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A New Zearalenone Biodegradation Strategy Using Non-Pathogenic Rhodococcus pyridinivorans K408 Strain

Zearalenone (hereafter referred to as ZEA) is a nonsteroidal estrogenic mycotoxin produced by several Fusarium spp. on cereal grains. ZEA is one of the most hazardous natural endocrine disrupting chemicals (EDC) which induces hyper estrogenic responses in mammals. This can result in reproductive dis...

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Autores principales: Kriszt, Rókus, Krifaton, Csilla, Szoboszlay, Sándor, Cserháti, Mátyás, Kriszt, Balázs, Kukolya, József, Czéh, Árpád, Fehér-Tóth, Szilvia, Török, Lívia, Szőke, Zsuzsanna, Kovács, Krisztina J., Barna, Teréz, Ferenczi, Szilamér
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3458049/
https://www.ncbi.nlm.nih.gov/pubmed/23049739
http://dx.doi.org/10.1371/journal.pone.0043608
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author Kriszt, Rókus
Krifaton, Csilla
Szoboszlay, Sándor
Cserháti, Mátyás
Kriszt, Balázs
Kukolya, József
Czéh, Árpád
Fehér-Tóth, Szilvia
Török, Lívia
Szőke, Zsuzsanna
Kovács, Krisztina J.
Barna, Teréz
Ferenczi, Szilamér
author_facet Kriszt, Rókus
Krifaton, Csilla
Szoboszlay, Sándor
Cserháti, Mátyás
Kriszt, Balázs
Kukolya, József
Czéh, Árpád
Fehér-Tóth, Szilvia
Török, Lívia
Szőke, Zsuzsanna
Kovács, Krisztina J.
Barna, Teréz
Ferenczi, Szilamér
author_sort Kriszt, Rókus
collection PubMed
description Zearalenone (hereafter referred to as ZEA) is a nonsteroidal estrogenic mycotoxin produced by several Fusarium spp. on cereal grains. ZEA is one of the most hazardous natural endocrine disrupting chemicals (EDC) which induces hyper estrogenic responses in mammals. This can result in reproductive disorders in farm animals as well as in humans. Consequently, detoxification strategies for contaminated crops are crucial for food safety. In this study we have developed a bacterial based detoxification system using a non-pathogen Rhodococcus pyridinivorans K408 strain. Following 5 days treatment of ZEA with R. pyridinivorans K408 strain HPLC analyses showed an 87.21% ZEA-degradation efficiency of the bacterial enzyme systems. In another approach, the strain biotransformation ability has also been confirmed by a bioluminescent version of the yeast estrogen screening system (BLYES), which detected an 81.75% of biodegradability of ZEA, in a good agreement with the chemical analyses. Furthermore, the capacity of R. pyridinivorans to eliminate the estrogenic effects of ZEA was tested by using an immature uterotrophic assay. Prepubertal female rats were treated with vehicle (olive oil), 17β-estradiol, ZEA (0.1-1-5-10 mg/kg body weight) and LB broth containing 500 mg/l ZEA that has already been incubated with or without Rhodococcus pyridinivorans K408 strain. Uterine weights were measured and the mRNA level changes relating to apelin, aquaporin 5, complement component 2, and calbindin-3 genes were measured by qRT-PCR. These genes represent the major pathways that are affected by estromimetic compounds. Zearalenone feeding significantly increased the uterus weight in a dose dependent manner and at the same time upregulated complement component 2 and calbindin-3 expression as well as decreased apelin and aquaporin 5 mRNA levels comparable to that seen in 17β-estradiol exposed rats. In contrast, LB broth in which ZEA was incubated with Rhodococcus pyridinivorans K408 prior to the feeding did not display any estrogenic effect neither on uterine weight nor on the expression of estrogen-regulated genes. Consequently, the identification of Rhodococcus pyridinivorans K408 strain in ZEA biodegradation proved to be a very efficient biological tool that is able to eliminate the complete estrogenic effects of ZEA. It is also remarkable that this biotransformation pathway of ZEA did not result in any residual estrogenic effects.
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spelling pubmed-34580492012-10-03 A New Zearalenone Biodegradation Strategy Using Non-Pathogenic Rhodococcus pyridinivorans K408 Strain Kriszt, Rókus Krifaton, Csilla Szoboszlay, Sándor Cserháti, Mátyás Kriszt, Balázs Kukolya, József Czéh, Árpád Fehér-Tóth, Szilvia Török, Lívia Szőke, Zsuzsanna Kovács, Krisztina J. Barna, Teréz Ferenczi, Szilamér PLoS One Research Article Zearalenone (hereafter referred to as ZEA) is a nonsteroidal estrogenic mycotoxin produced by several Fusarium spp. on cereal grains. ZEA is one of the most hazardous natural endocrine disrupting chemicals (EDC) which induces hyper estrogenic responses in mammals. This can result in reproductive disorders in farm animals as well as in humans. Consequently, detoxification strategies for contaminated crops are crucial for food safety. In this study we have developed a bacterial based detoxification system using a non-pathogen Rhodococcus pyridinivorans K408 strain. Following 5 days treatment of ZEA with R. pyridinivorans K408 strain HPLC analyses showed an 87.21% ZEA-degradation efficiency of the bacterial enzyme systems. In another approach, the strain biotransformation ability has also been confirmed by a bioluminescent version of the yeast estrogen screening system (BLYES), which detected an 81.75% of biodegradability of ZEA, in a good agreement with the chemical analyses. Furthermore, the capacity of R. pyridinivorans to eliminate the estrogenic effects of ZEA was tested by using an immature uterotrophic assay. Prepubertal female rats were treated with vehicle (olive oil), 17β-estradiol, ZEA (0.1-1-5-10 mg/kg body weight) and LB broth containing 500 mg/l ZEA that has already been incubated with or without Rhodococcus pyridinivorans K408 strain. Uterine weights were measured and the mRNA level changes relating to apelin, aquaporin 5, complement component 2, and calbindin-3 genes were measured by qRT-PCR. These genes represent the major pathways that are affected by estromimetic compounds. Zearalenone feeding significantly increased the uterus weight in a dose dependent manner and at the same time upregulated complement component 2 and calbindin-3 expression as well as decreased apelin and aquaporin 5 mRNA levels comparable to that seen in 17β-estradiol exposed rats. In contrast, LB broth in which ZEA was incubated with Rhodococcus pyridinivorans K408 prior to the feeding did not display any estrogenic effect neither on uterine weight nor on the expression of estrogen-regulated genes. Consequently, the identification of Rhodococcus pyridinivorans K408 strain in ZEA biodegradation proved to be a very efficient biological tool that is able to eliminate the complete estrogenic effects of ZEA. It is also remarkable that this biotransformation pathway of ZEA did not result in any residual estrogenic effects. Public Library of Science 2012-09-25 /pmc/articles/PMC3458049/ /pubmed/23049739 http://dx.doi.org/10.1371/journal.pone.0043608 Text en © 2012 Kriszt et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Kriszt, Rókus
Krifaton, Csilla
Szoboszlay, Sándor
Cserháti, Mátyás
Kriszt, Balázs
Kukolya, József
Czéh, Árpád
Fehér-Tóth, Szilvia
Török, Lívia
Szőke, Zsuzsanna
Kovács, Krisztina J.
Barna, Teréz
Ferenczi, Szilamér
A New Zearalenone Biodegradation Strategy Using Non-Pathogenic Rhodococcus pyridinivorans K408 Strain
title A New Zearalenone Biodegradation Strategy Using Non-Pathogenic Rhodococcus pyridinivorans K408 Strain
title_full A New Zearalenone Biodegradation Strategy Using Non-Pathogenic Rhodococcus pyridinivorans K408 Strain
title_fullStr A New Zearalenone Biodegradation Strategy Using Non-Pathogenic Rhodococcus pyridinivorans K408 Strain
title_full_unstemmed A New Zearalenone Biodegradation Strategy Using Non-Pathogenic Rhodococcus pyridinivorans K408 Strain
title_short A New Zearalenone Biodegradation Strategy Using Non-Pathogenic Rhodococcus pyridinivorans K408 Strain
title_sort new zearalenone biodegradation strategy using non-pathogenic rhodococcus pyridinivorans k408 strain
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3458049/
https://www.ncbi.nlm.nih.gov/pubmed/23049739
http://dx.doi.org/10.1371/journal.pone.0043608
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