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首页> 外文期刊>ACS applied materials & interfaces >Elucidating the Drug Release from Metal-Organic Framework Nanocomposites via In Situ Synchrotron Microspectroscopy and Theoretical Modeling
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Elucidating the Drug Release from Metal-Organic Framework Nanocomposites via In Situ Synchrotron Microspectroscopy and Theoretical Modeling

机译:通过原位同步微型光谱检测和理论建模阐明金属 - 有机框架纳米复合材料的药物释放

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摘要

Nanocomposites comprising metal-organic frameworks (MOFs) embedded in a polymeric matrix are promising carriers for drug delivery applications. While understanding the chemical and physical transformations of MOFs during the release of confined drug molecules is challenging, this is central to devising better ways for controlled release of therapeutic agents. Herein, we demonstrate the efficacy of synchrotron microspectroscopy to track the in situ release of 5-fluorouracil (5-FU) anticancer drug molecules from a drug@MOF/polymer composite (5-FU@HKUST-1 /polyurethane). Using experimental time-resolved infrared spectra jointly with newly developed density functional theory calculations, we reveal the detailed dynamics of vibrational motions underpinning the dissociation of 5-FU bound to the framework of HKUST-1 upon water exposure. We discover that HKUST-1 creates hydrophilic channels within the hydrophobic polyurethane matrix hence helping to tune drug release rate. The synergy between a hydrophilic MOF with a hydrophobic polymer can be harnessed to engineer a tunable nanocomposite that alleviates the unwanted burst effect commonly encountered in drug delivery.
机译:包含嵌入聚合物基质中的金属 - 有机框架(MOF)的纳米复合材料是用于药物递送应用的有前途的载体。在理解狭窄药物分子释放期间MOFS的化学和物理转化是挑战性的,而这是对治疗剂的控制释放的更好方式设计的核心。在此,我们证明了同步辐射微型光谱从药物/聚合物复合材料(5-FU / 1-1 /聚氨酯)的5-氟尿嘧啶(5-FU)抗癌药物分子的原位释放的效果。使用实验时间分辨的红外光谱与新开发的密度泛函理论计算,我们揭示了振动运动的详细动态,支撑了5-fu的解离,涉及水暴露后的HKust-1框架。我们发现HKust-1在疏水性聚氨酯基质内产生亲水通道,因此有助于调节药物释放速率。可以利用具有疏水性聚合物的亲水MOF之间的协同作用,以改造可调谐的纳米复合材料,可缓解药物递送中通常遇到的不需要的突发效果。

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