Tumor Microenvironment-Responsive Shell/Core Composite Nanoparticles for Enhanced Stability and Antitumor Efficiency Based on a pH-Triggered Charge-Reversal Mechanism

Tumor Microenvironment-Responsive Shell/Core Composite Nanoparticles for Enhanced Stability and Antitumor Efficiency Based on a pH-Triggered Charge-Reversal Mechanism

High systemic stability and effective tumor accumulation of chemotherapeutic agents are indispensable elements that determine their antitumor efficacy. PEGylation of nanoparticles (NPs) could prolong the retention time in vivo by improving their stability in circulation, but treatment suffers reduce...

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Main Authors: Qiuhua Luo, Wen Shi, Puxiu Wang, Yu Zhang, Jia Meng, Ling Zhang
Format: Article
Language:English
Published: MDPI AG 2021-06-01
Series:Pharmaceutics
Subjects:
shielding system
shell/core structure
charge-reversal
pH-triggered
cancer therapy
Online Access:https://www.mdpi.com/1999-4923/13/6/895
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spelling doaj-fb85db2f3d9e4760842ef426370aa2752021-07-01T00:20:25ZengMDPI AGPharmaceutics1999-49232021-06-011389589510.3390/pharmaceutics13060895Tumor Microenvironment-Responsive Shell/Core Composite Nanoparticles for Enhanced Stability and Antitumor Efficiency Based on a pH-Triggered Charge-Reversal MechanismQiuhua Luo0Wen Shi1Puxiu Wang2Yu Zhang3Jia Meng4Ling Zhang5Department of Pharmacy, The First Affiliated Hospital of China Medical University, Shenyang 110001, ChinaDepartment of Pharmacy, The First Affiliated Hospital of China Medical University, Shenyang 110001, ChinaDepartment of Pharmacy, The First Affiliated Hospital of China Medical University, Shenyang 110001, ChinaDepartment of Pharmaceutics, College of Pharmacy, Shenyang Pharmaceutical University, Shenyang 110016, ChinaDepartment of Pharmacy, Liaoning Institute of Basic Medicine, Shenyang 110101, ChinaDepartment of Biotherapy, Cancer Research Institute, The First Affiliated Hospital of China Medical University, Shenyang 110001, ChinaHigh systemic stability and effective tumor accumulation of chemotherapeutic agents are indispensable elements that determine their antitumor efficacy. PEGylation of nanoparticles (NPs) could prolong the retention time in vivo by improving their stability in circulation, but treatment suffers reduced tumor penetration and cellular uptake of nanomedicines. The tumor microenvironment (TME)-responsive NPs maintain their stealth features during circulation and undergo a stimuli-responsive dePEGylation once exposed to the site of action, thereby achieving enhanced internalization in tumor cells. Herein, TME-responsive shell/core composite nanoparticles were prepared and optimized with enhanced stability and tumor intake efficiency. We synthesized 12-hydroxystearic acid-poly (ethylene glycol)-YGRKKRRQRRR (HA-PEG-TAT) as a post-insert apparatus in disulfiram (DSF)-encapsulated naked nanoparticles (N-NPs) in order to form a cationic core (TAT-NPs). Accordingly, the negatively charged poly (glutamate acid)-graft-poly (ethylene glycol) (PGlu-PEG) was further applied to the surface of TAT-NPs as a negative charged shell (PGlu-PEG/TAT-NPs) via the electrostatic interaction between glutamic acids and arginine at the outer ring of the TAT-NPs. PGlu-PEG/TAT-NPs displayed a huge loading capability for DSF with reduced degradation in plasma and exhibited rapid charge reversal when pH decreased from 7.4 to pH 6.5, demonstrating an excellent systemic stability as well as intelligent stimuli-responsive performance within the acidic TME. Furthermore, the in vivo antitumor study revealed that PGlu-PEG/TAT-NPs provided greater antitumor efficacy compared with free DSF and N-NPs with no obvious systemic toxicity. In conclusion, the TME-responsive shell/core composite NPs, consisting of PGlu-PEG and HS-PEG-TAT, could mediate an effective and biocompatible delivery of chemotherapeutic agents with clinical potential.https://www.mdpi.com/1999-4923/13/6/895shielding systemshell/core structurecharge-reversalpH-triggeredcancer therapy
collection DOAJ
language English
format Article
sources DOAJ
author Qiuhua Luo
Wen Shi
Puxiu Wang
Yu Zhang
Jia Meng
Ling Zhang
spellingShingle Qiuhua Luo
Wen Shi
Puxiu Wang
Yu Zhang
Jia Meng
Ling Zhang
Tumor Microenvironment-Responsive Shell/Core Composite Nanoparticles for Enhanced Stability and Antitumor Efficiency Based on a pH-Triggered Charge-Reversal Mechanism
Pharmaceutics
shielding system
shell/core structure
charge-reversal
pH-triggered
cancer therapy
author_facet Qiuhua Luo
Wen Shi
Puxiu Wang
Yu Zhang
Jia Meng
Ling Zhang
author_sort Qiuhua Luo
title Tumor Microenvironment-Responsive Shell/Core Composite Nanoparticles for Enhanced Stability and Antitumor Efficiency Based on a pH-Triggered Charge-Reversal Mechanism
title_short Tumor Microenvironment-Responsive Shell/Core Composite Nanoparticles for Enhanced Stability and Antitumor Efficiency Based on a pH-Triggered Charge-Reversal Mechanism
title_full Tumor Microenvironment-Responsive Shell/Core Composite Nanoparticles for Enhanced Stability and Antitumor Efficiency Based on a pH-Triggered Charge-Reversal Mechanism
title_fullStr Tumor Microenvironment-Responsive Shell/Core Composite Nanoparticles for Enhanced Stability and Antitumor Efficiency Based on a pH-Triggered Charge-Reversal Mechanism
title_full_unstemmed Tumor Microenvironment-Responsive Shell/Core Composite Nanoparticles for Enhanced Stability and Antitumor Efficiency Based on a pH-Triggered Charge-Reversal Mechanism
title_sort tumor microenvironment-responsive shell/core composite nanoparticles for enhanced stability and antitumor efficiency based on a ph-triggered charge-reversal mechanism
publisher MDPI AG
series Pharmaceutics
issn 1999-4923
publishDate 2021-06-01
description High systemic stability and effective tumor accumulation of chemotherapeutic agents are indispensable elements that determine their antitumor efficacy. PEGylation of nanoparticles (NPs) could prolong the retention time in vivo by improving their stability in circulation, but treatment suffers reduced tumor penetration and cellular uptake of nanomedicines. The tumor microenvironment (TME)-responsive NPs maintain their stealth features during circulation and undergo a stimuli-responsive dePEGylation once exposed to the site of action, thereby achieving enhanced internalization in tumor cells. Herein, TME-responsive shell/core composite nanoparticles were prepared and optimized with enhanced stability and tumor intake efficiency. We synthesized 12-hydroxystearic acid-poly (ethylene glycol)-YGRKKRRQRRR (HA-PEG-TAT) as a post-insert apparatus in disulfiram (DSF)-encapsulated naked nanoparticles (N-NPs) in order to form a cationic core (TAT-NPs). Accordingly, the negatively charged poly (glutamate acid)-graft-poly (ethylene glycol) (PGlu-PEG) was further applied to the surface of TAT-NPs as a negative charged shell (PGlu-PEG/TAT-NPs) via the electrostatic interaction between glutamic acids and arginine at the outer ring of the TAT-NPs. PGlu-PEG/TAT-NPs displayed a huge loading capability for DSF with reduced degradation in plasma and exhibited rapid charge reversal when pH decreased from 7.4 to pH 6.5, demonstrating an excellent systemic stability as well as intelligent stimuli-responsive performance within the acidic TME. Furthermore, the in vivo antitumor study revealed that PGlu-PEG/TAT-NPs provided greater antitumor efficacy compared with free DSF and N-NPs with no obvious systemic toxicity. In conclusion, the TME-responsive shell/core composite NPs, consisting of PGlu-PEG and HS-PEG-TAT, could mediate an effective and biocompatible delivery of chemotherapeutic agents with clinical potential.
topic shielding system
shell/core structure
charge-reversal
pH-triggered
cancer therapy
url https://www.mdpi.com/1999-4923/13/6/895
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AT wenshi tumormicroenvironmentresponsiveshellcorecompositenanoparticlesforenhancedstabilityandantitumorefficiencybasedonaphtriggeredchargereversalmechanism
AT puxiuwang tumormicroenvironmentresponsiveshellcorecompositenanoparticlesforenhancedstabilityandantitumorefficiencybasedonaphtriggeredchargereversalmechanism
AT yuzhang tumormicroenvironmentresponsiveshellcorecompositenanoparticlesforenhancedstabilityandantitumorefficiencybasedonaphtriggeredchargereversalmechanism
AT jiameng tumormicroenvironmentresponsiveshellcorecompositenanoparticlesforenhancedstabilityandantitumorefficiencybasedonaphtriggeredchargereversalmechanism
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