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Nasal Delivery of P-gp Substrates to the Brain through the Nose–Brain Pathway

机译:通过鼻-脑通路将P-gp底物经鼻腔递送至大脑

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The objective of this study was to evaluate in rats the potential utility of the nasal route to enhance central nervous system (CNS) delivery of drugs recognized by P-glycoprotein (P-gp). Well-known P-gp substrates verapamil and talinolol were perfused nasally or infused intravenously, and when plasma concentrations following intravenous infusion and nasal perfusion showed similar profiles. The concentration of verapamil in the brain after nasal perfusion was twice that after intravenous infusion. Although talinolol in the brain and the cerebrospinal fluid after i.v. infusion were below the detection limit, it was detected after nasal perfusion. When rats were treated with cyclosporin A, brain concentrations of verapamil after both administration modes were increased significantly, while those of talinolol were not significantly changed. Since the permeability of talinolol is low, talinolol in the brain which was transported directly from the nasal cavity has little chance of transport by P-gp localized in the apical membrane of cerebral microvessel endothelial cells. The potential for drug delivery utilizing the nose–CNS route was confirmed for P-gp substrates. The advantage of nasal delivery over i.v. delivery of talinolol to the brain was more significant than that of verapamil, suggesting that nasal administration is more useful strategy for the brain delivery of low-permeability P-gp substrates than the use of P-gp inhibitors.
机译:这项研究的目的是评估大鼠鼻腔途径增强由P-糖蛋白(P-gp)识别的中枢神经系统(CNS)传递的潜在效用。众所周知的P-gp底物维拉帕米和他尼洛尔经鼻灌注或静脉内灌注,并且静脉内灌注和鼻腔灌注后的血浆浓度显示出相似的特征。鼻腔灌注后脑中维拉帕米的浓度是静脉内灌注后的两倍。尽管塔利洛尔在静脉注射后在大脑和脑脊液中输液均低于检出限,经鼻灌注后被检出。当用环孢菌素A治疗大鼠时,两种给药方式后维拉帕米的脑浓度均显着增加,而他尼洛尔的脑浓度未见明显变化。由于他尼洛尔的渗透性低,因此直接从鼻腔转运的脑中的他尼洛尔几乎没有机会被定位在脑微血管内皮细胞顶膜中的P-gp转运。对于P-gp底物,已经证实了通过鼻-CNS途径进行药物递送的潜力。鼻腔输送比静脉输液的优势他尼洛尔向大脑的传递比维拉帕米更重要,这表明与低剂量的P-gp抑制剂相比,鼻腔给药对低渗透性P-gp底物的大脑传递更有用。

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