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Biocompatible Fe3+ and Ca2+ Dual Cross-Linked G-Quadruplex Hydrogels as Effective Drug Delivery System for pH-Responsive Sustained Zero-Order Release of Doxorubicin

阿霉素 生物相容性材料 药物输送 化学 自愈水凝胶 零阶 对偶(语法数字) 生物医学工程 高分子化学 化疗 一级 医学 有机化学 艺术 外科 文学类 数学 应用数学
作者
Neha Thakur,Bhagwati Sharma,Suman Bishnoi,Siddarth Jain,Debasis Nayak,Tridib K. Sarma
出处
期刊:ACS applied bio materials [American Chemical Society]
卷期号:2 (8): 3300-3311 被引量:46
标识
DOI:10.1021/acsabm.9b00334
摘要

The ultimate aim in developing controlled drug delivery systems is to derive formulations to achieve drug release at a constant rate over a long duration. The drug release profile that follows zero-order kinetics is crucial for reduction in the drug administration frequency, reduced cytotoxicity, and improved convenience and compliance of patients. Designed drug delivery systems for achieving zero-order release are often complex, expensive, and difficult to manufacture. Herein, we demonstrate that a supramolecular hydrogel formed through the self-assembly of guanosine monophosphate (GMP) into highly ordered G-quadruplex structure and cross-linked through Fe3+ and Ca2+ ions exhibits potential for the pH-responsive controlled zero-order drug release of doxorubicin, a model chemotherapeutic drug. The fibril formation is initiated by the self-assembly of GMP into a quadruplex complex, which is cross-linked through the complexation of the phosphate groups with Fe(III) ions, resulting in a spontaneous hydrogel formation. The Ca2+ ions facilitate the improvement in the mechanical integrity of the fibril network in the Fe-GMP hydrogel via cross-linking of sugar moieties. The hydrogel showed a high loading capacity for drug molecules and a pH-responsive sustained zero-order drug release over several days owing to the lowered degradability of the cross-linked hydrogel in acidic buffer stimulant. In vitro drug-release studies further established a controlled pH-triggered drug release profile. The Ca2+ cross-linking of the Fe-GMP hydrogel also resulted in significant enhancement in the biocompatibility of the drug delivery system. The fabrication of biocompatible, low-cost, and efficient Ca2+ cross-linked metal-organic hydrogels may present promising applications in biological fields.
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