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Synthesis, characterization and brain targeting potential of paclitaxel loaded thiamine-PPI nanoconjugates

机译:紫杉醇硫胺素-PPI纳米共轭物的合成,表征和脑靶向潜力

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Brain tumor is insidious complication which is difficult to treat because of the poor uptake of many potentially useful antitumor drugs through the blood-brain barrier (BBB). Present study was aimed for developing and exploring the use of thiamine conjugated poly(propylene imine) (PPI) dendrimers for increased delivery of paclitaxel (PTX) across the BBB. PTX loaded thiamine conjugated PPI dendrimers (PTX-Tm-PPI) shown increased drug loading and reduced hemolytic toxicity with suitability for prolonged delivery of PTX during in vitro release. Ex vivo cytotoxicity studies of free PTX, PTX-PPI and PTX-Tm-PPI dendrimers over IMR-32 human neuroblastoma cell line revealed higher potential of PTX-Tm-PPI nanoconjugate to retard tumor cell viability as compared to plain PTX or PTX-PPI. In vivo pharmacokinetics studies revealed significant (p < 0.05) slow clearance of PTX from the body via Tm-PPI nanoconjugate. Biodistribution studies confirmed about the targeting efficiency and higher biodistribution of Tm-PPI conjugates into the brain. The results concluded that the developed nanoconjugate has potential to deliver significantly higher amount of drug to brain tumor for improved therapeutic outcome.
机译:脑肿瘤是一种隐匿性并发症,由于很难通过血脑屏障(BBB)吸收许多潜在有用的抗肿瘤药物,因此难以治疗。目前的研究旨在开发和探索硫胺素共轭聚丙烯亚胺(PPI)树状聚合物在整个血脑屏障中增加紫杉醇(PTX)的递送。载有PTX的硫胺素共轭PPI树状聚合物(PTX-Tm-PPI)显示出增加的载药量和降低的溶血毒性,并适合在体外释放过程中延长PTX的递送时间。游离PTX,PTX-PPI和PTX-Tm-PPI树状聚合物对IMR-32人成神经细胞瘤细胞系的离体细胞毒性研究表明,与普通PTX或PTX-PPI相比,PTX-Tm-PPI纳米复合物具有更大的潜力来延缓肿瘤细胞的生存能力。体内药代动力学研究显示PTX通过Tm-PPI纳米共轭物从体内清除的速度显着(p <0.05)。生物分布研究证实了Tm-PPI偶联物进入大脑的靶向效率和更高的生物分布。结果得出结论,开发的纳米共轭物具有向脑肿瘤输送明显更多量的药物以改善治疗效果的潜力。

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