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L-ornithine L-aspartate lowers ammonia and improves cognitive function but not mortality in hepatic encephalopathy from acute on chronic liver failure

L-ornithine L-aspartate lowers ammonia and improves cognitive function but not mortality in hepatic encephalopathy from acute on chronic liver failure
L-ornithine L-aspartate lowers ammonia and improves cognitive function but not mortality in hepatic encephalopathy from acute on chronic liver failure
L-ornithine L-aspartate (LOLA) has been known as an effective ammonia-lowering agent for more than 50 years with good evidence in hepatic encephalopathy. Administration of LOLA removes ammonia via two distinct mechanisms: by synthesis of urea and by the synthesis of glutamine via the enzyme glutamine synthetase. While LOLA has been used in cirrhosis and acute liver injury settings, it is less clear if LOLA could be used in non-alcoholic fatty liver disease (NAFLD). NAFLD and the progressive form non-alcoholic steatohepatitis (NASH) are currently the leading causes of chronic liver disease worldwide, with roughly 25% of the world population affected by NAFLD. Consequences of NASH are end-stage liver disease and cardiovascular morbidity and mortality. As the basis for NAFLD is excess calorie uptake and excess adipose tissue mass, the conservative therapeutic approach is weight loss by intense lifestyle change. However, no pharmacological treatment options are currently approved. LOLA is being investigated as a pharmacological tool to ameliorate liver injury in NAFLD on the basis that it lowers liver ammonia concentrations and supplies anti-oxidative glutamine and glutathione. Indirect hepatoprotective effects currently under investigation could also be beneficial.
10.1177_17511437221095122
McKenzie, Cathrine
ec344dee-5777-49c5-970e-6326e82c9f8c
Auzinger, George
49631160-aa3a-4fe9-a109-36563ef27c6d
Sawieres, Sarah
c55ccbbf-aeb5-4050-bf5c-e2ca01241961
McKenzie, Cathrine
ec344dee-5777-49c5-970e-6326e82c9f8c
Auzinger, George
49631160-aa3a-4fe9-a109-36563ef27c6d
Sawieres, Sarah
c55ccbbf-aeb5-4050-bf5c-e2ca01241961

McKenzie, Cathrine, Auzinger, George and Sawieres, Sarah (2021) L-ornithine L-aspartate lowers ammonia and improves cognitive function but not mortality in hepatic encephalopathy from acute on chronic liver failure. Intensive Care State of the Art Meeting 2021. 06 - 08 Dec 2021. 6 pp . (doi:10.1177_17511437221095122).

Record type: Conference or Workshop Item (Paper)

Abstract

L-ornithine L-aspartate (LOLA) has been known as an effective ammonia-lowering agent for more than 50 years with good evidence in hepatic encephalopathy. Administration of LOLA removes ammonia via two distinct mechanisms: by synthesis of urea and by the synthesis of glutamine via the enzyme glutamine synthetase. While LOLA has been used in cirrhosis and acute liver injury settings, it is less clear if LOLA could be used in non-alcoholic fatty liver disease (NAFLD). NAFLD and the progressive form non-alcoholic steatohepatitis (NASH) are currently the leading causes of chronic liver disease worldwide, with roughly 25% of the world population affected by NAFLD. Consequences of NASH are end-stage liver disease and cardiovascular morbidity and mortality. As the basis for NAFLD is excess calorie uptake and excess adipose tissue mass, the conservative therapeutic approach is weight loss by intense lifestyle change. However, no pharmacological treatment options are currently approved. LOLA is being investigated as a pharmacological tool to ameliorate liver injury in NAFLD on the basis that it lowers liver ammonia concentrations and supplies anti-oxidative glutamine and glutathione. Indirect hepatoprotective effects currently under investigation could also be beneficial.

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More information

Published date: 1 January 2021
Venue - Dates: Intensive Care State of the Art Meeting 2021, 2021-12-06 - 2021-12-08

Identifiers

Local EPrints ID: 479005
URI: http://eprints.soton.ac.uk/id/eprint/479005
PURE UUID: b5864e78-e3ae-4fdd-ad6b-473a1a22c48f
ORCID for Cathrine McKenzie: ORCID iD orcid.org/0000-0002-5190-9711

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Date deposited: 17 Jul 2023 16:54
Last modified: 10 Apr 2024 02:14

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Author: Cathrine McKenzie ORCID iD
Author: George Auzinger
Author: Sarah Sawieres

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