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System-based Approach for an Advanced Drug Delivery Platform

机译:基于系统的高级药物交付平台方法

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Present study is looking at the problem of integrating drug delivery microcapsule, a bio-sensor, and a control mechanism into a biomedical drug delivery system. A wide range of medical practices from cancer therapy to gastroenterological treatments can benefit from such novel bio-system. Drug release in our drug delivery system is achieved by electrochemically actuating an array of polymeric valves on a set of drug reservoirs. The valves are bi-layer structures, made in the shape of a flap hinged on one side to a valve seat, and consisting of thin films of evaporated gold and electrochemically deposited polypyrrole (PPy). These thin PPy(DBS) bi-layer flaps cover access holes of underlying chambers micromachined in a silicon substrate. Chromium and polyimide layers are applied to implement "differential adhesion" to obtain a voltage induced deflection of the bi-layer away from the drug reservoir. The Cr is an adhesion-promoting layer, which is used to strongly bind the gold layer down to the substrate, whereas the gold adheres weakly to polyimide. Drug actives (dry or wet) were pre-stored in the chambers and their release is achieved upon the application of a small bias (~ 1V). Negative voltage causes cation adsorption and volume change in PPy film. This translates into the bending of the PPy/Au bi-layer actuator and release of the drug from reservoirs. This design of the drug delivery module is miniaturized to the dimensions of 200μm valve diameter. Galvanostatic and potentiostatic PPy deposition methods were compared, and potentiostatic deposition method yields film of more uniform thickness. PPy deposition experiments with various pyrrole and NaDBS concentrations were also performed. Glucose biosensor based on glucose oxidase (GOx) embedded in the PPy matrix during elechtrochemical deposition was manufactured and successfully tested. Multiple-drug pulsatile release and continuous linear release patterns can be implemented by controlling the operation of an array of valves. Varying amounts of drugs, together with more complex controlling strategies would allow creation of more complex drug delivery patterns.
机译:目前的研究正在研究将药物递送微胶囊,生物传感器和控制机制整合到生物医药药物递送系统中的问题。从癌症治疗到胃肠病理学治疗的广泛的医疗措施可以受益于这种新的生物系统。通过在一组药物储存器上电化学致动一系列聚合物阀来实现我们的药物输送系统中的药物释放。阀门是双层结构,其形状的翼片铰接在一侧到阀座上,并由蒸发金和电化学沉积的聚吡咯(PPY)的薄膜组成。这些薄PPY(DBS)双层襟翼覆盖硅衬底中的下面的底部腔室的进入孔。铬和聚酰亚胺层应用于实现“差动粘合性”,以获得远离药物储存器的Bi层的电压诱导偏转。 Cr是粘合促进层,其用于将金层粘附到基板上,而金粘附弱到聚酰亚胺。将药物活性物(干燥或湿)预先储存在腔室中,并且在施加小偏压(〜1V)时达到它们的释放。负电压导致PPY膜中的阳离子吸附和体积变化。这转化为PPY / AU双层致动器的弯曲和来自储存器的药物释放。这种药物输送模块的设计小型化到阀门直径200μm的尺寸。比较了电压静脉和电位型PPY沉积方法,电位沉积方法产生更均匀的薄膜。还进行了各种吡咯和NADB浓度的PPY沉积实验。制造并成功地测试基于在Elechtrochemical沉积中嵌入PPY基质中的葡萄糖氧化酶(GOX)的葡萄糖生物传感器。通过控制阀阵列的操作,可以通过控制阀门的操作来实现多药物脉冲释放和连续线性释放图案。不同量的药物,以及更复杂的控制策略将允许创造更复杂的药物交付模式。

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