Development of an invasively monitored porcine model of acetaminophen-induced acute liver failure

Newsome, Philip N.; Henderson, Neil C.; Nelson, Leonard J.; Dabos, Costas; Filippi, Céline; Bellamy, Christopher; Howie, Forbes; Clutton, R Eddie; King, Tim; Lee, Alistair; Hayes, Peter; Plevris, John

doi:10.1186/1471-230x-10-34

Cited by 34 publications

(46 citation statements)

References 22 publications

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“…Previous attempts to establish a standardized APAP intoxication model[13-15,20] were unsuccessful. Thiel et al[20] administered APAP directly into the upper jejunum via an implanted catheter, and this route of administration was affected by anesthesia, laparotomy and jejunotomy.…”

Section: Discussionmentioning

confidence: 99%

Artificial liver support in pigs with acetaminophen-induced acute liver failure

He¹,

Feng²,

Cai³

et al. 2017

WJG

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AIMTo establish a reversible porcine model of acute liver failure (ALF) and treat it with an artificial liver system.METHODSSixteen pigs weighing 30-35 kg were chosen and administered with acetaminophen (APAP) to induce ALF. ALF pigs were then randomly assigned to either an experimental group (n = 11), in which a treatment procedure was performed, or a control group (n = 5). Treatment was started 20 h after APAP administration and continued for 8 h. Clinical manifestations of all animals, including liver and kidney functions, serum biochemical parameters and survival times were analyzed.RESULTSTwenty hours after APAP administration, the levels of serum aspartate aminotransferase, total bilirubin, creatinine and ammonia were significantly increased, while albumin levels were decreased (P < 0.05). Prothrombin time was found to be extended with progression of ALF. After continuous treatment for 8 h (at 28 h), aspartate aminotransferase, total bilirubin, creatinine, and ammonia showed a decrease in comparison with the control group (P < 0.05). A cross-section of livers revealed signs of vacuolar degeneration, nuclear fragmentation and dissolution. Concerning survival, porcine models in the treatment group survived for longer times with artificial liver system treatment (P < 0.05).CONCLUSIONThis model is reproducible and allows for quantitative evaluation of new liver systems, such as a bioartificial liver. The artificial liver system (ZHJ-3) is safe and effective for the APAP-induced porcine ALF model.

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Section: Discussionmentioning

confidence: 99%

Artificial liver support in pigs with acetaminophen-induced acute liver failure

He¹,

Feng²,

Cai³

et al. 2017

WJG

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“…The recently published acetaminophen intoxication model of Newsome et al [15] does not produce defined survival times. In addition to this, intravenous application of acetaminophen seems to produce more toxic side effects and does not reflect the clinical situation.…”

Section: Discussionmentioning

confidence: 99%

“…There is an unmet clinical need to provide a relevant, reproducible large animal model of acetaminophen-induced ALF in which to test putative therapies such as novel hepatic support systems or new pharmacological agents designed to address these issues. Numerous studies with pig models using acetaminophen to induce ALF have produced heterogeneous results [13,14,15] due to the existence of significant variations in the hepatic detoxifying metabolism of the drug related to species and age [16]. But reproducibility in the development of ALF within a reasonable time range and survival time in ALF remained unpredictable [17] and death of many pigs occurred due to toxic side effects.…”

Section: Introductionmentioning

confidence: 99%

A Reproducible Porcine Model of Acute Liver Failure Induced by Intrajejunal Acetaminophen Administration

Thiel

Thiel²,

Etspueler³

et al. 2011

Eur Surg Res

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Background and Aims: Severe intoxication following acetaminophen overdose is the most common cause of acute liver failure (ALF) in many Western European and North American countries. A reproducible large animal model of acetaminophen intoxication has not been successfully evaluated previously. Methods: Eight male pigs underwent acetaminophen intoxication receiving an initial enteric bolus of 250 mg/kg body weight acetaminophen followed by an acetaminophen plasma level (300–450 mg/l) adapted enteric maintenance dose of 1,000–3,000 mg/h to the onset of ALF (prothrombin time value <30%). Vital and ventilation parameters were continuously recorded until death. Saline, hydroxyethyl starch, fresh frozen plasma and erythrocyte units were used for volume substitution, and norepinephrine to prevent severe hypotension. Results: All animals developed ALF after 25 ± 3 h, which was confirmed by laboratory values, the clinical course and histological examinations. All animals died due to ALF after a further 21 ± 5 h, precipitated by cerebral edema. Conclusions: Using an initial enteric acetaminophen bolus, followed by body weight-adapted acetaminophen plasma level intoxication, it was possible to establish a reproducible, clinically relevant porcine model which may be used for the investigation of novel therapeutic approaches in this life-threatening condition.

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“…In these models, hepatic failure was achieved by intoxication with galactosamine or acetaminophen [8-10], hepatic ischemia by portocaval shunting following transient clamping of the hepatic artery [11,12], and extended resection or even total hepatectomy [13-21]. Unfortunately, all aforementioned models involve various limitations, thus affecting morbidity in the assessment of a given intervention.…”

Section: Introductionmentioning

confidence: 99%

Standardized intensive care unit management in an anhepatic pig model: new standards for analyzing liver support systems

Thiel

Etspueler

et al. 2010

Crit Care

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IntroductionSeveral anhepatic pig models were developed in the past. Most models suffer from short anhepatic survival times due to insufficient postoperative intensive care unit (ICU) management. The aim of this study was to analyze anhepatic survival time under standardized intensive care therapy in a pig model.MethodsEight pigs underwent total hepatectomy after Y-graft interposition between the infrahepatic vena cava and the portal vein to the suprahepatic vena cava. An intracranial probe was inserted for intracranial pressure (ICP) monitoring. Animals received pressure-controlled ventilation under deep narcosis. Vital parameters were continuously recorded. Urinary output, blood gas analysis, haemoglobin, hematocrit, serum electrolytes, lactate, and glucose were monitored hourly, and creatinine, prothrombin time, international normalised ratio, and serum albumin were monitored every 8 hours. Sodium chloride solution 0.9%, hydroxyethyl starch 6%, fresh frozen plasma, and erythrocyte units were used for volume substitution, and norepinephrine was used to prevent severe hypotension. Serum electrolytes and acid-base balance were corrected as required. Antibiotic prophylaxis with ceftriaxon was given daily, as well as furosemide, to maintain diuresis.ResultsPostoperative survival was 100% after 24 hours, with a maximum survival of 73 (mean, 58 ± 4) hours. Haemodynamic parameters such as heart rate, mean arterial pressure, and pulse oximetry remained stable during surgical procedures and following anhepatic status due to ICU therapy until escalating at time of death. Deteriorating pulmonary function could be stabilized by increasing oxygen concentration, positive end-expiratory pressure, and maximal airway pressure. Furosemide was used to maintain diuresis until renal failure occurred. ICP started at 15-17 mmHg and increased continuously up to levels of 41-43 mmHg at time of death. All animals died as a result of multiple-organ failure.ConclusionsUsing standardized intensive care management after total hepatectomy, we were able to prolong anhepatic survival over 58 hours without the use of liver support systems. The survival benefit of liver support systems in previous animal studies should be reevaluated against our model.

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Development of an invasively monitored porcine model of acetaminophen-induced acute liver failure

Cited by 34 publications

References 22 publications

Artificial liver support in pigs with acetaminophen-induced acute liver failure

Artificial liver support in pigs with acetaminophen-induced acute liver failure

A Reproducible Porcine Model of Acute Liver Failure Induced by Intrajejunal Acetaminophen Administration

Standardized intensive care unit management in an anhepatic pig model: new standards for analyzing liver support systems

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