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Authors = Sara F. Ferreiro

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Open AccessArticle Heart Alterations after Domoic Acid Administration in Rats
Toxins 2016, 8(3), 68; doi:10.3390/toxins8030068
Received: 13 January 2016 / Revised: 21 February 2016 / Accepted: 22 February 2016 / Published: 10 March 2016
Cited by 2 | Viewed by 966 | PDF Full-text (1993 KB) | HTML Full-text | XML Full-text
Abstract
Domoic acid (DA) is one of the best known marine toxins, causative of important neurotoxic alterations. DA effects are documented both in wildlife and experimental assays, showing that this toxin causes severe injuries principally in the hippocampal area. In the present study we
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Domoic acid (DA) is one of the best known marine toxins, causative of important neurotoxic alterations. DA effects are documented both in wildlife and experimental assays, showing that this toxin causes severe injuries principally in the hippocampal area. In the present study we have addressed the long-term toxicological effects (30 days) of DA intraperitoneal administration in rats. Different histological techniques were employed in order to study DA toxicity in heart, an organ which has not been thoroughly studied after DA intoxication to date. The presence of DA was detected by immunohistochemical assays, and cellular alterations were observed both by optical and transmission electron microscopy. Although histological staining methods did not provide any observable tissue damage, transmission electron microscopy showed several injuries: a moderate lysis of myofibrils and loss of mitochondrial conformation. This is the first time the association between heart damage and the presence of the toxin has been observed. Full article
(This article belongs to the collection Marine and Freshwater Toxins)
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Open AccessArticle Acute Cardiotoxicity Evaluation of the Marine Biotoxins OA, DTX-1 and YTX
Toxins 2015, 7(4), 1030-1047; doi:10.3390/toxins7041030
Received: 9 February 2015 / Revised: 17 March 2015 / Accepted: 18 March 2015 / Published: 27 March 2015
Cited by 9 | Viewed by 1421 | PDF Full-text (860 KB) | HTML Full-text | XML Full-text
Abstract
Phycotoxins are marine toxins produced by phytoplankton that can get accumulated in filter feeding shellfish. Human intoxication episodes occur due to contaminated seafood consumption. Okadaic acid (OA) and dynophysistoxins (DTXs) are phycotoxins responsible for a severe gastrointestinal syndrome called diarrheic shellfish poisoning (DSP).
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Phycotoxins are marine toxins produced by phytoplankton that can get accumulated in filter feeding shellfish. Human intoxication episodes occur due to contaminated seafood consumption. Okadaic acid (OA) and dynophysistoxins (DTXs) are phycotoxins responsible for a severe gastrointestinal syndrome called diarrheic shellfish poisoning (DSP). Yessotoxins (YTXs) are marine toxins initially included in the DSP class but currently classified as a separated group. Food safety authorities from several countries have regulated the content of DSPs and YTXs in shellfish to protect human health. In mice, OA and YTX have been associated with ultrastructural heart damage in vivo. Therefore, this study explored the potential of OA, DTX-1 and YTX to cause acute heart toxicity. Cardiotoxicity was evaluated in vitro by measuring hERG (human èter-a-go-go gene) channel activity and in vivo using electrocardiogram (ECG) recordings and cardiac damage biomarkers. The results demonstrated that these toxins do not exert acute effects on hERG channel activity. Additionally, in vivo experiments showed that these compounds do not alter cardiac biomarkers and ECG in rats acutely. Despite the ultrastructural damage to the heart reported for these toxins, no acute alterations of heart function have been detected in vivo, suggesting a functional compensation in the short term. Full article
(This article belongs to the collection Marine and Freshwater Toxins)

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