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探索以生物相容性脂肪酸为相变材料、在乙基纤维素纳米纤维中实现温度响应性药物递送。

Exploring temperature-responsive drug delivery with biocompatible fatty acids as phase change materials in ethyl cellulose nanofibers.

作者信息

Wildy Michael, Wei Wanying, Xu Kai, Schossig John, Hu Xiao, la Cruz David Salas-de, Hyun Dong Choon, Lu Ping

机构信息

Department of Chemistry and Biochemistry, Rowan University, Glassboro, NJ 08028, United States.

Department of Physics and Astronomy, Rowan University, Glassboro, NJ 08028, United States.

出版信息

Int J Biol Macromol. 2024 May;266(Pt 1):131187. doi: 10.1016/j.ijbiomac.2024.131187. Epub 2024 Mar 28.

Abstract

This study introduces a novel temperature-responsive drug delivery system using ethyl cellulose (EC) nanofibers encapsulating a eutectic mixture of lauric acid/stearic acid (LA/SA) as phase change materials (PCMs) and Rhodamine B (RhB) as a model drug. Employing blend electrospinning, the nanofibers achieved controlled drug release responsive to temperature changes. The peak shift of the carbonyl group in FTIR analysis confirmed drug-polymer compatibility, while the absence of RhB peaks in the XRD and DSC assessments revealed RhB's amorphous distribution within the fibers. Our findings demonstrate that RhB release is dependent on its loading, with a slow initial release (<2 %) for 1 % and 5 % RhB loadings and a burst release (~12 %) for 10 % loading. Notably, the release rate was tunable at 37 °C by adjusting LA/SA concentration. The optimal LA/SA loading for temperature-responsive release is identified as 10 %. Over 240 h, there is a 32 % increase in RhB release at 37 °C, and an additional 8 % increase at 40 °C, compared to 25 °C. This research illustrates the potential of PCM-integrated nanofibers in smart drug delivery, particularly for chemotherapy, antibiotics, and anti-inflammatory drugs, showcasing an innovative approach to improving therapeutic efficiency while reducing side effects.

摘要

本研究介绍了一种新型的温度响应型药物递送系统,该系统使用乙基纤维素(EC)纳米纤维包裹月桂酸/硬脂酸(LA/SA)的低共熔混合物作为相变材料(PCM),并以罗丹明B(RhB)作为模型药物。通过共混静电纺丝,纳米纤维实现了对温度变化的可控药物释放。傅里叶变换红外光谱(FTIR)分析中羰基的峰位移动证实了药物与聚合物的相容性,而X射线衍射(XRD)和差示扫描量热法(DSC)评估中RhB峰的缺失表明RhB在纤维内呈无定形分布。我们的研究结果表明,RhB的释放取决于其负载量,1%和5%RhB负载量时初始释放缓慢(<2%),10%负载量时出现突释(约12%)。值得注意的是,通过调节LA/SA浓度,可在37℃调节释放速率。确定温度响应释放的最佳LA/SA负载量为10%。与25℃相比,在37℃下2S0小时内RhB释放增加32%,在40℃下再增加8%。本研究说明了集成PCM的纳米纤维在智能药物递送中的潜力,特别是在化疗、抗生素和抗炎药物方面,展示了一种提高治疗效率同时减少副作用的创新方法。

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