Literature DB >> 28836704

A novel lipoate attachment enzyme is shared by Plasmodium and Chlamydia species.

Gustavo A Afanador1, Alfredo J Guerra1, Russell P Swift1, Ryan E Rodriguez1, David Bartee2, Krista A Matthews1, Arne Schön3, Ernesto Freire3, Caren L Freel Meyers2, Sean T Prigge1.   

Abstract

Lipoate is an essential cofactor for enzymes that are important for central metabolism and other processes. In malaria parasites, scavenged lipoate from the human host is required for survival. The Plasmodium falciparum mitochondrion contains two enzymes (PfLipL1 and PfLipL2) that are responsible for activating mitochondrial proteins through the covalent attachment of lipoate (lipoylation). Lipoylation occurs via a novel redox-gated mechanism that remains poorly understood. We show that PfLipL1 functions as a redox switch that determines which downstream proteins will be activated. Based on the lipoate redox state, PfLipL1 either functions as a canonical lipoate ligase or as a lipoate activating enzyme which works in conjunction with PfLipL2. We demonstrate that PfLipL2 is a lipoyltransferase and is a member of a novel clade of lipoate attachment enzymes. We show that a LipL2 enzyme from Chlamydia trachomatis has similar activity, demonstrating conservation between intracellular pathogens from different phylogenetic kingdoms and supporting the hypothesis that an early ancestor of malaria parasites once contained a chlamydial endosymbiont. Redox-dependent lipoylation may regulate processes such as central metabolism and oxidative defense pathways.
© 2017 John Wiley & Sons Ltd.

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Year:  2017        PMID: 28836704      PMCID: PMC5653438          DOI: 10.1111/mmi.13776

Source DB:  PubMed          Journal:  Mol Microbiol        ISSN: 0950-382X            Impact factor:   3.501


  54 in total

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3.  Crystal structure of lipoate-bound lipoate ligase 1, LipL1, from Plasmodium falciparum.

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6.  A Novel Lipoate-Protein Ligase, Mhp-LplJ, Is Required for Lipoic Acid Metabolism in Mycoplasma hyopneumoniae.

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