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MAD (Multiagent Delivery) Nanolayer: Delivering Multiple Therapeutics from Hierarchically Assembled Surface Coatings

机译:MAD(多剂递送)纳米层:从分层组装的表面涂层中递送多种疗法

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摘要

We present hydrolytically degradable polymeric multilayer films that call codeliver multiple therapeutics of differing chemical characteristics (charged biomacromolecules and neutral hydrophobic small molecules) from a surface. This multiagent-delivery (MAD) nanolayer system integrates the hydrolytically degradable poly(beta-amino ester) as a structural component to control the degradation of the multilayers to release active therapeutic macromolecules as well as hydrophobic drugs imbedded within amphiphilic block copolymer micellar carriers within layer-by-layer (LbL) Films, which would otherwise be difficult to include within the multilayers. By varying the anionic therapeutic agents (heparin and dextran sulfate) within the multilayer, we examine how different structural components call be used to control the release kinetics of multiple therapeutics from MAD nanolayers. Controlled release profiles and the in vitro efficacy of the MAD nanolayers ill Suppressing the growth of human smooth muscle cell lines were evaluated. The dual delivery of a charged macromolecular heparin and a small hydrophobic drug, paclitaxel, is found to be synergistic and beneficial toward effective therapeutic activity. Furthermore, we compared the classical dipping method that we employed here with an automated spray-LbL technique. Spray-LbL significantly facilitates film processing time while preserving the characteristic release profiles of the MAD nanolayers. With the highly versatile and tunable nature or LbL assembly, we anticipate that MAD nanolayers call provide a unique platform for delivering multiple therapeutics from macromolecules to small molecules with distinct release profiles for applications in biological and biomedical surface coatings.
机译:我们提出了一种可水解降解的聚合物多层膜,该膜称为Codeliver从表面起具有不同化学特征(带电的生物大分子和中性的疏水性小分子)的多种疗法。该多试剂传递(MAD)纳米层系统集成了可水解降解的聚(β-氨基酯)作为结构成分,以控制多层的降解,从而释放出活性治疗性大分子以及嵌入层内两亲嵌段共聚物胶束载体中的疏水性药物层(LbL)膜,否则很难包含在多层膜中。通过改变多层内的阴离子治疗剂(肝素和硫酸葡聚糖),我们研究了如何调用不同的结构成分来控制多种治疗剂从MAD纳米层的释放动力学。评估了抑制人平滑肌细胞系生长的MAD纳米层的控释曲线和体外功效。发现带电荷的大分子肝素和小的疏水性药物紫杉醇的双重递送具有协同作用,并且对有效的治疗活性有益。此外,我们将我们在此处采用的经典浸渍方法与自动喷雾LbL技术进行了比较。 Spray-LbL显着缩短了膜处理时间,同时保留了MAD纳米层的特征性释放曲线。凭借高度通用和可调谐的特性或LbL组装,我们预计MAD纳米层将为从大分子到具有不同释放曲线的小分子提供多种治疗药物,用于生物和生物医学表面涂层,提供独特的平台。

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