Brain Muscle Axis During Treatment of Hepatic Encephalopathy With L-ornithine L-aspartate
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About
Patients with cirrhosis of the liver may suffer from a condition called hepatic encephalopathy which in its mildest form as mental slowing and impaired reaction times in driving and machinery operation. Left untreated it may lead to deep coma. The cause is not fully understood but is though to be related to the inability of a damaged liver to filter out toxins such as ammonia in the blood, which then accumulate within the brain and result in altered function and swelling within certain brain cells,astrocytes. These patients also suffer from muscle loss, which is associated with a poor outcome. L-ornithine L-aspartate(LOLA) is a licensed drug in Germany and has been shown to promote ammonia elimination from the body in the form of urea. Some experimental studies have suggested that LOLA also potentially attenuates muscle loss by incorporating ammonia into muscle in the form of glutamine. The aim of this study is to determine cognitive and nutritional effects of 12 weeks of LOLA administration and its effect on brain muscle structure and function in patients with cirrhosis.
Full description
This is a Phase IV randomised double blind, placebo controlled study. Thirty four patients with cirrhosis will be studied with psychometric tests, clinical brain magnetic resonance imaging(MRI),including functional MRI) and magnetic resonance spectroscopy (MRS) and muscle MRI of leg muscle before (time 0)during (4weeks)and after LOLA or placebo treatment at 12 weeks. Samples will also be taken for ex vivo MRS of blood and urine to identify potential biomarkers. Histological analysis and MRS would also be performed on the muscle tissue at the same time points.
Hypotheses Primary objective
- Improvement in mental state by paper and pencil based Psychometric Hepatic Encephalopathy Score (PHES) and Cogstate Research test (computer based cognitive research assessment tool)
Secondary objectives
- Brain volume reduction due to reduction in brain swelling measured by MRI and improvement in the chemical structure of the brain due to (cerebral osmolytes)measured by in vivo MR Spectroscopy (MRS)scanning of the brain.
- Improvement in brain function
- Improvement in muscle function (muscle metabolome normalisation) and increased muscle size (fat free mass), measured in vivo by MRI scanning and by in vitro mass spectroscopy and NMR spectroscopy and histological analysis of muscle samples.
- Improvement in the chemical profile of key chemicals in the blood and urine, measured with in vitro NMR spectroscopy
Enrollment
Sex
Ages
Volunteers
Inclusion criteria
- Ambulant patients of any Child-Pugh stage cirrhosi and PHEs defined MHe or grade 1 encephalopathy
Exclusion criteria
- Previous episodes of overt HE without a clear precipitant
- Recurrent excessive alcohol consumption (abstinence for those with alcoholic liver disease otherwise less than 28 units per week)
- Severe coagulopathy (INR>2, platelets <60 000/uL, Fibrinogen <1mg/dl)
- known myopathy or myositis, taruma to lower extremities within 3 months)
- Renal dysfunction with a serum creatinine>3mg/dl (265micromol/L)
- Ferromagnetic implants
- Recent intestinal haemorrhage within 1 month
- Claustrophobia
- Weight >120kg
- Major psychoactive medication such as antipsychotic agents
- Known cerebrovascular disease or pre-existing neurological conditions
- Age less than 18 or greater than 65.
Trial design
Primary purpose
Allocation
Interventional model
Masking
42 participants in 2 patient groups, including a placebo group
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Data sourced from clinicaltrials.gov
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