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首页> 外文期刊>Biomacromolecules >Evaluation of Amphiphilic Star/Linear-Dendritic Polymer Reverse Micelles for Transdermal Drug Delivery: Directing Carrier Properties by Tailoring Core versus Peripheral Branching
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Evaluation of Amphiphilic Star/Linear-Dendritic Polymer Reverse Micelles for Transdermal Drug Delivery: Directing Carrier Properties by Tailoring Core versus Peripheral Branching

机译:用于透皮药物递送的两亲星形/线性树枝状聚合物反转胶束的评价:通过剪裁芯与外周支化引导载体性能

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The reverse micelle self-assembly of lipophile-functionalized poly(ethylene glycol) (PEG) dendrimer hybrids is probed for applications in carrier-mediated transdermal drug delivery. Under investigation are topologically diverse amphiphiles featuring controlled branching motifs at either the polymer core (one-, two-, and four-arm PEG) and the polar/nonpolar interface (peripheral dendritic generations 0-2). Thus, a systematic investigation of the effect of branching location (core vs peripheral) on carrier properties is described. Dye-encapsulation experiments verify these materials are capable of forming well-defined aggregates and solubilizing polar compounds. Further quantification of reverse micelle critical micelle concentration and dye loading capacity for the branched amphiphile library was obtained through spectroscopy characterization. Both core and peripheral branching are shown to significantly influence dynamic encapsulation behavior, with evidence of location-based contributions extending beyond multiplicity of branching alone. Finally, the in vitro transdermal diffusion of the reverse micelle carriers was investigated through Franz diffusion cell experiments using physiologically relevant juvenile porcine dermis. The permeation results, combined with previously reported aggregate size trends, show the complex relationship between polymer branching and transdermal transport, with the lowest core- and highest peripherally-branched amphiphilic analogs exhibiting optimal transdermal permeation characteristics for this set of branched carriers.
机译:脂肪磷酸官能化聚(乙二醇)(PEG)树枝状聚合物杂交物的反向胶束自组装被用于载体介导的透皮药物递送中的应用。在调查中是拓扑多样的两种两亲层,其特征在于聚合物芯(单,两个和四臂PEG)和极性/非极性接口(外周树枝状代120-2)。因此,描述了对支链位置(核心Vs外周)对载体性质的影响的系统研究。染料包封实验验证这些材料能够形成明确定义的聚集体和溶解极性化合物。通过光谱表征获得反向胶束临界胶束浓度和染料负载染料负载染料负载能力的量化。核心和外围分支两者都被证明可以显着影响动态封装行为,证据显示超出多个分支的基于位置的贡献。最后,通过使用生理相关的幼年猪真皮通过Franz扩散细胞实验研究了反胶束载体的体外透皮扩散。渗透结果与先前报道的总体大小趋势结合,表现出聚合物分支和透皮转运之间的复杂关系,具有最低的核和最高的外周支化两亲类似物,其对于该组分支载体具有最佳的透皮渗透特性。

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