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The role of polymer matrix structure and interparticle interactions in diffusion-limited drug release.

机译:聚合物基质结构和颗粒间相互作用在扩散受限药物释放中的作用。

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摘要

A lattice random-walk model is used to simulate diffusion in a porous polymer. This model may be useful for the practical design of drug-release systems. Both interacting and noninteracting particles (random walkers) were allowed to diffuse through a pore with a single exit hole. It was found that the specific interactions among the diffusing particles have little influence on the overall release rate. Diffusion through more complicated structures was investigated by simulating the diffusion of particles through two pores connected by a constricted channel whose length and width were varied. The overall rate of release was found to be proportional to the width of the constricted channel. When the length of the channel was greater than or equal to the length of the pore, the rate of release was also inversely proportional to the channel length. From a practical standpoint, release rates can be decreased (and times for release increased) by one or two orders of magnitude by decreasing the width and expanding the length of the interconnecting channels in the polymer matrix.
机译:晶格随机游走模型用于模拟在多孔聚合物中的扩散。该模型对于药物释放系统的实际设计可能有用。相互作用和非相互作用的粒子(随机游动粒子)都可以通过具有单个出口的孔扩散。发现扩散颗粒之间的特定相互作用对总释放速率几乎没有影响。通过模拟颗粒在两个孔中的扩散情况,扩散是通过更复杂的结构进行的,该孔由长度和宽度变化的狭窄通道连接。发现总的释放速率与狭窄通道的宽度成比例。当通道的长度大于或等于孔的长度时,释放速率也与通道长度成反比。从实际的角度来看,通过减小聚合物基质中互连通道的宽度和长度,可以将释放速率降低一个或两个数量级(并且释放时间增加)。

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