Efficient nuclear drug translocation and improved drug efficacy mediated by acidity-responsive boronate-linked dextran/cholesterol nanoassembly

Jing-Yi Zhu; Qi Lei; Bin Yang; Hui-Zhen Jia; Wen-Xiu Qiu; Xuli Wang; Xuan Zeng; Ren-Xi Zhuo; Jun Feng; Xian-Zheng Zhang

doi:10.1016/j.biomaterials.2015.02.048

Efficient nuclear drug translocation and improved drug efficacy mediated by acidity-responsive boronate-linked dextran/cholesterol nanoassembly

Biomaterials. 2015 Jun:52:281-90. doi: 10.1016/j.biomaterials.2015.02.048. Epub 2015 Feb 28.

Authors

Jing-Yi Zhu¹, Qi Lei¹, Bin Yang¹, Hui-Zhen Jia¹, Wen-Xiu Qiu¹, Xuli Wang², Xuan Zeng¹, Ren-Xi Zhuo¹, Jun Feng³, Xian-Zheng Zhang¹

Affiliations

¹ Key Laboratory of Biomedical Polymers of Ministry of Education & Department of Chemistry, Wuhan University, Wuhan 430072, China.
² Department of Pharmaceutics and Pharmaceutical Chemistry, University of Utah, Salt Lake City, UT 84108, USA.
³ Key Laboratory of Biomedical Polymers of Ministry of Education & Department of Chemistry, Wuhan University, Wuhan 430072, China. Electronic address: fengjun@whu.edu.cn.

PMID: 25818434
DOI: 10.1016/j.biomaterials.2015.02.048

Abstract

The present study reported a lysosome-acidity-targeting bio-responsive nanovehicle self-assembled from dextran (Dex) and phenylboronic acid modified cholesterol (Chol-PBA), aiming at the nucleus-tropic drug delivery. The prominent advantage of this assembled nanoconstruction arose from its susceptibility to acidity-labile dissociation concurrently accompanied with the fast liberation of encapsulated drugs, leading to efficient nuclear drug translocation and consequently favorable drug efficacy. By elaborately exploiting NH4Cl pretreatment to interfere with the cellular endosomal acidification progression, this study clearly evidenced at a cellular level the strong lysosomal-acidity dependency of nuclear drug uptake efficiency, which was shown to be the main factor influencing the drug efficacy. The boronate-linked nanoassembly displayed nearly no cytotoxicity and can remain structural stability under the simulated physiological conditions including 10% serum and the normal blood sugar concentration. The cellular exposure to cholesterol was found to bate the cellular uptake of nanoassembly in a dose-dependent manner, suggesting a cholesterol-associated mechanism of the intracellular internalization. The in vivo antitumor assessment in xenograft mouse models revealed the significant superiority of DOX-loaded Dex/Chol-PBA nanoassembly over the controls including free DOX and the DOX-loaded non-sensitive Dex-Chol, as reflected by the more effective tumor-growth inhibition and the better systematic safety. In terms of the convenient preparation, sensitive response to lysosomal acidity and efficient nuclear drug translocation, Dex/Chol-PBA nanoassembly derived from natural materials shows promising potentials as the nanovehicle for nucleus-tropic drug delivery especially for antitumor agents. More attractively, this study offers a deeper insight into the mechanism concerning the contribution of acidity-responsive delivery to the enhanced chemotherapy performance.

Keywords: Acidity-responsiveness; Boronate linking; Lysosomal acidity; Nanoassembly; Nuclear drug translocation; Tumor chemotherapy.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Active Transport, Cell Nucleus
Animals
Antineoplastic Agents / administration & dosage
Boron / chemistry*
Boronic Acids / chemistry
Carbamates / chemistry
Cell Nucleus / drug effects
Cell Nucleus / metabolism*
Cholesterol / chemistry*
Cytoplasm / metabolism
Dextrans / chemistry*
Drug Carriers / chemistry*
Endosomes / metabolism
Female
HeLa Cells
Humans
Lysosomes / chemistry
Magnetic Resonance Spectroscopy
Mice
Mice, Inbred BALB C
Mice, Nude
Micelles
Microscopy, Electron, Transmission
Nanomedicine
Nanoparticles / chemistry*
Neoplasm Transplantation
Particle Size

Substances

Antineoplastic Agents
Boronic Acids
Carbamates
Dextrans
Drug Carriers
Micelles
Cholesterol
benzeneboronic acid
Boron