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Effects of P-Glycoprotein on the Transport of DL0410, a Potential Multifunctional Anti-Alzheimer Agent

机译:P糖蛋白对潜在的多功能抗阿尔茨海默病药物DL0410转运的影响

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In our study, we attempted to investigate the influences of P-glycoprotein (P-gp) on DL0410, a novel synthetic molecule for Alzheimer’s disease (AD) treatment, for intestinal absorption and blood-brain barrier permeability in vitro and related binding mechanisms in silico. Caco-2, MDCK, and MDCK-MDR1 cells were utilized for transport studies, and homology modelling of human P-gp was built for further docking study to uncover the binding mode of DL0410. The results showed that the apparent permeability (Papp) value of DL0410 was approximately 1 × 10?6 cm/s, indicating the low permeability of DL0410. With the presence of verapamil, the directional transport of DL0410 disappeared in Caco-2 and MDCK-MDR1 cells, suggesting that DL0410 should be a substrate of P-gp, which was also confirmed by P-gp ATPase assay. In addition, DL0410 could competitively inhibit the transport of Rho123, a P-gp known substrate. According to molecular docking, we also found that DL0410 could bind to the drug binding pocket (DBP), but not the nucleotide binding domain (NBD). In conclusion, DL0410 was a substrate as well as a competitive inhibitor of P-gp, and P-gp had a remarkable impact on the intestine and brain permeability of DL0410, which is of significance for drug research and development. View Full-Text
机译:在我们的研究中,我们试图研究P-糖蛋白(P-gp)对DL0410(一种用于阿尔茨海默氏病(AD)治疗的新型合成分子)在体外的肠道吸收和血脑屏障通透性的影响以及相关的结合机制。硅片。 Caco-2,MDCK和MDCK-MDR1细胞用于转运研究,并建立了人P-gp的同源性模型用于进一步的对接研究,以揭示DL0410的结合模式。结果表明,DL0410的表观渗透率(Papp)约为1×10?6 cm / s,表明DL0410的渗透率较低。在维拉帕米的存在下,DL0410的定向转运在Caco-2和MDCK-MDR1细胞中消失了,这表明DL0410应该是P-gp的底物,这也通过P-gp ATPase测定得到了证实。另外,DL0410可以竞争性地抑制Rho123(一种P-gp已知底物)的转运。根据分子对接,我们还发现DL0410可以与药物结合袋(DBP)结合,但不能与核苷酸结合域(NBD)结合。总之,DL0410是P-gp的底物和竞争性抑制剂,P-gp对DL0410的肠和脑通透性具有显着影响,这对药物的研究和开发具有重要意义。查看全文

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