L -Ornithine- L -aspartate lowers plasma and cerebrospinal fluid ammonia and prevents brain edema in rats with acute liver failure

Rose, Christopher F.; Michalak, Adrianna; Rao, Kakulavarapu V. Rama; Quack, G.; Kircheis, G.; Butterworth, Roger F.

doi:10.1002/hep.510300311

Cited by 142 publications

(86 citation statements)

References 27 publications

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“…Similar results have been described in vitro following the exposure of cultured astrocytes to ammonia (Norenberg et al, 1991). Furthermore, prevention of brain edema in rats with ALF has been shown with ammonia-lowering strategies (Cordoba et al, 1999;Rose et al, 1999Rose et al, , 2000. Unrelated to ammonia, swelling-induced glutamate release was demonstrated in cortical astrocytes exposed to a hypo-osmotic medium (Kimelberg et al, 1990).…”

Section: Calcium-independent Glutamate Releasesupporting

confidence: 78%

“…It has been suggested that ammonia plays an important role in the pathogenesis of brain edema (astrocytic swelling) in ALF. Increased brain water content has been described in both normal (Takahashi et al, 1991) and in portacaval shunted (Blei et al, 1994) rats infused with ammonia as well as in rats with liver devascularization (Rose et al, 1999). Similar results have been described in vitro following the exposure of cultured astrocytes to ammonia (Norenberg et al, 1991).…”

Section: Calcium-independent Glutamate Releasesupporting

confidence: 64%

“…In experimental animal models of ALF, brain ammonia levels may reach concentrations as high as 5 mM (Swain et al, 1992a), concentrations known to result in deleterious effects, by both direct and indirect mechanisms, on cerebral metabolism and neurotransmission. The importance of ammonia in ALF is emphasized and demonstrated in studies where ammonia-lowering strategies were shown to be beneficial in the prevention of brain edema and severe HE in rats with ALF (Cordoba et al, 1999;Rose et al, 1999Rose et al, , 2000. In the present review article, "ammonia" will be used to represent the sum of ammonium ions (NH4) and ammonia (NH3) unless a distinction is made.…”

Section: Ammonia In Alfmentioning

confidence: 99%

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Rose

2002

Metabolic Brain Disease

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Glutamatergic dysfunction has been suggested to play an important role in the pathogenesis of hepatic encephalopathy (HE) in acute liver failure (ALF). Increased extracellular brain glutamate concentrations have consistently been described in different experimental animal models of ALF and in patients with increased intracranial pressure due to ALF. High brain ammonia levels remain the leading candidate in the pathogenesis of HE in ALF and studies have demonstrated a correlation between ammonia and increased concentrations of extracellular brain glutamate both clinically and in experimental animal models of ALF. Inhibition of glutamate uptake or increased glutamate release from neurons and/or astrocytes could cause an increase in extracellular glutamate. This review analyses the effect of ammonia on glutamate release from (and uptake into) both neurons and astrocytes and how these pathophysiological mechanisms may be involved in the pathogenesis of HE in ALF.

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Section: Calcium-independent Glutamate Releasesupporting

confidence: 78%

Section: Calcium-independent Glutamate Releasesupporting

confidence: 64%

Section: Ammonia In Alfmentioning

confidence: 99%

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Rose

2002

Metabolic Brain Disease

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“…49 In rat model of acute liver failure (ALF), LOLA has been shown to prevent brain edema and hepatic encephalopathy which was accompanied by up regulation of muscle glutamine synthase activity and plasma glutamine levels were also raised indicating that LOLA in ALF may be beneficial. 50 A randomized placebo controlled double blind trial of LOLA in patients with ALF was recently published. 51 However LOLA therapy was not associated with decrease in ammonia levels or improvement in encephalopathy or survival (Figure 2).…”

Section: Ammonia Lowering Strategiesmentioning

confidence: 99%

Management in Acute Liver Failure

Shalimar

Acharya

2015

Journal of Clinical and Experimental Hepatology

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Acute liver failure (ALF) is a rare, potentially fatal complication of severe hepatic illness resulting from various causes. In a clinical setting, severe hepatic injury is usually recognised by the appearance of jaundice, encephalopathy and coagulopathy. The central and most important clinical event in ALF is occurrence of hepatic encephalopathy (HE) and cerebral edema which is responsible for most of the fatalities in this serious clinical syndrome. The pathogenesis of encephalopathy and cerebral edema in ALF is unique and multifactorial. Ammonia plays a central role in the pathogenesis. The role of newer ammonia lowering agents is still evolving. Liver transplant is the only effective therapy that has been identified to be of promise in those with poor prognostic factors, whereas in the others, aggressive intensive medical management has been documented to salvage a substantial proportion of patients. A small fraction of patients undergo liver transplant and the remaining are usually treated with medical therapy. Therefore, identification of the complications and causes of death in such patients, and use of appropriate prognostic models to identify those who need liver transplant and those who can be managed with medical treatment is a vital component of therapeutic strategy. In this review, we discuss the various pathogenetic mechanisms and treatment options available. ( J CLIN EXP HEPATOL 2015;5:S104-S115)A cute liver failure (ALF) can be a fatal complication of acute hepatic injury and occurs unpredictably. It is a rare clinical entity marked by the sudden loss of hepatic function and a severe life-threatening course in a person with no prior history of liver disease. ALF represents a syndrome rather than a specific disease, having multiple causes that vary in course and outcome. ALF is difficult to identify in its early stages, resulting in frequent delays in initiation of treatment. The causes of ALF include viral hepatitis, drug induced and toxin-induced liver damage, metabolic errors, ischemia, and miscellaneous rare causes.ALF is defined by three criteria: (1) rapid development of hepatocellular dysfunction (jaundice, coagulopathy), (2) encephalopathy, and (3) absence of a prior history of liver disease. 1 However, the interval between onset of acute hepatic injury (jaundice) and onset of liver failure (encephalopathy with or without coagulopathy) in such patients (icterus-encephalopathy interval; IEI) has been described to be between 4 weeks (Indian definition) 2-4 to 24 weeks (AASLD-ALF study group). 5 Further, due to the diverse natural course, ALF has been sub-classified as hyperacute (IEI # 7 day), acute (IEI # 4 weeks) and sub-acute ALF (IEI $ 5 week to #12 weeks) by British authors. 6 Despite these differences in definitions, the central and most important clinical event in ALF is occurrence of hepatic encephalopathy (HE) and cerebral edema which is responsible for most of the fatalities in this serious clinical syndrome. The pathogenesis of encephalopathy and cerebral edema in ALF is unique an...

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“…An infusion of ornithine-aspartate to rats with ischemic FHF reduced hyperammonemia and prevented the development of brain edema while resulting in a post-translational increase in glutamine synthetase activity in muscle. 22,23 Clinical trials with this agent, commercially available in Europe, should be performed cautiously, because the nitrogenous load could result in worsening of the clinical picture if human muscle does not respond in a similar fashion.…”

Section: The Swollen Astrocytementioning

confidence: 99%

Medical Therapy of Brain Edema in Fulminant Hepatic Failure

Blei

2000

Hepatology

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L -Ornithine- L -aspartate lowers plasma and cerebrospinal fluid ammonia and prevents brain edema in rats with acute liver failure

Cited by 142 publications

References 27 publications

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Management in Acute Liver Failure

Medical Therapy of Brain Edema in Fulminant Hepatic Failure

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