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Nanoscale architectural tuning of parylene patch devices to control therapeutic release rates

机译:聚对二甲苯贴片设备的纳米级结构调整,以控制治疗释放速率

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The advent of therapeutic functionalized implant coatings has significantly impacted the medical device field by enabling prolonged device functionality for enhanced patient treatment. Incorporation of drug release from a stable, biocompatible surface is instrumental in decreasing systemic application of toxic therapeutics and increasing the lifespan of implants by the incorporation of antibiotics and anti-inflammatories. In this study, we have developed a parylene C-based device for controlled release of Doxorubicin, an anti-cancer chemotherapy and definitive read-out for preserved drug functionality, and further characterized the parylene deposition condition-dependent tunability of drug release. Drug release is controlled by the deposition of a layer of 20-200 nm thick parylene over the drug layer. This places a porous layer above the Doxorubicin, limiting drug elution based on drug accessibility to solvent and the solvent used. An increase in the thickness of the porous top layer prolongs the elution of active drug from the device from, in the conditions tested, the order of 10 min to the order of 2d in water and from the order of 10 min to no elution in PBS. Thus, the controlled release of an anti-cancer therapeutic has been achieved via scalably fabricated, parylene C-encapsulated drug delivery devices.
机译:治疗性功能化植入物涂层的出现通过实现延长的设备功能性以增强患者治疗能力,极大地影响了医疗设备领域。通过稳定的,具有生物相容性的表面释放药物,有助于减少毒性疗法的全身应用,并通过结合抗生素和消炎药来延长植入物的使用寿命。在这项研究中,我们开发了基于聚对二甲苯C的装置来控制阿霉素的释放,抗癌化学疗法和确定的读数以保持药物的功能,并进一步表征了聚对二甲苯沉积条件依赖性的药物释放可调性。药物释放是通过在药物层上沉积20-200 nm厚的聚对二甲苯层来控制的。这会在阿霉素上方放置一个多孔层,基于药物对溶剂和所用溶剂的可及性限制药物洗脱。多孔顶层厚度的增加将活性药物从设备中的洗脱时间延长,在测试条件下,在水中的时间从10分钟左右增加到2d,从PBS中的10分钟左右延长到无洗脱。因此,已经通过可缩放地制造的聚对二甲苯C包封的药物递送装置实现了抗癌治疗剂的控制释放。

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