## Abstract The mass fragmentation of potato glycoalkaloids, α‐solanine and α‐chaconine, and the aglycons, demissidine and solasodine were studied using the Orbitrap Fourier transform (FT) mass spectrometer. Using the linear ion trap (LIT) mass spectrometry, multistage collisional‐induced dissociat
Elucidation of the fragmentation pathways of azaspiracids, using electrospray ionisation, hydrogen/deuterium exchange, and multiple-stage mass spectrometry
✍ Scribed by Mónica Díaz Sierra; Ambrose Furey; Brett Hamilton; Mary Lehane; Kevin J. James
- Publisher
- John Wiley and Sons
- Year
- 2003
- Tongue
- English
- Weight
- 170 KB
- Volume
- 38
- Category
- Article
- ISSN
- 1076-5174
- DOI
- 10.1002/jms.526
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✦ Synopsis
Abstract
Collision‐induced dissociation (CID) mass spectra were generated for azaspiracids using electrospray ionisation (ESI), and hydrogen/deuterium (H/D) exchange was used to ascertain the number and type of replaceable hydrogens in the three predominant azaspiracid toxins. H/D exchange was conveniently achieved using deuterated solvents for liquid chromatography (LC). Using ion‐trap mass spectrometry, multiple‐stage CID experiments (MS^n^) on the protonated and fully exchanged ions were performed to decipher characteristic fragmentation pathways. The precursor and product ions from azaspiracids lost up to five water molecules from different regions during MS^n^ experiments and it was possible to distinguish between the water losses from different molecular regions. These studies confirmed that the first water‐loss ion in the spectra of azaspiracids resulted from dehydration at the vicinal diol at C20–C21. Five MS dissociation pathways were identified that resulted from fragmentation of the carbon skeleton of azaspiracids producing nitrogen‐containing ions. Two pathways, involving cleavage of the E‐ring and C27–C28, gave ions that were found in all azaspiracids. Three pathways, A‐ring, C‐ring and C19–C20 cleavages, were useful for distinguishing between azaspiracid analogues. The same product ions from backbone fragmentation were also observed using hybrid quadrupole time‐of‐flight mass spectrometry (QqTOFMS). The fragmentation of the A‐ring was the most facile and was exploited in the development of LC/MS^n^ methods for the analysis of azaspiracids. Copyright © 2003 John Wiley & Sons, Ltd.
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