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Optimizing molecular weight of octyl chitosan as drug carrier for improving tumor therapeutic efficacy

机译:优化辛基壳聚糖的分子量作为药物载体提高肿瘤治疗效果

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摘要

Macromolecular drug carriers have attracted much attention taking advantage of passive tumor targeting property and excellent biocompatibility. For many biomedical applications, however, the effectiveness of the carriers is insufficient, which complicate further development into clinical use. Here, we systematically investigated the effects of molecular weight (from 1KDa to 300KDa) of macromolecular drug carrier, octyl chitosan, on tumor accumulation and penetration, as well as drug loading and releasing profiles. It was found that the molecular weight of chitosan influenced the cellular uptake and pharmacokinetic behavior of the nanocarriers, which ultimately determined their drug delivery efficiency. Interestingly, increased molecular weight of chitosan decreased its cellular uptake but increased its resident time in blood, which provided ample time for tumor accumulation. Moreover, the molecular weight altered the drug loading capability and release profile. Our results demonstrated that 10KDa octyl chitosan was an ideal candidate for anticancer drug delivery, which could deliver anticancer agent to tumor tissues and release drugs in tumor cells more effectively than those of other molecular weights, and finally result in better therapeutic effect.
机译:大分子药物载体由于具有被动靶向肿瘤的特性和出色的生物相容性而备受关注。然而,对于许多生物医学应用而言,载体的效力不足,这使得进一步开发临床应用变得复杂。在这里,我们系统地研究了高分子药物载体辛基壳聚糖的分子量(从1KDa到300KDa)对肿瘤积累和渗透以及载药量和释放曲线的影响。发现壳聚糖的分子量影响纳米载体的细胞摄取和药代动力学行为,这最终决定了它们的药物递送效率。有趣的是,壳聚糖分子量的增加降低了其细胞摄取,但增加了其在血液中的停留时间,这为肿瘤积累提供了充足的时间。此外,分子量改变了药物负载能力和释放曲线。我们的结果表明10KDa辛基壳聚糖是抗癌药物的理想候选药物,与其他分子量的抗癌药物相比,它可以将抗癌药物输送到肿瘤组织并更有效地在肿瘤细胞中释放药物,最终产生更好的治疗效果。

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