Facile design of lidocaine-loaded polymeric hydrogel to persuade effects of local anesthesia drug delivery system: complete in vitro and in vivo toxicity analyses

Facile design of lidocaine-loaded polymeric hydrogel to persuade effects of local anesthesia drug delivery system: complete in vitro and in vivo toxicity analyses

The principal goal of the present investigation was to enterprise new and effective drug delivery vesicle for the sustained delivery of local anesthetic lidocaine hydrochloride (LDC), using a novel combination of copolymeric hydrogel with tetrahydroxyborate (COP–THB) to improve bioactivity and thera...

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Main Authors: Yan Li, Erxian Zhao, Li Li, Liying Bai, Wei Zhang
Format: Article
Language:English
Published: Taylor & Francis Group 2021-01-01
Series:Drug Delivery
Subjects:
hydrogel
ldc
in vitro release
l929 cells
in vivo evaluations
drug delivery
Online Access:http://dx.doi.org/10.1080/10717544.2021.1931558
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spelling doaj-c5dcc9d0d65546b1a0ea9a7c37e7a0a82021-06-21T12:25:18ZengTaylor & Francis GroupDrug Delivery1071-75441521-04642021-01-012811080109210.1080/10717544.2021.19315581931558Facile design of lidocaine-loaded polymeric hydrogel to persuade effects of local anesthesia drug delivery system: complete in vitro and in vivo toxicity analysesYan Li0Erxian Zhao1Li Li2Liying Bai3Wei Zhang4Department of Anesthesiology, The First Affiliated Hospital of Zhengzhou UniversityDepartment of Anesthesiology, The First Affiliated Hospital of Zhengzhou UniversityDepartment of Anesthesiology, The First Affiliated Hospital of Zhengzhou UniversityDepartment of Anesthesiology, The First Affiliated Hospital of Zhengzhou UniversityDepartment of Anesthesiology, The First Affiliated Hospital of Zhengzhou UniversityThe principal goal of the present investigation was to enterprise new and effective drug delivery vesicle for the sustained delivery of local anesthetic lidocaine hydrochloride (LDC), using a novel combination of copolymeric hydrogel with tetrahydroxyborate (COP–THB) to improve bioactivity and therapeutic potential. To support this contention, the physical and mechanical properties, rheological characteristics, and component release of candidate formulations were investigated. An optimized formulation of COP–THB containing LDC to an upper maximum concentration of 1.5% w/w was assessed for drug crystallization. The biocompatibility of the prepared COP–THB hydrogel was exhibited strong cell survival (96%) and growth compatibility on L929 fibroblast cell lines, which was confirmed by using methods of MTT assay and microscopic observations. The COP–THB hydrogel release pattern is distinct from that of COP–THB/LDC hydrogels by the slow-release rate and the low percentage of cumulative release. In vivo evaluations were demonstrated the anesthetic effects and toxicity value of treated samples by using mice models. In addition, COP–THB/LDC hydrogels significantly inhibit in vivo tumor growth in mice model and effectively reduced it is in vivo toxicity. The pharmacological evaluation showed that encapsulation of LDC in COP–THB hydrogels prolonged its anesthetic action with favorable in vitro and in vivo compatibility. This novel design may theoretically be used in promising studies involving the controlled release of local anesthetics.Highlights Development a modified sustained release system for the local anesthetic lidocaine. PVP-THB hydrogel to improve the pharmacological properties of the drug and their anesthetic activities. Profiles of PVP-THB/LDC showed that the effective release of associated lidocaine. This new formulation could potentially be used in future local anesthetics.http://dx.doi.org/10.1080/10717544.2021.1931558hydrogelldcin vitro releasel929 cellsin vivo evaluationsdrug delivery
collection DOAJ
language English
format Article
sources DOAJ
author Yan Li
Erxian Zhao
Li Li
Liying Bai
Wei Zhang
spellingShingle Yan Li
Erxian Zhao
Li Li
Liying Bai
Wei Zhang
Facile design of lidocaine-loaded polymeric hydrogel to persuade effects of local anesthesia drug delivery system: complete in vitro and in vivo toxicity analyses
Drug Delivery
hydrogel
ldc
in vitro release
l929 cells
in vivo evaluations
drug delivery
author_facet Yan Li
Erxian Zhao
Li Li
Liying Bai
Wei Zhang
author_sort Yan Li
title Facile design of lidocaine-loaded polymeric hydrogel to persuade effects of local anesthesia drug delivery system: complete in vitro and in vivo toxicity analyses
title_short Facile design of lidocaine-loaded polymeric hydrogel to persuade effects of local anesthesia drug delivery system: complete in vitro and in vivo toxicity analyses
title_full Facile design of lidocaine-loaded polymeric hydrogel to persuade effects of local anesthesia drug delivery system: complete in vitro and in vivo toxicity analyses
title_fullStr Facile design of lidocaine-loaded polymeric hydrogel to persuade effects of local anesthesia drug delivery system: complete in vitro and in vivo toxicity analyses
title_full_unstemmed Facile design of lidocaine-loaded polymeric hydrogel to persuade effects of local anesthesia drug delivery system: complete in vitro and in vivo toxicity analyses
title_sort facile design of lidocaine-loaded polymeric hydrogel to persuade effects of local anesthesia drug delivery system: complete in vitro and in vivo toxicity analyses
publisher Taylor & Francis Group
series Drug Delivery
issn 1071-7544
1521-0464
publishDate 2021-01-01
description The principal goal of the present investigation was to enterprise new and effective drug delivery vesicle for the sustained delivery of local anesthetic lidocaine hydrochloride (LDC), using a novel combination of copolymeric hydrogel with tetrahydroxyborate (COP–THB) to improve bioactivity and therapeutic potential. To support this contention, the physical and mechanical properties, rheological characteristics, and component release of candidate formulations were investigated. An optimized formulation of COP–THB containing LDC to an upper maximum concentration of 1.5% w/w was assessed for drug crystallization. The biocompatibility of the prepared COP–THB hydrogel was exhibited strong cell survival (96%) and growth compatibility on L929 fibroblast cell lines, which was confirmed by using methods of MTT assay and microscopic observations. The COP–THB hydrogel release pattern is distinct from that of COP–THB/LDC hydrogels by the slow-release rate and the low percentage of cumulative release. In vivo evaluations were demonstrated the anesthetic effects and toxicity value of treated samples by using mice models. In addition, COP–THB/LDC hydrogels significantly inhibit in vivo tumor growth in mice model and effectively reduced it is in vivo toxicity. The pharmacological evaluation showed that encapsulation of LDC in COP–THB hydrogels prolonged its anesthetic action with favorable in vitro and in vivo compatibility. This novel design may theoretically be used in promising studies involving the controlled release of local anesthetics.Highlights Development a modified sustained release system for the local anesthetic lidocaine. PVP-THB hydrogel to improve the pharmacological properties of the drug and their anesthetic activities. Profiles of PVP-THB/LDC showed that the effective release of associated lidocaine. This new formulation could potentially be used in future local anesthetics.
topic hydrogel
ldc
in vitro release
l929 cells
in vivo evaluations
drug delivery
url http://dx.doi.org/10.1080/10717544.2021.1931558
work_keys_str_mv AT yanli faciledesignoflidocaineloadedpolymerichydrogeltopersuadeeffectsoflocalanesthesiadrugdeliverysystemcompleteinvitroandinvivotoxicityanalyses
AT erxianzhao faciledesignoflidocaineloadedpolymerichydrogeltopersuadeeffectsoflocalanesthesiadrugdeliverysystemcompleteinvitroandinvivotoxicityanalyses
AT lili faciledesignoflidocaineloadedpolymerichydrogeltopersuadeeffectsoflocalanesthesiadrugdeliverysystemcompleteinvitroandinvivotoxicityanalyses
AT liyingbai faciledesignoflidocaineloadedpolymerichydrogeltopersuadeeffectsoflocalanesthesiadrugdeliverysystemcompleteinvitroandinvivotoxicityanalyses
AT weizhang faciledesignoflidocaineloadedpolymerichydrogeltopersuadeeffectsoflocalanesthesiadrugdeliverysystemcompleteinvitroandinvivotoxicityanalyses
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