Astaxanthin and Docosahexaenoic Acid Reverse the Toxicity of the Maxi-K (BK) Channel Antagonist Mycotoxin Penitrem A

Astaxanthin and Docosahexaenoic Acid Reverse the Toxicity of the Maxi-K (BK) Channel Antagonist Mycotoxin Penitrem A

Penitrem A (PA) is a food mycotoxin produced by several terrestrial and few marine Penicillium species. PA is a potent tremorgen through selective antagonism of the calcium-dependent potassium BK (Maxi-K) channels. Discovery of natural products that can prevent the toxic effects of PA is important f...

Full description

Bibliographic Details
Main Authors: Amira A. Goda, Khayria M. Naguib, Magdy M. Mohamed, Hassan A. Amra, Somaia A. Nada, Abdel-Rahman B. Abdel-Ghaffar, Chris R. Gissendanner, Khalid A. El Sayed
Format: Article
Language:English
Published: MDPI AG 2016-11-01
Series:Marine Drugs
Subjects:
astaxanthin
BK (Maxi-K) channels
docosahexaenoic acid
food mycotoxin
penitrem A
toxicity
Online Access:http://www.mdpi.com/1660-3397/14/11/208
id doaj-2daea6e98c044fe993bf886cfa3d5b12
record_format Article
spelling doaj-2daea6e98c044fe993bf886cfa3d5b122020-11-24T20:52:10ZengMDPI AGMarine Drugs1660-33972016-11-01141120810.3390/md14110208md14110208Astaxanthin and Docosahexaenoic Acid Reverse the Toxicity of the Maxi-K (BK) Channel Antagonist Mycotoxin Penitrem AAmira A. Goda0Khayria M. Naguib1Magdy M. Mohamed2Hassan A. Amra3Somaia A. Nada4Abdel-Rahman B. Abdel-Ghaffar5Chris R. Gissendanner6Khalid A. El Sayed7Department of Basic Pharmaceutical Sciences, School of Pharmacy, University of Louisiana at Monroe, 1800 Bienville Drive, Monroe, LA 71201, USADepartment of Food Contaminant and Toxicology, National Research Center, Cairo 12622, EgyptBiochemistry Department, Faculty of Science, Ain Shams University, Cairo 11566, EgyptDepartment of Food Contaminant and Toxicology, National Research Center, Cairo 12622, EgyptDepartment of Food Contaminant and Toxicology, National Research Center, Cairo 12622, EgyptBiochemistry Department, Faculty of Science, Ain Shams University, Cairo 11566, EgyptDepartment of Basic Pharmaceutical Sciences, School of Pharmacy, University of Louisiana at Monroe, 1800 Bienville Drive, Monroe, LA 71201, USADepartment of Basic Pharmaceutical Sciences, School of Pharmacy, University of Louisiana at Monroe, 1800 Bienville Drive, Monroe, LA 71201, USAPenitrem A (PA) is a food mycotoxin produced by several terrestrial and few marine Penicillium species. PA is a potent tremorgen through selective antagonism of the calcium-dependent potassium BK (Maxi-K) channels. Discovery of natural products that can prevent the toxic effects of PA is important for food safety. Astaxanthin (AST) is a marine natural xanthophyll carotenoid with documented antioxidant activity. Unlike other common antioxidants, AST can cross blood brain barriers (BBBs), inducing neuroprotective effects. Docosahexaenoic acid (DHA) is polyunsaturated ω-3 fatty acid naturally occurring in fish and algae. DHA is essential for normal neurological and cellular development. This study evaluated the protective activity of AST and DHA against PA-induced toxicity, in vitro on Schwann cells CRL-2765 and in vivo in the worm Caenorhbitidis elegans and Sprague Dawley rat models. PA inhibited the viability of Schwann cells, with an IC50 of 22.6 μM. Dose-dependent treatments with 10–100 μM DHA significantly reversed the PA toxicity at its IC50 dose, and improved the survival of Schwann cells to 70.5%–98.8%. Similarly, dose-dependent treatments with 10–20 μM AST reversed the PA toxicity at its IC50 dose and raised these cells’ survival to 61.7%–70.5%. BK channel inhibition in the nematode C. elegans is associated with abnormal reversal locomotion. DHA and AST counteracted the in vivo PA BK channel antagonistic activity in the C. elegans model. Rats fed a PA-contaminated diet showed high levels of glutamate (GLU), aspartate (ASP), and gamma amino butyric acid (GABA), with observed necrosis or absence of Purkinjie neurons, typical of PA-induced neurotoxicity. Dopamine (DA), serotonin (5-HT), and norepinephrine (NE) levels were abnormal, Nitric Oxide (NO) and Malondialdehyde (MDA) levels were significantly increased, and total antioxidant capacity (TAC) level in serum and brain homogenates was significantly decreased in PA-treated rats. DHA and AST treatments effectively counteracted the toxic effects of PA and normalized most biochemical parameters in rats. DHA and AST can be useful food additives to prevent and reverse PA food-induced toxicity.http://www.mdpi.com/1660-3397/14/11/208astaxanthinBK (Maxi-K) channelsdocosahexaenoic acidfood mycotoxinpenitrem Atoxicity
collection DOAJ
language English
format Article
sources DOAJ
author Amira A. Goda
Khayria M. Naguib
Magdy M. Mohamed
Hassan A. Amra
Somaia A. Nada
Abdel-Rahman B. Abdel-Ghaffar
Chris R. Gissendanner
Khalid A. El Sayed
spellingShingle Amira A. Goda
Khayria M. Naguib
Magdy M. Mohamed
Hassan A. Amra
Somaia A. Nada
Abdel-Rahman B. Abdel-Ghaffar
Chris R. Gissendanner
Khalid A. El Sayed
Astaxanthin and Docosahexaenoic Acid Reverse the Toxicity of the Maxi-K (BK) Channel Antagonist Mycotoxin Penitrem A
Marine Drugs
astaxanthin
BK (Maxi-K) channels
docosahexaenoic acid
food mycotoxin
penitrem A
toxicity
author_facet Amira A. Goda
Khayria M. Naguib
Magdy M. Mohamed
Hassan A. Amra
Somaia A. Nada
Abdel-Rahman B. Abdel-Ghaffar
Chris R. Gissendanner
Khalid A. El Sayed
author_sort Amira A. Goda
title Astaxanthin and Docosahexaenoic Acid Reverse the Toxicity of the Maxi-K (BK) Channel Antagonist Mycotoxin Penitrem A
title_short Astaxanthin and Docosahexaenoic Acid Reverse the Toxicity of the Maxi-K (BK) Channel Antagonist Mycotoxin Penitrem A
title_full Astaxanthin and Docosahexaenoic Acid Reverse the Toxicity of the Maxi-K (BK) Channel Antagonist Mycotoxin Penitrem A
title_fullStr Astaxanthin and Docosahexaenoic Acid Reverse the Toxicity of the Maxi-K (BK) Channel Antagonist Mycotoxin Penitrem A
title_full_unstemmed Astaxanthin and Docosahexaenoic Acid Reverse the Toxicity of the Maxi-K (BK) Channel Antagonist Mycotoxin Penitrem A
title_sort astaxanthin and docosahexaenoic acid reverse the toxicity of the maxi-k (bk) channel antagonist mycotoxin penitrem a
publisher MDPI AG
series Marine Drugs
issn 1660-3397
publishDate 2016-11-01
description Penitrem A (PA) is a food mycotoxin produced by several terrestrial and few marine Penicillium species. PA is a potent tremorgen through selective antagonism of the calcium-dependent potassium BK (Maxi-K) channels. Discovery of natural products that can prevent the toxic effects of PA is important for food safety. Astaxanthin (AST) is a marine natural xanthophyll carotenoid with documented antioxidant activity. Unlike other common antioxidants, AST can cross blood brain barriers (BBBs), inducing neuroprotective effects. Docosahexaenoic acid (DHA) is polyunsaturated ω-3 fatty acid naturally occurring in fish and algae. DHA is essential for normal neurological and cellular development. This study evaluated the protective activity of AST and DHA against PA-induced toxicity, in vitro on Schwann cells CRL-2765 and in vivo in the worm Caenorhbitidis elegans and Sprague Dawley rat models. PA inhibited the viability of Schwann cells, with an IC50 of 22.6 μM. Dose-dependent treatments with 10–100 μM DHA significantly reversed the PA toxicity at its IC50 dose, and improved the survival of Schwann cells to 70.5%–98.8%. Similarly, dose-dependent treatments with 10–20 μM AST reversed the PA toxicity at its IC50 dose and raised these cells’ survival to 61.7%–70.5%. BK channel inhibition in the nematode C. elegans is associated with abnormal reversal locomotion. DHA and AST counteracted the in vivo PA BK channel antagonistic activity in the C. elegans model. Rats fed a PA-contaminated diet showed high levels of glutamate (GLU), aspartate (ASP), and gamma amino butyric acid (GABA), with observed necrosis or absence of Purkinjie neurons, typical of PA-induced neurotoxicity. Dopamine (DA), serotonin (5-HT), and norepinephrine (NE) levels were abnormal, Nitric Oxide (NO) and Malondialdehyde (MDA) levels were significantly increased, and total antioxidant capacity (TAC) level in serum and brain homogenates was significantly decreased in PA-treated rats. DHA and AST treatments effectively counteracted the toxic effects of PA and normalized most biochemical parameters in rats. DHA and AST can be useful food additives to prevent and reverse PA food-induced toxicity.
topic astaxanthin
BK (Maxi-K) channels
docosahexaenoic acid
food mycotoxin
penitrem A
toxicity
url http://www.mdpi.com/1660-3397/14/11/208
work_keys_str_mv AT amiraagoda astaxanthinanddocosahexaenoicacidreversethetoxicityofthemaxikbkchannelantagonistmycotoxinpenitrema
AT khayriamnaguib astaxanthinanddocosahexaenoicacidreversethetoxicityofthemaxikbkchannelantagonistmycotoxinpenitrema
AT magdymmohamed astaxanthinanddocosahexaenoicacidreversethetoxicityofthemaxikbkchannelantagonistmycotoxinpenitrema
AT hassanaamra astaxanthinanddocosahexaenoicacidreversethetoxicityofthemaxikbkchannelantagonistmycotoxinpenitrema
AT somaiaanada astaxanthinanddocosahexaenoicacidreversethetoxicityofthemaxikbkchannelantagonistmycotoxinpenitrema
AT abdelrahmanbabdelghaffar astaxanthinanddocosahexaenoicacidreversethetoxicityofthemaxikbkchannelantagonistmycotoxinpenitrema
AT chrisrgissendanner astaxanthinanddocosahexaenoicacidreversethetoxicityofthemaxikbkchannelantagonistmycotoxinpenitrema
AT khalidaelsayed astaxanthinanddocosahexaenoicacidreversethetoxicityofthemaxikbkchannelantagonistmycotoxinpenitrema
_version_ 1716800665563430912

Similar Items