Targeted acetylcholinesterase-responsive drug carriers with long duration of drug action and reduced hepatotoxicity

Targeted acetylcholinesterase-responsive drug carriers with long duration of drug action and reduced hepatotoxicity

Yulong Lin, Yalin Wang, Jie Lv, Nannan Wang, Jing Wang, Meng LiCollege of Pharmaceutical Sciences, Hebei Medical University, Shijiazhuang 050017, People’s Republic of ChinaPurpose: Acetylcholinesterase (AChE) plays a critical role in the transmission of nerve impulse at the cholinergic syn...

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Main Authors: Lin Y, Wang Y, Lv J, Wang N, Wang J, Li M
Format: Article
Language:English
Published: Dove Medical Press 2019-07-01
Series:International Journal of Nanomedicine
Subjects:
Acetylcholinesterase inhibitor
controlled drug release
mesoporous silica nanoparticles
drug action
hepatotoxicity
Online Access:https://www.dovepress.com/targeted-acetylcholinesterase-responsive-drug-carriers-with-long-durat-peer-reviewed-article-IJN
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spelling doaj-0d686f4cae024fb98b70cdede6a6f4d02020-11-24T22:11:26ZengDove Medical PressInternational Journal of Nanomedicine1178-20132019-07-01Volume 145817582947446Targeted acetylcholinesterase-responsive drug carriers with long duration of drug action and reduced hepatotoxicityLin YWang YLv JWang NWang JLi MYulong Lin, Yalin Wang, Jie Lv, Nannan Wang, Jing Wang, Meng LiCollege of Pharmaceutical Sciences, Hebei Medical University, Shijiazhuang 050017, People’s Republic of ChinaPurpose: Acetylcholinesterase (AChE) plays a critical role in the transmission of nerve impulse at the cholinergic synapses. Design and synthesis of AChE inhibitors that increase the cholinergic transmission by blocking the degradation of acetylcholine can serve as a strategy for the treatment of AChE-associated disease. Herein, an operational targeted drug delivery platform based on AChE-responsive system has been presented by combining the unique properties of enzyme-controlled mesoporous silica nanoparticles (MSN) with clinical-used AChE inhibitor.Methods: Functionalized MSNs were synthesized by liquid phase method and characterized by using different analytical methods. The biocompatibility and cytotoxicity of MSNs were determined by hemolysis experiment and MTT assay, respectively. Comparison of AChE activity between drug-loading system and inhibitor was developed with kits and by ELISA method. The efficacy of drug-loaded nanocarriers was investigated in a mouse model.Results: Compared with AChE inhibitor itself, the inhibition efficiency of this drug delivery system was strongly dependent on the concentration of AChE. Only AChE with high concentration could cause the opening of pores in the MSN, leading to the controlled release of AChE inhibitor in disease condition. Critically, the drug delivery system can not only exhibit long duration of drug action on AChE inhibition but also reduce the hepatotoxicity in vivo.Conclusion: In summary, AChE-responsive drug release systems have been far less explored. Our results would shed lights on the design of enzyme controlled-release multifunctional system for enzyme-associated disease treatment.Keywords: acetylcholinesterase inhibitor, controlled drug release, mesoporous silica nanoparticles, drug action, hepatotoxicityhttps://www.dovepress.com/targeted-acetylcholinesterase-responsive-drug-carriers-with-long-durat-peer-reviewed-article-IJNAcetylcholinesterase inhibitorcontrolled drug releasemesoporous silica nanoparticlesdrug actionhepatotoxicity
collection DOAJ
language English
format Article
sources DOAJ
author Lin Y
Wang Y
Lv J
Wang N
Wang J
Li M
spellingShingle Lin Y
Wang Y
Lv J
Wang N
Wang J
Li M
Targeted acetylcholinesterase-responsive drug carriers with long duration of drug action and reduced hepatotoxicity
International Journal of Nanomedicine
Acetylcholinesterase inhibitor
controlled drug release
mesoporous silica nanoparticles
drug action
hepatotoxicity
author_facet Lin Y
Wang Y
Lv J
Wang N
Wang J
Li M
author_sort Lin Y
title Targeted acetylcholinesterase-responsive drug carriers with long duration of drug action and reduced hepatotoxicity
title_short Targeted acetylcholinesterase-responsive drug carriers with long duration of drug action and reduced hepatotoxicity
title_full Targeted acetylcholinesterase-responsive drug carriers with long duration of drug action and reduced hepatotoxicity
title_fullStr Targeted acetylcholinesterase-responsive drug carriers with long duration of drug action and reduced hepatotoxicity
title_full_unstemmed Targeted acetylcholinesterase-responsive drug carriers with long duration of drug action and reduced hepatotoxicity
title_sort targeted acetylcholinesterase-responsive drug carriers with long duration of drug action and reduced hepatotoxicity
publisher Dove Medical Press
series International Journal of Nanomedicine
issn 1178-2013
publishDate 2019-07-01
description Yulong Lin, Yalin Wang, Jie Lv, Nannan Wang, Jing Wang, Meng LiCollege of Pharmaceutical Sciences, Hebei Medical University, Shijiazhuang 050017, People’s Republic of ChinaPurpose: Acetylcholinesterase (AChE) plays a critical role in the transmission of nerve impulse at the cholinergic synapses. Design and synthesis of AChE inhibitors that increase the cholinergic transmission by blocking the degradation of acetylcholine can serve as a strategy for the treatment of AChE-associated disease. Herein, an operational targeted drug delivery platform based on AChE-responsive system has been presented by combining the unique properties of enzyme-controlled mesoporous silica nanoparticles (MSN) with clinical-used AChE inhibitor.Methods: Functionalized MSNs were synthesized by liquid phase method and characterized by using different analytical methods. The biocompatibility and cytotoxicity of MSNs were determined by hemolysis experiment and MTT assay, respectively. Comparison of AChE activity between drug-loading system and inhibitor was developed with kits and by ELISA method. The efficacy of drug-loaded nanocarriers was investigated in a mouse model.Results: Compared with AChE inhibitor itself, the inhibition efficiency of this drug delivery system was strongly dependent on the concentration of AChE. Only AChE with high concentration could cause the opening of pores in the MSN, leading to the controlled release of AChE inhibitor in disease condition. Critically, the drug delivery system can not only exhibit long duration of drug action on AChE inhibition but also reduce the hepatotoxicity in vivo.Conclusion: In summary, AChE-responsive drug release systems have been far less explored. Our results would shed lights on the design of enzyme controlled-release multifunctional system for enzyme-associated disease treatment.Keywords: acetylcholinesterase inhibitor, controlled drug release, mesoporous silica nanoparticles, drug action, hepatotoxicity
topic Acetylcholinesterase inhibitor
controlled drug release
mesoporous silica nanoparticles
drug action
hepatotoxicity
url https://www.dovepress.com/targeted-acetylcholinesterase-responsive-drug-carriers-with-long-durat-peer-reviewed-article-IJN
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