Your search keyword '"Ciguatera Poisoning metabolism"' showing total 12 results

1. Determination of the toxicity equivalency factors for ciguatoxins using human sodium channels.

Author

Raposo-Garcia S, Louzao MC, Fuwa H, Sasaki M, Vale C, and Botana LM

Subjects

Cell Line, Ciguatera Poisoning etiology, Ciguatera Poisoning genetics, Ciguatoxins chemistry, Humans, Kinetics, Voltage-Gated Sodium Channels chemistry, Voltage-Gated Sodium Channels genetics, Ciguatera Poisoning metabolism, Ciguatoxins toxicity, Toxicity Tests methods, Voltage-Gated Sodium Channels metabolism

Abstract

Ciguatoxins (CTXs) which are produced by dinoflagellates of the genus Gambierdiscus and Fukuyoa and share a ladder-shaped polyether structure, are causative compounds of one of the most frequent foodborne illness disease known as ciguatera fish poisoning (CFP). CFP was initially found in tropical and subtropical areas but nowadays the dinoflagellates producers of ciguatoxins had spread to European coasts. Therefore, this raises the need of establishing toxicity equivalency factors for the different compounds that can contribute to ciguatera fish poisoning, since biological methods have been replaced by analytical techniques. Thus, in this work, the effects of six compounds causative of ciguatera, on their main target, the human voltage-gated sodium channels have been analyzed for the first time. The results presented here led to the conclusion that the order of potency was CTX1B, CTX3B, CTX4A, gambierol, gambierone and MTX3. Furthermore, the data indicate that the activation voltage of sodium channels is more sensitive to detect ciguatoxins than their effect on the peak sodium current amplitude., (Copyright © 2022 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2022

2. In Vitro Glucuronidation of Caribbean Ciguatoxins in Fish: First Report of Conjugative Ciguatoxin Metabolites.

Author

Gwinn JK, Uhlig S, Ivanova L, Fæste CK, Kryuchkov F, and Robertson A

Subjects

Animals, Biotransformation, Caribbean Region, Ciguatera Poisoning etiology, Ciguatera Poisoning metabolism, Food Chain, Humans, Microsomes, Liver metabolism, Rats, Wistar, Seafood poisoning, Rats, Ciguatoxins metabolism, Fishes metabolism, Glucuronides metabolism

Abstract

Ciguatoxins (CTX) are potent marine neurotoxins, which can bioaccumulate in seafood, causing a severe and prevalent human illness known as ciguatera poisoning (CP). Despite the worldwide impact of ciguatera, effective disease management is hindered by a lack of knowledge regarding the movement and biotransformation of CTX congeners in marine food webs, particularly in the Caribbean and Western Atlantic. In this study we investigated the hepatic biotransformation of C-CTX across several fish and mammalian species through a series of in vitro metabolism assays focused on phase I (CYP P450; functionalization) and phase II (UGT; conjugation) reactions. Using liquid chromatography high-resolution mass spectrometry to explore potential C-CTX metabolites, we observed two glucuronide products of C-CTX-1/-2 and provided additional evidence from high-resolution tandem mass spectrometry to support their identification. Chemical reduction experiments confirmed that the metabolites were comprised of four distinct glucuronide products with the sugar attached at two separate sites on C-CTX-1/-2 and excluded the C-56 hydroxyl group as the conjugation site. Glucuronidation is a novel biotransformation pathway not yet reported for CTX or other related polyether phycotoxins, yet its occurrence across all fish species tested suggests that it could be a prevalent and important detoxification mechanism in marine organisms. The absence of glucuronidation observed in this study for both rat and human microsomes suggests that alternate biotransformation pathways may be dominant in higher vertebrates.

Published

2021

3. Acute Exposure to Pacific Ciguatoxin Reduces Electroencephalogram Activity and Disrupts Neurotransmitter Metabolic Pathways in Motor Cortex.

Author

Kumar G, Au NPB, Lei ENY, Mak YL, Chan LLH, Lam MHW, Chan LL, Lam PKS, and Ma CHE

Subjects

Animals, Chromatography, High Pressure Liquid methods, Chromatography, Liquid methods, Ciguatera Poisoning metabolism, Fishes, Male, Mice, Inbred C57BL, Ciguatoxins toxicity, Electroencephalography drug effects, Metabolic Networks and Pathways drug effects, Motor Cortex drug effects, Neurotransmitter Agents metabolism

Abstract

Ciguatera fish poisoning (CFP) is a common human food poisoning caused by consumption of ciguatoxin (CTX)-contaminated fish affecting over 50,000 people worldwide each year. CTXs are classified depending on their origin from the Pacific (P-CTXs), Indian Ocean (I-CTXs), and Caribbean (C-CTXs). P-CTX-1 is the most toxic CTX known and the major source of CFP causing an array of neurological symptoms. Neurological symptoms in some CFP patients last for several months or years; however, the underlying electrophysiological properties of acute exposure to CTXs remain unknown. Here, we used CTX purified from ciguatera fish sourced in the Pacific Ocean (P-CTX-1). Delta and theta electroencephalography (EEG) activity was reduced remarkably in 2 h and returned to normal in 6 h after a single exposure. However, second exposure to P-CTX-1 induced not only a further reduction in EEG activities but also a 2-week delay in returning to baseline EEG values. Ciguatoxicity was detected in the brain hours after the first and second exposure by mouse neuroblastoma assay. The spontaneous firing rate of single motor cortex neuron was reduced significantly measured by single-unit recording with high spatial resolution. Expression profile study of neurotransmitters using targeted profiling approach based on liquid chromatography-tandem mass spectrometry revealed an imbalance between excitatory and inhibitory neurotransmitters in the motor cortex. Our study provides a possible link between the brain oscillations and neurotransmitter release after acute exposure to P-CTX-1. Identification of EEG signatures and major metabolic pathways affected by P-CTX-1 provides new insight into potential biomarker development and therapeutic interventions.

Published

2017

4. Ciguatoxins Evoke Potent CGRP Release by Activation of Voltage-Gated Sodium Channel Subtypes Na V 1.9, Na V 1.7 and Na V 1.1.

Author

Touska F, Sattler S, Malsch P, Lewis RJ, Reeh PW, and Zimmermann K

Subjects

Animals, Calcitonin Gene-Related Peptide drug effects, Calcium metabolism, Ciguatera Poisoning metabolism, Ciguatoxins chemistry, Enzyme-Linked Immunosorbent Assay, Humans, Hyperalgesia chemically induced, Lidocaine pharmacology, Male, Marine Toxins pharmacology, Membrane Potentials drug effects, Mice, Mice, Transgenic, Rats, Tetrodotoxin pharmacology, Ciguatoxins pharmacology, NAV1.1 Voltage-Gated Sodium Channel drug effects, NAV1.7 Voltage-Gated Sodium Channel drug effects, NAV1.9 Voltage-Gated Sodium Channel drug effects, Receptors, Calcitonin Gene-Related Peptide drug effects

Abstract

Ciguatoxins (CTXs) are marine toxins that cause ciguatera fish poisoning, a debilitating disease dominated by sensory and neurological disturbances that include cold allodynia and various painful symptoms as well as long-lasting pruritus. Although CTXs are known as the most potent mammalian sodium channel activator toxins, the etiology of many of its neurosensory symptoms remains unresolved. We recently described that local application of 1 nM Pacific Ciguatoxin-1 (P-CTX-1) into the skin of human subjects induces a long-lasting, painful axon reflex flare and that CTXs are particularly effective in releasing calcitonin-gene related peptide (CGRP) from nerve terminals. In this study, we used mouse and rat skin preparations and enzyme-linked immunosorbent assays (ELISA) to study the molecular mechanism by which P-CTX-1 induces CGRP release. We show that P-CTX-1 induces CGRP release more effectively in mouse as compared to rat skin, exhibiting EC 50 concentrations in the low nanomolar range. P-CTX-1-induced CGRP release from skin is dependent on extracellular calcium and sodium, but independent from the activation of various thermosensory transient receptor potential (TRP) ion channels. In contrast, lidocaine and tetrodotoxin (TTX) reduce CGRP release by 53-75%, with the remaining fraction involving L-type and T-type voltage-gated calcium channels (VGCC). Using transgenic mice, we revealed that the TTX-resistant voltage-gated sodium channel (VGSC) Na V 1.9, but not Na V 1.8 or Na V 1.7 alone and the combined activation of the TTX-sensitive VGSC subtypes Na V 1.7 and Na V 1.1 carry the largest part of the P-CTX-1-caused CGRP release of 42% and 34%, respectively. Given the contribution of CGRP to nociceptive and itch sensing pathways, our findings contribute to a better understanding of sensory symptoms of acute and chronic ciguatera that may help in the identification of potential therapeutics., Competing Interests: The authors declare no conflict of interest.

Published

2017

5. Ladder-Shaped Ion Channel Ligands: Current State of Knowledge.

Author

Shmukler YB and Nikishin DA

Subjects

Animals, Ciguatoxins metabolism, Dinoflagellida metabolism, Humans, Ligands, Ciguatera Poisoning metabolism, Marine Toxins metabolism, Oxocins metabolism, Potassium Channels, Voltage-Gated metabolism

Abstract

Ciguatoxins (CTX) and brevetoxins (BTX) are polycyclic ethereal compounds biosynthesized by the worldwide distributed planktonic and epibenthic dinoflagellates of Gambierdiscus and Karenia genera, correspondingly. Ciguatera, evoked by CTXs, is a type of ichthyosarcotoxism, which involves a variety of gastrointestinal and neurological symptoms, while BTXs cause so-called neurotoxic shellfish poisoning. Both types of toxins are reviewed together because of similar mechanisms of their action. These are the only molecules known to activate voltage-sensitive Na⁺-channels in mammals through a specific interaction with site 5 of its α-subunit and may compete for it, which results in an increase in neuronal excitability, neurotransmitter release and impairment of synaptic vesicle recycling. Most marine ciguatoxins potentiate Na v channels, but a considerable number of them, such as gambierol and maitotoxin, have been shown to affect another ion channel. Although the extrinsic function of these toxins is probably associated with the function of a feeding deterrent, it was suggested that their intrinsic function is coupled with the regulation of photosynthesis via light-harvesting complex II and thioredoxin. Antagonistic effects of BTXs and brevenal may provide evidence of their participation as positive and negative regulators of this mechanism., Competing Interests: The authors declare no conflict of interest.

Published

2017

6. Flow cytometric-membrane potential detection of sodium channel active marine toxins: application to ciguatoxins in fish muscle and feasibility of automating saxitoxin detection.

Author

Manger R, Woodle D, Berger A, Dickey RW, Jester E, Yasumoto T, Lewis R, Hawryluk T, and Hungerford J

Subjects

Animals, Automation, Cell Line, Tumor, Flatfishes, Food Analysis, Muscle, Skeletal metabolism, Neuroblastoma, Ciguatera Poisoning metabolism, Ciguatoxins chemistry, Flow Cytometry methods, Muscle, Skeletal chemistry, Saxitoxin chemistry, Sodium Channels chemistry

Abstract

Ciguatoxins are potent neurotoxins with a significant public health impact. Cytotoxicity assays have allowed the most sensitive means of detection of ciguatoxin-like activity without reliance on mouse bioassays and have been invaluable in studying outbreaks. An improvement of these cell-based assays is presented here in which rapid flow cytometric detection of ciguatoxins and saxitoxins is demonstrated using fluorescent voltage sensitive dyes. A depolarization response can be detected directly due to ciguatoxin alone; however, an approximate 1000-fold increase in sensitivity is observed in the presence of veratridine. These results demonstrate that flow cytometric assessment of ciguatoxins is possible at levels approaching the trace detection limits of our earlier cytotoxicity assays, however, with a significant reduction in analysis time. Preliminary results are also presented for detection of brevetoxins and for automation and throughput improvements to a previously described method for detecting saxitoxins in shellfish extracts.

Published

2014

7. Bioavailability and intravenous toxicokinetic parameters for Pacific ciguatoxin P-CTX-1 in rats.

Author

Ledreux A and Ramsdell JS

Subjects

Administration, Oral, Animals, Area Under Curve, Biological Availability, Cell Line, Tumor, Cell Survival drug effects, Ciguatera Poisoning chemically induced, Ciguatoxins administration & dosage, Half-Life, Injections, Intraperitoneal, Injections, Intravenous, Male, Mice, Neuroblastoma drug therapy, Neuroblastoma pathology, Rats, Rats, Sprague-Dawley, Sodium Channels drug effects, Ciguatera Poisoning metabolism, Ciguatoxins pharmacokinetics, Ciguatoxins toxicity

Abstract

Ciguatoxins are sodium channel activator toxins responsible for ciguatera fish poisoning. In this study, we determined the toxicokinetic parameters of the Pacific ciguatoxin P-CTX-1 in rats after an intravenous (iv) dose of 0.13 ng P-CTX-1 per g of body weight. The ciguatoxin activity was assessed over time in blood using the sensitive functional Neuro2a assay. The data were analyzed with a two-compartmental model. After exposure, the ciguatoxin activity exhibited a rapid (alpha half-life of 6 min) and extensive distribution into tissues (apparent steady state volume of distribution of 7.8 L). Ciguatoxin elimination from blood was slower with a beta half-life estimated at 35.5 h. The toxicokinetic parameters determined from this study were compared to data previously obtained after oral and intraperitoneal exposure of rats to 0.26 ng P-CTX-1 per g of body weight. Maximal bioavailability was determined by the area under the concentration curve, and was used to calculate the absolute P-CTX-1 bioavailabilities for oral and intraperitoneal routes of exposures of 39% and 75%, respectively., (Published by Elsevier Ltd.)

Published

2013

8. Toxicokinetics of the ciguatoxin P-CTX-1 in rats after intraperitoneal or oral administration.

Author

Bottein MY, Wang Z, and Ramsdell JS

Subjects

Administration, Oral, Animals, Ciguatera Poisoning chemically induced, Ciguatera Poisoning metabolism, Ciguatoxins administration & dosage, Eels, Injections, Intraperitoneal, Male, Pharmacokinetics, Rats, Rats, Sprague-Dawley, Tissue Distribution drug effects, Tissue Distribution physiology, Ciguatoxins pharmacokinetics, Ciguatoxins toxicity

Abstract

Ciguatoxins are voltage-gated selective algal toxins responsible for ciguatera fish poisoning. In this study we evaluate the toxicokinetics of one of the most common ciguatoxins found in the Pacific, the P-CTX-1, in rat after an oral or intraperitoneal (ip) dose of 0.26 μg/kg body weight. We report levels of ciguatoxin activity assessed over time in blood, urine and feces, and at 4 days in liver, muscle and brain, using the functional in vitro N2A cytotoxicity assay. Following exposure, the ciguatoxin activity exhibited a rapid systemic absorption that was followed by a bi-exponential decline, and data best fit a two-compartment model analysis. Maximum blood concentrations were reached at 1.97 and 0.43 h after the oral and ip dose, respectively. Ciguatoxin elimination from blood was slow with terminal half lives (t(½)β) estimated at 82 h for oral and 112 h for ip dosing. Ciguatoxin activity remained in liver, muscle and brain 96 h after ip and oral administration. While smaller amounts appeared in the urine, the main excretion route was feces, with peak rates reaching > 10 pg P-CTX-1 equivalents/h in both routes of administration. Assay guided fractionation showed the presence in the feces and liver of peaks of activity corresponding to the P-CTX-1 and to other less polar metabolites. In conclusion, biologically active ciguatoxins are detectable in blood, liver, muscle and brain, and continued to be excreted in urine and feces 4 days following exposure. Blood, as well as urine and feces may be useful matrices for low-invasive testing methods for ciguatera clinical cases., (Copyright © 2011 Elsevier Ireland Ltd. All rights reserved.)

Published

2011

9. Ability of certain plant extracts traditionally used to treat ciguatera fish poisoning to inhibit nitric oxide production in RAW 264.7 macrophages.

Author

Kumar-Roiné S, Matsui M, Reybier K, Darius HT, Chinain M, Pauillac S, and Laurent D

Subjects

Animals, Cell Line, Humans, Lipopolysaccharides, Macrophages metabolism, Medicine, Traditional, Mice, Nitric Oxide biosynthesis, Plant Extracts therapeutic use, Plants, Medicinal, Ciguatera Poisoning drug therapy, Ciguatera Poisoning metabolism, Ciguatoxins metabolism, Macrophages drug effects, Magnoliopsida, Nitric Oxide antagonists & inhibitors, Plant Extracts pharmacology

Abstract

Aim of the Study: Ciguatera fish poisoning (CFP) is an intertropical ichthyosarcotoxism that manifests in complex assortment of symptoms in humans. Ciguatoxins (CTXs), issued from Gambierdicus spp., are causative agents of this intoxication. We have recently demonstrated that a Pacific CTX (P-CTX-1B) strongly modulated iNOS expression, leading to overproduction of nitric oxide (NO) in RAW 264.7 murine macrophage cells. NO produced in large amounts is involved in a wide range of pathophysiological processes. Many traditional remedies are commonly used in the Pacific against CFP. In this context, bioassay-guided screening was carried out to study NO inhibiting capacity of 28 selected plant extracts., Materials and Methods: We prepared aqueous extracts of plants used in New Caledonia in the treatment of CFP and screened their NO inhibitory activity in lipopolysaccharide (LPS)-activated RAW 264.7 macrophages., Results: Among 28 plants tested, Euphorbia hirta (Euphorbiaceae), Syzygium malaccense (Myrtaceae), Schinus terebenthifolius (Anacardiaceae), Punica granatum (Punicaceae), Cerbera manghas (Apocynaceae), Vitex trifolia (Labiateae) and Ximenia americana (Olacaceae) showed inhibitory activity, validating their use as traditional remedies in CFP, and the potential for use in the treatment of conditions accompanied by NO overproduction., Conclusion: These plants are promising candidates for further screening of their active compounds through activity-guided fractionation.

Published

2009

10. Synthetic ciguatoxins selectively activate Nav1.8-derived chimeric sodium channels expressed in HEK293 cells.

Author

Yamaoka K, Inoue M, Miyazaki K, Hirama M, Kondo C, Kinoshita E, Miyoshi H, and Seyama I

Subjects

Animals, Base Sequence, Cell Line, Ciguatera Poisoning genetics, Gene Expression, Humans, Molecular Sequence Data, Muscle Proteins genetics, NAV1.4 Voltage-Gated Sodium Channel, NAV1.8 Voltage-Gated Sodium Channel, Nerve Tissue Proteins genetics, Peptide Mapping, Protein Structure, Tertiary genetics, Rats, Recombinant Fusion Proteins genetics, Recombinant Fusion Proteins metabolism, Sodium Channels genetics, Ciguatera Poisoning metabolism, Ciguatoxins pharmacology, Muscle Proteins metabolism, Nerve Tissue Proteins metabolism, Sodium Channels metabolism

Abstract

The synthetic ciguatoxin CTX3C has been shown to activate tetrodotoxin (TTX)-sensitive sodium channels (Na(v)1.2, Na(v)1.4, and Na(v)1.5) by accelerating activation kinetics and shifting the activation curve toward hyperpolarization (Yamaoka, K., Inoue, M., Miyahara, H., Miyazaki, K., and Hirama, M. (2004) Br. J. Pharmacol. 142, 879-889). In this study, we further explored the effects of CTX3C on the TTX-resistant sodium channel Na(v)1.8. TTX-resistant channels have been shown to be involved in transducing pain and related sensations (Akopian, A. N., Sivilotti, L., and Wood, J. N. (1996) Nature 379, 257-262). Thus, we hypothesized that ciguatoxin-induced activation of the Na(v)1.8 current would account for the neurological symptoms of ciguatera poisoning. We found that 0.1 mum CTX3C preferentially affected the activation process of the Na(v)1.8 channel compared with those of the Na(v)1.2 and Na(v)1.4 channels. Importantly, without stimulation, 0.1 mum CTX3C induced a large leakage current (I (L)). The conductance of the I (L) calculated relative to the maximum conductance (G (max)) was 10 times larger than that of Na(v)1.2 or Na(v)1.4. To determine the molecular domain of Na(v)1.8 responsible for conferring higher sensitivity to CTX3C, we made two chimeric constructs from Na(v)1.4 and Na(v)1.8. Chimeras containing the N-terminal half of Na(v)1.8 exhibited a large response similar to wild-type Na(v)1.8, indicating that the region conferring high sensitivity to ciguatoxin action is located in the D1 or D2 domains.

Published

2009

11. Liver genomic responses to ciguatoxin: evidence for activation of phase I and phase II detoxification pathways following an acute hypothermic response in mice.

Author

Morey JS, Ryan JC, Bottein Dechraoui MY, Rezvani AH, Levin ED, Gordon CJ, Ramsdell JS, and Van Dolah FM

Subjects

Animals, Body Temperature drug effects, Body Temperature Regulation genetics, Ciguatera Poisoning metabolism, Cytochrome P-450 Enzyme System biosynthesis, Cytochrome P-450 Enzyme System genetics, Down-Regulation drug effects, Genomics, Glutathione Transferase biosynthesis, Glutathione Transferase genetics, Liver chemistry, Liver enzymology, Liver metabolism, Mice, Oligonucleotide Array Sequence Analysis, RNA, Messenger analysis, RNA, Messenger metabolism, Transcription, Genetic drug effects, Body Temperature Regulation drug effects, Ciguatera Poisoning genetics, Ciguatoxins toxicity, Liver drug effects, Metabolic Detoxication, Phase I genetics, Metabolic Detoxication, Phase II genetics, Poisons toxicity

Abstract

Ciguatoxins (CTX) are polyether neurotoxins that target voltage-gated sodium channels and are responsible for ciguatera, the most common fish-borne food poisoning in humans. This study characterizes the global transcriptional response of mouse liver to a symptomatic dose (0.26 ng/g) of the highly potent Pacific ciguatoxin-1 (P-CTX-1). At 1 h post-exposure 2.4% of features on a 44K whole genome array were differentially expressed (p < or = 0.0001), increasing to 5.2% at 4 h and decreasing to 1.4% by 24 h post-CTX exposure. Data were filtered (/fold change/ > or = 1.5 and p < or = 0.0001 in at least one time point) and a trend set of 1550 genes were used for further analysis. Early gene expression was likely influenced prominently by an acute 4 degrees C decline in core body temperature by 1 h, which resolved by 8 h following exposure. An initial downregulation of 32 different solute carriers, many involved in sodium transport, was observed. Differential gene expression in pathways involving eicosanoid biosynthesis and cholesterol homeostasis was also noted. Cytochrome P450s (Cyps) were of particular interest due to their role in xenobiotic metabolism. Twenty-seven genes, mostly members of Cyp2 and Cyp4 families, showed significant changes in expression. Many Cyps underwent an initial downregulation at 1 h but were quickly and strongly upregulated at 4 and 24 h post-exposure. In addition to Cyps, increases in several glutathione S-transferases were observed, an indication that both phase I and phase II metabolic reactions are involved in the hepatic response to CTX in mice.

Published

2008

12. Paralytic shellfish poisoning (PSP) in Margarita Island, Venezuela.

Author

La Barbera-Sánchez A, Franco Soler J, Rojas de Astudillo L, and Chang-Yen I

Subjects

Animals, Bivalvia metabolism, Chromatography, High Pressure Liquid, Ciguatera Poisoning metabolism, Dinoflagellida chemistry, Dinoflagellida classification, Disease Outbreaks, Environmental Monitoring, Epidemiological Monitoring, Humans, Rats, Saxitoxin analysis, Saxitoxin metabolism, Shellfish analysis, Time Factors, Venezuela epidemiology, Bivalvia chemistry, Ciguatera Poisoning epidemiology, Dinoflagellida growth & development, Eutrophication, Saxitoxin poisoning, Shellfish Poisoning

Abstract

A severe outbreak of Paralytic Shellfish Poisoning (PSP) occurred in Manzanillo and Guayacán, northwestern coast of Margarita Island, Venezuela, between August and October 1991. A bloom of dinoflagellates including Prorocentrum gracile, Gymnodinium catenatum and Alexandrium tamarense seemed to be responsible for this outbreak. Levels of PSP toxins in mussels (Perna perna) exceeded the international safety limit of saxitoxin, 80 microg STX/100 microg meat. PSP toxin values varied between 2548 and 115 microg STX/100 g meat in Manzanillo, and between 1422 and 86 microg STX/100 g meat in Guayacán. At both locations, the highest levels were detected in August, when 24 patients exhibited typical symptoms of PSP toxicity after consuming cooked mussels (16 required hospitalization). A high pressure liquid chromatographic (HPLC) procedure was recently used on the 1991 samples. The major toxin detected in samples of both locations was decarbamoyl saxitoxin (dcSTX), but low concentrations of saxitoxin were also found in Manzanillo samples. Gonyautoxins GTX1, GTX2 and GTX3 were detected only at Guayacán, while in both locations, decarbamoylgonyatouxin (dcGTX2,3) toxins were detected. These findings represent the first time that causative toxins of PSP in Venezuela have been chemically identified, and confirm the presence of dcSTX and dcGTX in mussels from the Caribbean Sea. The presence of dcSTX and dcGTX in shellfish is indicative that Gymnodinium catenatum was a causative organism for outbreak of PSP.

Published

2004