Literature DB >> 32843480

Defining Caenorhabditis elegans as a model system to investigate lipoic acid metabolism.

Antonela Lavatelli1,2, Diego de Mendoza1,2, María Cecilia Mansilla3,2.   

Abstract

Lipoic acid (LA) is a sulfur-containing cofactor that covalently binds to a variety of cognate enzymes that are essential for redox reactions in all three domains of life. Inherited mutations in the enzymes that make LA, namely lipoyl synthase, octanoyltransferase, and amidotransferase, result in devastating human metabolic disorders. Unfortunately, because many aspects of this essential pathway are still obscure, available treatments only serve to alleviate symptoms. We envisioned that the development of an organismal model system might provide new opportunities to interrogate LA biochemistry, biology, and physiology. Here we report our investigations on three Caenorhabditis elegans orthologous proteins involved in this post-translational modification. We established that M01F1.3 is a lipoyl synthase, ZC410.7 an octanoyltransferase, and C45G3.3 an amidotransferase. Worms subjected to RNAi against M01F1.3 and ZC410.7 manifest larval arrest in the second generation. The arrest was not rescued by LA supplementation, indicating that endogenous synthesis of LA is essential for C. elegans development. Expression of the enzymes M01F1.3, ZC410.7, and C45G3.3 completely rescue bacterial or yeast mutants affected in different steps of the lipoylation pathway, indicating functional overlap. Thus, we demonstrate that, similarly to humans, C. elegans is able to synthesize LA de novo via a lipoyl-relay pathway, and suggest that this nematode could be a valuable model to dissect the role of protein mislipoylation and to develop new therapies.
© 2020 Lavatelli et al.

Entities:  

Keywords:  Caenorhabditis elegans (C. elegans); RNA interference; RNA interference (RNAi); development; energy metabolism; fatty acid metabolism; inborn error of metabolism; lipoic acid; mitochondrial metabolism; oxidative stress; post-translational modification

Year:  2020        PMID: 32843480      PMCID: PMC7606682          DOI: 10.1074/jbc.RA120.013760

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  66 in total

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Authors:  Quin H Christensen; Natalia Martin; Maria C Mansilla; Diego de Mendoza; John E Cronan
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  1 in total

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