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Relationships between mechanical properties and drug release from electrospun fibers of PCL and PLGA blends

机译:机械性能与PCL和PLGA共混物电纺纤维中药物释放之间的关系

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摘要

Electrospun nanofibers have the potential to achieve high drug loading and the ability to sustain drug release. Mechanical properties of the drug-incorporated fibers suggest the importance of drug–polymer interactions. In this study, we investigated the mechanical properties of electrospun polycaprolactone (PCL) and poly (D,L-lactic-co-glycolic) acid (PLGA) fibers at various blend ratios in the presence and absence of a small molecule hydrophilic drug, tenofovir (TFV). Young׳s modulus of the blend fibers showed dependence on PLGA content and the addition of the drug. At a PCL/PLGA (20/80) composition, Young׳s modulus and tensile strength were independent of drug loading up to 40 wt% due to offsetting effects from drug–polymer interactions. In vitro drug release studies suggested that release of TFV significantly decreased fiber mechanical properties. In addition, mechanically stretched fibers displayed a faster release rate as compared to the non-stretched fibers. Finally, drug partition in the blend fibers was estimated using a mechanical model and then experimentally confirmed with a composite of individually stacked fiber meshes. This work provides scientific understanding on the dependence of drug release and drug loading on the mechanical properties of drug-eluting fibers.
机译:电纺纳米纤维具有实现高载药量和维持药物释放的能力。掺入药物的纤维的机械性能表明药物与聚合物相互作用的重要性。在这项研究中,我们研究了在存在和不存在小分子亲水性药物替诺福韦的情况下,电纺聚己内酯(PCL)和聚(D,L-乳酸-乙醇酸)(PLGA)纤维在各种混合比下的机械性能。 (TFV)。共混纤维的杨氏模量显示出对PLGA含量和药物添加的依赖性。在PCL / PLGA(20/80)组成下,由于药物与聚合物相互作用的抵消作用,杨氏模量和抗张强度与高达40 wt%的药物负载无关。体外药物释放研究表明,TFV的释放显着降低了纤维的机械性能。另外,与未拉伸的纤维相比,机械拉伸的纤维表现出更快的释放速率。最后,使用机械模型估算混合纤维中的药物分配,然后通过单独堆叠的纤维网复合材料进行实验确认。这项工作提供了对药物释放和药物负载对药物洗脱纤维机械性能的依赖性的科学理解。

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