Characterization of polar brevetoxin derivatives isolated from Karenia brevis cultures and natural blooms. |
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Authors: | Ann Abraham Steven M Plakas Zhihong Wang Edward L E Jester Kathleen R El Said Hudson R Granade Michael S Henry Patricia C Blum Richard H Pierce Robert W Dickey |
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Affiliation: | Gulf Coast Seafood Laboratory, US Food and Drug Administration, P.O. Box 158, 1 Iberville Drive, Dauphin Island, AL 36528-0158, USA. ann.abraham@fda.hhs.gov |
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Abstract: | Several novel brevetoxin derivatives were isolated and identified in Karenia brevis cultures and natural blooms by using solid phase extraction (SPE) and LC/MS(MS) techniques. These analogs were more polar compared with previously described brevetoxins, and were poorly extractable by conventional non-polar solvent (chloroform) partitioning. Brevetoxin analogs were structurally confirmed as hydrolyzed (open A-ring) forms of brevetoxins PbTx-1, PbTx-7, PbTx-2, and PbTx-3, and of oxidized PbTx-1 and PbTx-2. Some of these open A-ring derivatives were in greater abundance than their non-hydrolyzed counterparts. All were in much greater abundance in bloom water filtrate compared with cell-rich fractions. Open A-ring compounds were cytotoxic in mouse neuroblastoma (N2a) cell assay. In the K. brevis bloom-exposed Eastern oyster, brevetoxin metabolites with opened A rings were identified (e.g., open-ring cysteine-PbTx conjugates), contributing to their overall toxin burden. |
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Keywords: | Brevetoxins Karenia brevis Eastern oyster LC/MS |
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