Marine Toxins as Pharmaceutical Treasure Troves: A Focus on Saxitoxin Derivatives from a Computational Point of View

This work highlights the significant potential of marine toxins, particularly saxitoxin (STX) and its derivatives, in the exploration of novel pharmaceuticals. These toxins, produced by aquatic microorganisms and collected by bivalve mollusks and other filter-feeding organisms, offer a vast reservoi...

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Published inMolecules (Basel, Switzerland) Vol. 29; no. 1; p. 275
Main Authors Flores-Holguín, Norma, Salas-Leiva, Joan S, Núñez-Vázquez, Erick J, Tovar-Ramírez, Dariel, Glossman-Mitnik, Daniel
Format Journal Article
LanguageEnglish
Published Switzerland MDPI AG 01.01.2024
MDPI
Subjects
Carbamates
chemical reactivity properties
chemical structures
Chemicals
computational chemistry
conceptual DFT
Density functionals
Drug development
Drug dosages
Marine toxins
Pharmaceuticals
Physiological aspects
Physiology
saxitoxins
Sodium
Software
Toxicity
Toxicology
Toxins
bioavailability scores
marine toxins
conceptual DFT
chemical reactivity properties
computational chemistry
saxitoxins
chemical structures
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Summary:This work highlights the significant potential of marine toxins, particularly saxitoxin (STX) and its derivatives, in the exploration of novel pharmaceuticals. These toxins, produced by aquatic microorganisms and collected by bivalve mollusks and other filter-feeding organisms, offer a vast reservoir of chemical and biological diversity. They interact with sodium channels in physiological processes, affecting various functions in organisms. Exposure to these toxins can lead to symptoms ranging from tingling sensations to respiratory failure and cardiovascular shock, with STX being one of the most potent. The structural diversity of STX derivatives, categorized into carbamate, N-sulfocarbamoyl, decarbamoyl, and deoxydecarbamoyl toxins, offers potential for drug development. The research described in this work aimed to computationally characterize 18 STX derivatives, exploring their reactivity properties within marine sponges using conceptual density functional theory (CDFT) techniques. Additionally, their pharmacokinetic properties, bioavailability, and drug-likeness scores were assessed. The outcomes of this research were the chemical reactivity parameters calculated via CDFT as well as the estimated pharmacokinetic and ADME properties derived using computational tools. While they may not align directly, the integration of these distinct datasets enriches our comprehensive understanding of the compound's properties and potential applications. Thus, this study holds promise for uncovering new pharmaceutical candidates from the considered marine toxins.
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ISSN:1420-3049
1420-3049
DOI:10.3390/molecules29010275