Literature DB >> 29686076

Elucidation of the trigonelline degradation pathway reveals previously undescribed enzymes and metabolites.

Nadia Perchat1, Pierre-Loïc Saaidi1, Ekaterina Darii1, Christine Pellé1, Jean-Louis Petit1, Marielle Besnard-Gonnet1, Véronique de Berardinis1, Maeva Dupont1, Alexandra Gimbernat1, Marcel Salanoubat1, Cécile Fischer2, Alain Perret2.   

Abstract

Trigonelline (TG; N-methylnicotinate) is a ubiquitous osmolyte. Although it is known that it can be degraded, the enzymes and metabolites have not been described so far. In this work, we challenged the laboratory model soil-borne, gram-negative bacterium Acinetobacter baylyi ADP1 (ADP1) for its ability to grow on TG and we identified a cluster of catabolic, transporter, and regulatory genes. We dissected the pathway to the level of enzymes and metabolites, and proceeded to in vitro reconstruction of the complete pathway by six purified proteins. The four enzymatic steps that lead from TG to methylamine and succinate are described, and the structures of previously undescribed metabolites are provided. Unlike many aromatic compounds that undergo hydroxylation prior to ring cleavage, the first step of TG catabolism proceeds through direct cleavage of the C5-C6 bound, catalyzed by a flavin-dependent, two-component oxygenase, which yields (Z)-2-((N-methylformamido)methylene)-5-hydroxy-butyrolactone (MFMB). MFMB is then oxidized into (E)-2-((N-methylformamido) methylene) succinate (MFMS), which is split up by a hydrolase into carbon dioxide, methylamine, formic acid, and succinate semialdehyde (SSA). SSA eventually fuels up the TCA by means of an SSA dehydrogenase, assisted by a Conserved Hypothetical Protein. The cluster is conserved across marine, soil, and plant-associated bacteria. This emphasizes the role of TG as a ubiquitous nutrient for which an efficient microbial catabolic toolbox is available.

Entities:  

Keywords:  LC/MS-Orbitrap; N-heterocycle degradation; bacterial metabolism; functional genomics; trigonelline

Mesh:

Substances:

Year:  2018        PMID: 29686076      PMCID: PMC5948990          DOI: 10.1073/pnas.1722368115

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


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