=0.01; ammonia 562±124 vs. 1382±92 μg/dl, p=0.006) and protein-bound toxins (nitrate/nitrite 5.54±1.57 vs. 49.82±13.27 μmol/l, p=0.01). No adverse events that could be attributed to the Hepa Wash treatment were observed.

CONCLUSIONS

Hepa Wash was a safe procedure and improved multiorgan system failure in pigs with ALF. The survival benefit could be the result of ameliorating different organ functions in association with the detoxification capacity of water soluble and protein-bound toxins.
Handle
https://boris-portal.unibe.ch/handle/20.500.12422/117112
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1471-230X-13-83.pdftextAdobe PDF530.35 KBAttribution (CC BY 4.0)publishedOpen
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