Discovery of a series of portimine-A fatty acid esters in mussels

Discovery of a series of portimine-A fatty acid esters in mussels

•Analyses of marine biotoxins in mussels by LC-MS/HRMS and LC-MS/MS.•Identification of unknown toxin analogs in shellfish.•Implementation of molecular networking for mapping and identifying toxin analogs.•Production of semi-synthesized fatty acid esters of portimine-A.•Discovery of 13-O-acyl esters...

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Veröffentlicht in:Harmful algae 2024-04, Vol.134, p.102621, Article 102621
Hauptverfasser: Hort, Vincent, Bourcier, Sophie
Format: Artikel
Sprache:eng
Schlagworte:
Animals
Bivalvia - chemistry
Bivalvia - metabolism
Chemical Sciences
Chromatography, Liquid
Dinoflagellida - chemistry
Dinoflagellida - metabolism
Environmental Sciences
Esters - chemistry
Esters - metabolism
Fatty Acids - analysis
Fatty Acids - chemistry
Fatty Acids - metabolism
France
Marine biotoxin fatty acid esters
Marine Toxins - chemistry
Marine Toxins - metabolism
Mass spectrometry
Pinnatoxins
Portimines
Shellfish
Vulcanodinium rugosum
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Zusammenfassung:•Analyses of marine biotoxins in mussels by LC-MS/HRMS and LC-MS/MS.•Identification of unknown toxin analogs in shellfish.•Implementation of molecular networking for mapping and identifying toxin analogs.•Production of semi-synthesized fatty acid esters of portimine-A.•Discovery of 13-O-acyl esters of portimine-A (n = 13) and a new pinnatoxin analog. Vulcanodinium rugosum is a benthic dinoflagellate known for producing pinnatoxins, pteriatoxins, portimines and kabirimine. In this study, we aimed to identify unknown analogs of these emerging toxins in mussels collected in the Ingril lagoon, France. First, untargeted data acquisitions were conducted by means of liquid chromatography coupled to hybrid quadrupole-orbitrap mass spectrometry. Data processing involved a molecular networking approach, and a workflow dedicated to the identification of biotransformed metabolites. Additionally, targeted analyses by liquid chromatography coupled to triple quadrupole mass spectrometry were also implemented to further investigate and confirm the identification of new compounds. For the first time, a series of 13-O-acyl esters of portimine-A (n = 13) were identified, with fatty acid chains ranging between C12:0 and C22:6. The profile was dominated by the palmitic acid conjugation. This discovery was supported by fractionation experiments combined with the implementation of a hydrolysis reaction, providing further evidence of the metabolite identities. Furthermore, several analogs were semi-synthesized, definitively confirming the discovery of these metabolization products. A new analog of pinnatoxin, with a molecular formula of C42H65NO9, was also identified across the year 2018, with the highest concentration observed in August (4.5 μg/kg). The MS/MS data collected for this compound exhibited strong structural similarities with PnTX-A and PnTX-G, likely indicating a substituent C2H5O2 in the side chain at C33. The discovery of these new analogs will contribute to deeper knowledge of the chemodiversity of toxins produced by V. rugosum or resulting from shellfish metabolism, thereby improving our ability to characterize the risks associated with these emerging toxins.
ISSN:1568-9883
1878-1470
1878-1470
DOI:10.1016/j.hal.2024.102621