Literature DB >> 23485643

Substrate specificity of human carnitine acetyltransferase: Implications for fatty acid and branched-chain amino acid metabolism.

Sara Violante1, Lodewijk Ijlst, Jos Ruiter, Janet Koster, Henk van Lenthe, Marinus Duran, Isabel Tavares de Almeida, Ronald J A Wanders, Sander M Houten, Fátima V Ventura.   

Abstract

Carnitine acyltransferases catalyze the reversible conversion of acyl-CoAs into acylcarnitine esters. This family includes the mitochondrial enzymes carnitine palmitoyltransferase 2 (CPT2) and carnitine acetyltransferase (CrAT). CPT2 is part of the carnitine shuttle that is necessary to import fatty acids into mitochondria and catalyzes the conversion of acylcarnitines into acyl-CoAs. In addition, when mitochondrial fatty acid β-oxidation is impaired, CPT2 is able to catalyze the reverse reaction and converts accumulating long- and medium-chain acyl-CoAs into acylcarnitines for export from the matrix to the cytosol. However, CPT2 is inactive with short-chain acyl-CoAs and intermediates of the branched-chain amino acid oxidation pathway (BCAAO). In order to explore the origin of short-chain and branched-chain acylcarnitines that may accumulate in various organic acidemias, we performed substrate specificity studies using purified recombinant human CrAT. Various saturated, unsaturated and branched-chain acyl-CoA esters were tested and the synthesized acylcarnitines were quantified by ESI-MS/MS. We show that CrAT converts short- and medium-chain acyl-CoAs (C2 to C10-CoA), whereas no activity was observed with long-chain species. Trans-2-enoyl-CoA intermediates were found to be poor substrates for this enzyme. Furthermore, CrAT turned out to be active towards some but not all the BCAAO intermediates tested and no activity was found with dicarboxylic acyl-CoA esters. This suggests the existence of another enzyme able to handle the acyl-CoAs that are not substrates for CrAT and CPT2, but for which the corresponding acylcarnitines are well recognized as diagnostic markers in inborn errors of metabolism.
Copyright © 2013 Elsevier B.V. All rights reserved.

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Year:  2013        PMID: 23485643     DOI: 10.1016/j.bbadis.2013.02.012

Source DB:  PubMed          Journal:  Biochim Biophys Acta        ISSN: 0006-3002


  21 in total

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2.  Rewired metabolism in drug-resistant leukemia cells: a metabolic switch hallmarked by reduced dependence on exogenous glutamine.

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3.  Label-free quantitative protein profiling of vastus lateralis muscle during human aging.

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Journal:  Mol Cell Proteomics       Date:  2013-11-11       Impact factor: 5.911

4.  An LC-MS/MS method to quantify acylcarnitine species including isomeric and odd-numbered forms in plasma and tissues.

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Journal:  Genet Med       Date:  2020-10-19       Impact factor: 8.822

9.  Advantages of Studying the Metabolome in Response to Mixed-Macronutrient Challenges and Suggestions for Future Research Designs.

Authors:  Jennifer L LaBarre; Kanakadurga Singer; Charles F Burant
Journal:  J Nutr       Date:  2021-10-01       Impact factor: 4.687

10.  Lipidomic analysis of serum samples from migraine patients.

Authors:  Caixia Ren; Jia Liu; Juntuo Zhou; Hui Liang; Yayun Wang; Yinping Sun; Bin Ma; Yuxin Yin
Journal:  Lipids Health Dis       Date:  2018-02-02       Impact factor: 3.876

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