Artículo
Impairment of lipoylation mediated by bromooctanoate targets eukaryotic amidotransferases
Scattolini, Albertina
; Costa, Joaquin; Pianessi, Tulio L.; Uttaro, Antonio Domingo
; Mansilla, Maria Cecilia



Fecha de publicación:
12/2024
Editorial:
Wiley Blackwell Publishing, Inc
Revista:
Molecular Microbiology
ISSN:
0950-382X
Idioma:
Inglés
Tipo de recurso:
Artículo publicado
Clasificación temática:
Resumen
Lipoylation is a post-translational modification in which lipoic acid is attached to specific apoproteins of enzyme complexes, like E2 subunits of dehydrogenases or GcvH of the glycine cleavage system. A defining feature of organisms with a lipoyl-relay system is the presence of amidotransferase activity, which enables the transfer of lipoyl groups attached to intermediary proteins to the E2 subunits. In this study, we characterized the lipoate metabolism of Capsaspora owczarzaki and Plasmodium falciparum. Both organisms utilize amidotransferases in their lipoylation pathways, with the filasterian enzyme playing a key role in lipoate synthesis, while the apicomplexan counterpart, previously considered a lipoyltransferase, is essential in its lipoate salvage pathway. We also discovered that specific structural features and certain conserved domains in eukaryotic amidotransferases can significantly influence their mechanism of action and susceptibility to the lipoate analog bromooctanoate. Overall, this study highlights the metabolic strategies of C. owczarzaki and emphasizes the critical role of amidotransferases as ancestral enzymes in the evolution of lipoate metabolism, suggesting that the lipoyl relay may represent a universal pathway across diverse clades.
Palabras clave:
AMIDOTRANSFERASE
,
ANTIMICROBIAL
,
CAPSASPORA
,
LIPOIC ACID
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Articulos(IBR)
Articulos de INST.DE BIOLOGIA MOLECULAR Y CELULAR DE ROSARIO
Articulos de INST.DE BIOLOGIA MOLECULAR Y CELULAR DE ROSARIO
Citación
Scattolini, Albertina; Costa, Joaquin; Pianessi, Tulio L.; Uttaro, Antonio Domingo; Mansilla, Maria Cecilia; Impairment of lipoylation mediated by bromooctanoate targets eukaryotic amidotransferases; Wiley Blackwell Publishing, Inc; Molecular Microbiology; 2024; 12-2024; 1-23
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