Dually acid- and GSH-triggered bis(β-cyclodextrin) as drugs delivery nanoplatform for effective anticancer monotherapy

Author:

Chen Jian,Liu Hui,Li Xiufang,Li Jianbing,Tang Rongdi,Deng Zhiwei,Yang Yanjing,Zhong ShianORCID

Abstract

Abstract The intrinsic poor solubility and limited load capacity of β-cyclodextrins (β-CDs) results in reduced bioavailability, rendering the material unsuitable in complex biological environments. In this work, a pair of β-CDs was methylated and covalently linked with acid-sensitive acylhydrazone and GSH-sensitive disulfide bonds to ensure a precise drug release pattern. The hydrophobic anticancer drug doxorubicin (Dox) was encapsulated inside the hydrophobic core of bis(β-CD) via hydrophobic association with loading capacity of 24% in weight and a hydrodynamic size of about 100 nm. When exposed to acidic and reductive environments, the acylhydrazone and disulfide bonds were found to be cleaved, resulting in Dox release. Using fluorescence imaging and flow cytometry analysis, the designed bis(β-CD) were determined to activate the drug release behavior by specific intracellular stimuli (pH and GSH). In vivo studies demonstrated specific drug delivery characteristics and controlled drug release behaviors in the tumor sites, giving rise to high antitumor activity and low toxicity. Taken in concert, this dual stimuli-responsive bis(β-CD) with superior amphiphilicity and biocompatibility features showed great potential for future clinical applications.

Funder

Natural Science Foundation of Hunan Province

Scientific Research Fund of Hunan Provincial Education Department

National Natural Science Foundation of China

Publisher

IOP Publishing

Subject

Electrical and Electronic Engineering,Mechanical Engineering,Mechanics of Materials,General Materials Science,General Chemistry,Bioengineering

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