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Isolation of Echimidine and Its C-7 Isomers from Echium plantagineum L. and Their Hepatotoxic Effect on Rat Hepatocytes

Echimidine is the main pyrrolizidine alkaloid of Echium plantagineum L., a plant domesticated in many countries. Because of echimidine’s toxicity, this alkaloid has become a target of the European Food Safety Authority regulations, especially in regard to honey contamination. In this study, we deter...

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Autores principales: Gleńsk, Michał, Dudek, Marta K., Kinkade, Peter, Santos, Evelyn C. S., Glinski, Vitold B., Ferreira, Daneel, Seweryn, Ewa, Kaźmierski, Sławomir, Calixto, Joao B., Glinski, Jan A.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9102911/
https://www.ncbi.nlm.nih.gov/pubmed/35566223
http://dx.doi.org/10.3390/molecules27092869
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author Gleńsk, Michał
Dudek, Marta K.
Kinkade, Peter
Santos, Evelyn C. S.
Glinski, Vitold B.
Ferreira, Daneel
Seweryn, Ewa
Kaźmierski, Sławomir
Calixto, Joao B.
Glinski, Jan A.
author_facet Gleńsk, Michał
Dudek, Marta K.
Kinkade, Peter
Santos, Evelyn C. S.
Glinski, Vitold B.
Ferreira, Daneel
Seweryn, Ewa
Kaźmierski, Sławomir
Calixto, Joao B.
Glinski, Jan A.
author_sort Gleńsk, Michał
collection PubMed
description Echimidine is the main pyrrolizidine alkaloid of Echium plantagineum L., a plant domesticated in many countries. Because of echimidine’s toxicity, this alkaloid has become a target of the European Food Safety Authority regulations, especially in regard to honey contamination. In this study, we determined by NMR spectroscopy that the main HPLC peak purified from zinc reduced plant extract with an MS [M + H](+) signal at m/z 398 corresponding to echimidine (1), and in fact also represents an isomeric echihumiline (2). A third isomer present in the smallest amount and barely resolved by HPLC from co-eluting (1) and (2) was identified as hydroxymyoscorpine (3). Before the zinc reduction, alkaloids (1) and (2) were present mostly (90%) in the form of an N-oxide, which formed a single peak in HPLC. This is the first report of finding echihumiline and hydroxymyoscorpine in E. plantagineum. Retroanalysis of our samples of E. plantagineum collected in New Zealand, Argentina and the USA confirmed similar co-occurrence of the three isomeric alkaloids. In rat hepatocyte primary culture cells, the alkaloids at 3 to 300 µg/mL caused concentration-dependent inhibition of hepatocyte viability with mean IC(50) values ranging from 9.26 to 14.14 µg/mL. Our discovery revealed that under standard HPLC acidic conditions, echimidine co-elutes with its isomers, echihumiline and to a lesser degree with hydroxymyoscorpine, obscuring real alkaloidal composition, which may have implications for human toxicity.
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spelling pubmed-91029112022-05-14 Isolation of Echimidine and Its C-7 Isomers from Echium plantagineum L. and Their Hepatotoxic Effect on Rat Hepatocytes Gleńsk, Michał Dudek, Marta K. Kinkade, Peter Santos, Evelyn C. S. Glinski, Vitold B. Ferreira, Daneel Seweryn, Ewa Kaźmierski, Sławomir Calixto, Joao B. Glinski, Jan A. Molecules Article Echimidine is the main pyrrolizidine alkaloid of Echium plantagineum L., a plant domesticated in many countries. Because of echimidine’s toxicity, this alkaloid has become a target of the European Food Safety Authority regulations, especially in regard to honey contamination. In this study, we determined by NMR spectroscopy that the main HPLC peak purified from zinc reduced plant extract with an MS [M + H](+) signal at m/z 398 corresponding to echimidine (1), and in fact also represents an isomeric echihumiline (2). A third isomer present in the smallest amount and barely resolved by HPLC from co-eluting (1) and (2) was identified as hydroxymyoscorpine (3). Before the zinc reduction, alkaloids (1) and (2) were present mostly (90%) in the form of an N-oxide, which formed a single peak in HPLC. This is the first report of finding echihumiline and hydroxymyoscorpine in E. plantagineum. Retroanalysis of our samples of E. plantagineum collected in New Zealand, Argentina and the USA confirmed similar co-occurrence of the three isomeric alkaloids. In rat hepatocyte primary culture cells, the alkaloids at 3 to 300 µg/mL caused concentration-dependent inhibition of hepatocyte viability with mean IC(50) values ranging from 9.26 to 14.14 µg/mL. Our discovery revealed that under standard HPLC acidic conditions, echimidine co-elutes with its isomers, echihumiline and to a lesser degree with hydroxymyoscorpine, obscuring real alkaloidal composition, which may have implications for human toxicity. MDPI 2022-04-30 /pmc/articles/PMC9102911/ /pubmed/35566223 http://dx.doi.org/10.3390/molecules27092869 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Gleńsk, Michał
Dudek, Marta K.
Kinkade, Peter
Santos, Evelyn C. S.
Glinski, Vitold B.
Ferreira, Daneel
Seweryn, Ewa
Kaźmierski, Sławomir
Calixto, Joao B.
Glinski, Jan A.
Isolation of Echimidine and Its C-7 Isomers from Echium plantagineum L. and Their Hepatotoxic Effect on Rat Hepatocytes
title Isolation of Echimidine and Its C-7 Isomers from Echium plantagineum L. and Their Hepatotoxic Effect on Rat Hepatocytes
title_full Isolation of Echimidine and Its C-7 Isomers from Echium plantagineum L. and Their Hepatotoxic Effect on Rat Hepatocytes
title_fullStr Isolation of Echimidine and Its C-7 Isomers from Echium plantagineum L. and Their Hepatotoxic Effect on Rat Hepatocytes
title_full_unstemmed Isolation of Echimidine and Its C-7 Isomers from Echium plantagineum L. and Their Hepatotoxic Effect on Rat Hepatocytes
title_short Isolation of Echimidine and Its C-7 Isomers from Echium plantagineum L. and Their Hepatotoxic Effect on Rat Hepatocytes
title_sort isolation of echimidine and its c-7 isomers from echium plantagineum l. and their hepatotoxic effect on rat hepatocytes
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9102911/
https://www.ncbi.nlm.nih.gov/pubmed/35566223
http://dx.doi.org/10.3390/molecules27092869
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