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Mechanisms of antiproliferative drug release from bioresorbable porous structures

机译:从生物可吸收的多孔结构释放抗增殖药物的机制

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Restenosis (renarrowing of the blood vessel wall) and cancer are two different pathologies that have drawn extensive research attention over the years. Antiproliferative drugs such as paclitaxel inhibit cell proliferation and are therefore effective in the treatment of cancer as well as neointimal hyperplasia, which is known to be the main cause of restenosis. Antiproliferative drugs are highly hydrophobic and their release from porous biodegradable structures is therefore advantageous. The release profiles of four antiproliferative drugs from highly porous polymeric structures were studied in this study in light of the physical properties of both the host polymers and the drug molecules, and a qualitative model was developed. The chemical structure of the polymer chain directly affects the drug release profile through water uptake in the early stages or degradation and erosion in later stages. It also affects the release profile indirectly, through the polymer's 3D porous structure. However, this effect is minor. The drug volume and molecular area dominantly affect its diffusion rate from the 3D porous structure and the drug's solubility parameter compared with that of the host polymer has some effect on the drug release profile. This model can also be used to describe release mechanisms of other hydrophobic drugs from porous structures.
机译:再狭窄(血管壁变窄)和癌症是两种不同的病理学,多年来引起了广泛的研究关注。紫杉醇等抗增殖药可抑制细胞增殖,因此可有效治疗癌症以及新内膜增生,这是再狭窄的主要原因。抗增殖药物是高度疏水的,因此它们从多孔的可生物降解结构中释放是有利的。根据宿主聚合物和药物分子的物理特性,研究了四种抗增殖药物从高度多孔的聚合物结构中的释放曲线,并建立了定性模型。聚合物链的化学结构通过在早期吸收水分或在后期降解和侵蚀直接影响药物释放曲线。它还通过聚合物的3D多孔结构间接影响释放曲线。但是,这种影响很小。与主体聚合物的溶解度参数相比,药物的体积和分子面积主要影响其从3D多孔结构的扩散速率,并且药物的溶解度参数对药物释放曲线有一定影响。该模型还可用于描述其他疏水性药物从多孔结构中释放的机理。

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