Mitochondrial targets in hyperammonemia: Addressing urea cycle function to improve drug therapies

Marco F Moedas; Ricardo J M Simões; Margarida F B Silva

doi:10.1016/j.bcp.2024.116034

Mitochondrial targets in hyperammonemia: Addressing urea cycle function to improve drug therapies

Biochem Pharmacol. 2024 Apr:222:116034. doi: 10.1016/j.bcp.2024.116034. Epub 2024 Feb 1.

Authors

Marco F Moedas¹, Ricardo J M Simões², Margarida F B Silva³

Affiliations

¹ Research Institute for Medicines-iMed.ULisboa, Faculty of Pharmacy, Universidade de Lisboa, Av. Prof. Gama Pinto, 1649-003 Lisboa, Portugal; Centre for Inherited Metabolic Diseases, Karolinska University Hospital, Stockholm, Sweden; Department of Medical Biochemistry and Biophysics, Karolinska Institutet, Stockholm, Sweden.
² Research Institute for Medicines-iMed.ULisboa, Faculty of Pharmacy, Universidade de Lisboa, Av. Prof. Gama Pinto, 1649-003 Lisboa, Portugal.
³ Research Institute for Medicines-iMed.ULisboa, Faculty of Pharmacy, Universidade de Lisboa, Av. Prof. Gama Pinto, 1649-003 Lisboa, Portugal. Electronic address: mbsilva@ff.ulisboa.pt.

PMID: 38307136
DOI: 10.1016/j.bcp.2024.116034

Abstract

The urea cycle (UC) is a critically important metabolic process for the disposal of nitrogen (ammonia) produced by amino acids catabolism. The impairment of this liver-specific pathway induced either by primary genetic defects or by secondary causes, namely those associated with hepatic disease or drug administration, may result in serious clinical consequences. Urea cycle disorders (UCD) and certain organic acidurias are the major groups of inherited rare diseases manifested with hyperammonemia (HA) with UC dysregulation. Importantly, several commonly prescribed drugs, including antiepileptics in monotherapy or polytherapy from carbamazepine to valproic acid or specific antineoplastic agents such as asparaginase or 5-fluorouracil may be associated with HA by mechanisms not fully elucidated. HA, disclosing an imbalance between ammoniagenesis and ammonia disposal via the UC, can evolve to encephalopathy which may lead to significant morbidity and central nervous system damage. This review will focus on biochemical mechanisms related with HA emphasizing some poorly understood perspectives behind the disruption of the UC and mitochondrial energy metabolism, namely: i) changes in acetyl-CoA or NAD⁺ levels in subcellular compartments; ii) post-translational modifications of key UC-related enzymes, namely acetylation, potentially affecting their catalytic activity; iii) the mitochondrial sirtuins-mediated role in ureagenesis. Moreover, the main UCD associated with HA will be summarized to highlight the relevance of investigating possible genetic mutations to account for unexpected HA during certain pharmacological therapies. The ammonia-induced effects should be avoided or overcome as part of safer therapeutic strategies to protect patients under treatment with drugs that may be potentially associated with HA.

Keywords: Ammonia; Drug-induced liver injury; Hepatic encephalopathy; Hyperammonemia; Urea cycle disorders; Valproate-induced hyperammonemic encephalopathy.

Publication types

Review

MeSH terms

Ammonia / metabolism
Humans
Hyperammonemia* / drug therapy
Hyperammonemia* / etiology
Hyperammonemia* / metabolism
Liver Diseases*
Urea / therapeutic use

Substances

Ammonia
Urea