Acoustically responsive scaffolds: Unraveling release kinetics and mechanisms for sustained, steady drug delivery

药物输送 动力学 自愈水凝胶 乳状液 超声波 化学 生物物理学 生物医学工程 治疗性超声 纤维蛋白 毒品携带者 微气泡 材料科学 纳米技术 医学 生物化学 高分子化学 免疫学 物理 量子力学 生物 放射科
作者
Haijun Xiao,Mitra Aliabouzar,Mario L. Fabiilli
出处
期刊:Journal of Controlled Release [Elsevier BV]
卷期号:374: 205-218
标识
DOI:10.1016/j.jconrel.2024.08.001
摘要

Hydrogels can serve as local drug delivery depots that protect the biological activity of labile therapeutics. However, drug release from conventional hydrogels is typically rapid, which is not ideal for many therapeutic agents. We developed a composite hydrogel that enables sustained drug release in response to ultrasound. The composite, termed an acoustically responsive scaffold (ARS), consists of a fibrin hydrogel and a phase-shift emulsion. Upon exposure to ultrasound, the emulsion is vaporized into bubbles, which leads to release of drugs contained within the emulsion. Previously, ARSs have been used in regenerative applications to stimulate blood vessel growth. Here, we characterize the release kinetics and mechanisms of ARSs. Release exhibits a triphasic pattern compromising a slow phase prior to ultrasound exposure; a transient, fast phase immediately after ultrasound exposure that follows a sigmoidal profile; and a sustained, steady phase. In each phase, we demonstrate how derived kinetics parameters are impacted by the ARS composition (e.g., fibrin and emulsion concentrations) and ultrasound properties (e.g., acoustic pressure, pulse duration). Using confocal microscopy, protein assays, and B-mode ultrasound imaging, we demonstrate that drug release from an ARS is independent of fibrin degradation and dependent on bubble growth. These results are critical in optimizing ARSs for delivery of therapeutic agents.
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