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Cytoprotection, Genoprotection, and Dermal Exposure Assessment of Chitosan-Based Agronanofungicides

Health risks which result from exposure to pesticides have sparked awareness among researchers, triggering the idea of developing nanoencapsulation pesticides with the aim to enhance cytoprotection as well as genoprotection of the pesticides. In addition, nanocapsules of pesticides have slow release...

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Autores principales: Maluin, Farhatun Najat, Hussein, Mohd Zobir, Yusof, Nor Azah, Idris, Abu Seman, Daim, Leona Daniela Jeffery, Sarian, Murni Nazira, Rajab, Nor Fadilah, Ee Ling, Siew, Rashid, Noramiwati, Fakurazi, Sharida
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7356519/
https://www.ncbi.nlm.nih.gov/pubmed/32486034
http://dx.doi.org/10.3390/pharmaceutics12060497
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author Maluin, Farhatun Najat
Hussein, Mohd Zobir
Yusof, Nor Azah
Idris, Abu Seman
Daim, Leona Daniela Jeffery
Sarian, Murni Nazira
Rajab, Nor Fadilah
Ee Ling, Siew
Rashid, Noramiwati
Fakurazi, Sharida
author_facet Maluin, Farhatun Najat
Hussein, Mohd Zobir
Yusof, Nor Azah
Idris, Abu Seman
Daim, Leona Daniela Jeffery
Sarian, Murni Nazira
Rajab, Nor Fadilah
Ee Ling, Siew
Rashid, Noramiwati
Fakurazi, Sharida
author_sort Maluin, Farhatun Najat
collection PubMed
description Health risks which result from exposure to pesticides have sparked awareness among researchers, triggering the idea of developing nanoencapsulation pesticides with the aim to enhance cytoprotection as well as genoprotection of the pesticides. In addition, nanocapsules of pesticides have slow release capability, high bioavailability, and site-specific delivery, which has attracted great interest from researchers. Hence, the objective of this work is to synthesize a nanoformulation of a fungicide of different sizes, namely, chitosan-hexaconazole nanoparticles (18 nm), chitosan-dazomet nanoparticles (7 nm), and chitosan-hexaconazole-dazomet nanoparticles (5 nm), which were then subjected to toxicological evaluations, including cytotoxicity, genotoxicity, cell death assay, and dermal irritation assays. Incubation of chitosan-based nanofungicides with V79-4 hamster lung cell did not reveal cytotoxicity or genotoxicity, potentially suggesting that encapsulation with chitosan reduces direct toxicity of the toxic fungicides. Meanwhile, pure fungicide revealed its high cytotoxic effect on V79-4 hamster lung cells. In addition, dermal exposure assessment on rabbits revealed that chitosan-hexaconazole nanoparticles are classified under corrosive subcategory 1C, while chitosan-dazomet nanoparticles are classified under corrosive subcategory 1B. Moreover, both chitosan-hexaconazole nanoparticles and chitosan-dazomet nanoparticles are classified as causing mild irritation.
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spelling pubmed-73565192020-07-30 Cytoprotection, Genoprotection, and Dermal Exposure Assessment of Chitosan-Based Agronanofungicides Maluin, Farhatun Najat Hussein, Mohd Zobir Yusof, Nor Azah Idris, Abu Seman Daim, Leona Daniela Jeffery Sarian, Murni Nazira Rajab, Nor Fadilah Ee Ling, Siew Rashid, Noramiwati Fakurazi, Sharida Pharmaceutics Article Health risks which result from exposure to pesticides have sparked awareness among researchers, triggering the idea of developing nanoencapsulation pesticides with the aim to enhance cytoprotection as well as genoprotection of the pesticides. In addition, nanocapsules of pesticides have slow release capability, high bioavailability, and site-specific delivery, which has attracted great interest from researchers. Hence, the objective of this work is to synthesize a nanoformulation of a fungicide of different sizes, namely, chitosan-hexaconazole nanoparticles (18 nm), chitosan-dazomet nanoparticles (7 nm), and chitosan-hexaconazole-dazomet nanoparticles (5 nm), which were then subjected to toxicological evaluations, including cytotoxicity, genotoxicity, cell death assay, and dermal irritation assays. Incubation of chitosan-based nanofungicides with V79-4 hamster lung cell did not reveal cytotoxicity or genotoxicity, potentially suggesting that encapsulation with chitosan reduces direct toxicity of the toxic fungicides. Meanwhile, pure fungicide revealed its high cytotoxic effect on V79-4 hamster lung cells. In addition, dermal exposure assessment on rabbits revealed that chitosan-hexaconazole nanoparticles are classified under corrosive subcategory 1C, while chitosan-dazomet nanoparticles are classified under corrosive subcategory 1B. Moreover, both chitosan-hexaconazole nanoparticles and chitosan-dazomet nanoparticles are classified as causing mild irritation. MDPI 2020-05-29 /pmc/articles/PMC7356519/ /pubmed/32486034 http://dx.doi.org/10.3390/pharmaceutics12060497 Text en © 2020 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Maluin, Farhatun Najat
Hussein, Mohd Zobir
Yusof, Nor Azah
Idris, Abu Seman
Daim, Leona Daniela Jeffery
Sarian, Murni Nazira
Rajab, Nor Fadilah
Ee Ling, Siew
Rashid, Noramiwati
Fakurazi, Sharida
Cytoprotection, Genoprotection, and Dermal Exposure Assessment of Chitosan-Based Agronanofungicides
title Cytoprotection, Genoprotection, and Dermal Exposure Assessment of Chitosan-Based Agronanofungicides
title_full Cytoprotection, Genoprotection, and Dermal Exposure Assessment of Chitosan-Based Agronanofungicides
title_fullStr Cytoprotection, Genoprotection, and Dermal Exposure Assessment of Chitosan-Based Agronanofungicides
title_full_unstemmed Cytoprotection, Genoprotection, and Dermal Exposure Assessment of Chitosan-Based Agronanofungicides
title_short Cytoprotection, Genoprotection, and Dermal Exposure Assessment of Chitosan-Based Agronanofungicides
title_sort cytoprotection, genoprotection, and dermal exposure assessment of chitosan-based agronanofungicides
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7356519/
https://www.ncbi.nlm.nih.gov/pubmed/32486034
http://dx.doi.org/10.3390/pharmaceutics12060497
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