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Publikasjoner

Clarification of the C-35 stereochemistries of dinophysistoxin-1 and dinophysistoxin-2 and its consequences for binding to protein phosphatase

Vitenskapelig artikkel
Publiseringsår
2007
Tidsskrift
Chemical Research in Toxicology
Eksterne nettsted
Cristin
NIVA-involverte
Jan Thomas Rundberget
Forfattere
Kristofer Larsen, Dirk Petersen, Alistair Wilkins, Ingunn Samdal, Morten Sandvik, Thomas Rundberget, David Goldstone, Vickery Arcus, Peter Hovgaard, Frode Rise, Nils Rehmann, Philipp Hess, Christopher Miles

Sammendrag

Okadaic acid analogues are well known as protein phosphatase inhibitors and occur naturally in marine shellfish feeding on dinoflagellates of the genus Dinophysis, leading to diarrhetic shellfish poisoning of shellfish consumers. Knowledge of the correct structures for these toxins is important in understanding their toxicology, biochemistry, and biosynthesis. We have performed extensive NMR analyses on okadaic acid (1), dinophysistoxin-1 (DTX-1), and dinophysistoxin-2 (DTX-2) obtained from natural sources. Consequently, we were able to unambiguously deduce the stereochemistries at C-35 for DTX-1 and DTX-2 based on analysis of NMR coupling constants and NOE interactions. Our results revealed that DTX-2 (3) has a stereochemistry opposite to that of DTX-1 (2) at C-35. Molecular modeling of the docking of 1-3 with protein phosphatase-1 and protein phosphatase 2A (PP2A) suggested that the reduced affinity of DTX-2 for PP2A may be due to the newly defined stereochemistry at the 35-methyl group. The implications of these findings for biosynthesis and toxicology are discussed.