Design and construction of self-hidden and pH-reversed targeting drug delivery nanovehicles via noncovalent interactions to overcome drug resistance

Design and construction of self-hidden and pH-reversed targeting drug delivery nanovehicles via noncovalent interactions to overcome drug resistance

Using the host-guest interaction between β-cyclodextrin (β-CD) and adamantane (Ad), and borate formation between phenylboronic acid (PBA) and cis-diols, a smart pH-responsible targeting drug delivery nanovehicle, PBA-PEG-CD/Ad-lys(Diol)-PCL, was prepared via one-step self-assembly. Under physiologic...

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Veröffentlicht in:Journal of materials chemistry. B, Materials for biology and medicine Materials for biology and medicine, 2017-04, Vol.5 (15), p.2823-2831
Hauptverfasser: Zhao, Dan, Yi, Xiaoqing, Xu, Jiaqi, Yuan, Gongdao, Zhuo, Renxi, Li, Feng
Format: Artikel
Sprache:eng
Schlagworte:
Binding
Chemotherapy
Drug delivery systems
Drugs
Nanostructure
Self assembly
Toxicity
Uptakes
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container_end_page 2831
container_issue 15
container_start_page 2823
container_title Journal of materials chemistry. B, Materials for biology and medicine
container_volume 5
creator Zhao, Dan
Yi, Xiaoqing
Xu, Jiaqi
Yuan, Gongdao
Zhuo, Renxi
Li, Feng
description Using the host-guest interaction between β-cyclodextrin (β-CD) and adamantane (Ad), and borate formation between phenylboronic acid (PBA) and cis-diols, a smart pH-responsible targeting drug delivery nanovehicle, PBA-PEG-CD/Ad-lys(Diol)-PCL, was prepared via one-step self-assembly. Under physiological conditions, the targeted PBA function could be restrained by binding PBA with diol components located at the interface of self-assemblies, and hydrophilic PEG segments could be shielded simultaneously. When the environmental pH decreased, the PBA groups could be unbound and exposed on the surface of self-assemblies, leading to recovery of its targeted function, as shown using fluorescence spectroscopy, in vitro cell toxicity, and uptake. Under acidic conditions, PBA-PEG-CD/Ad-lys(Diol)-PCL/Dox showed significantly increased uptake and toxicity toward HepG2 cells in comparison with the control group. The smart vehicles were further utilized to test their efficiency in overcoming drug resistance in chemotherapy. Compared with free Dox, PBA-PEG-CD/Ad-lys(Diol)-PCL delivered six times more Dox into MCF-7/ADR cells and showed greater toxicity toward the ADR cells. As a result, this may be a facile strategy toward constructing efficient targeting vehicles through the rational utilization of noncovalent interactions.
doi_str_mv 10.1039/C6TB03211G
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source Royal Society Of Chemistry Journals 2008-
subjects Binding
Chemotherapy
Drug delivery systems
Drugs
Nanostructure
Self assembly
Toxicity
Uptakes
title Design and construction of self-hidden and pH-reversed targeting drug delivery nanovehicles via noncovalent interactions to overcome drug resistance
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