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甲氨蝶呤载壳聚糖基水凝胶纳米粒用于中枢神经系统药物递送的机制研究:是否存在特洛伊木马效应?

A mechanistic investigation on methotrexate-loaded chitosan-based hydrogel nanoparticles intended for CNS drug delivery: Trojan horse effect or not?

机构信息

Pharmaceutical Sciences Research Center, Shiraz University of Medical Sciences, Shiraz, Iran.

Department of Pharmaceutics, School of Pharmacy, Shiraz University of Medical Sciences, Shiraz, Iran.

出版信息

Int J Biol Macromol. 2019 Mar 15;125:785-790. doi: 10.1016/j.ijbiomac.2018.12.093. Epub 2018 Dec 10.

Abstract

Chitosan-based hydrogel nanoparticles provide a higher brain concentration of methotrexate (MTX) following IV administration in comparison with the drug's simple solution. The present study investigates the mechanism of this phenomenon, focusing on the possible role of P-gp. A previously developed MTX containing chitosan nanogel was fabricated and characterised. Then 48 rats were divided into four groups: two receiving nanogels and two receiving solution of MTX, while 1 of each two had received a verapamil dose 30 min before MTX. Then, rats were sacrificed in four time points in triplicate, and MTX concentration in their plasma and brains were quantified and were compared statistically. Following IV injection, spherical nanogels with a mean diameter of <200 nm, zeta potential of 22.8 ± 6.55 mv, Loading efficiency of 72.03 ± 0.85, and loading capacity of 1.41 ± 0.02 produce a significantly higher brain concentration compared with the simple solution. Furthermore, those receiving verapamil presented a higher brain concentration. It seems that in the short term after drug administration (<1 h) nanogels facilitate MTX passage by providing a higher concentration of drug in contact with BBB, but in a more extended period nanogels pass the BBB and release their content beyond that.

摘要

壳聚糖基水凝胶纳米颗粒经静脉给药后,与药物的简单溶液相比,可使甲氨蝶呤(MTX)在大脑中的浓度更高。本研究探讨了这一现象的机制,重点研究了 P-糖蛋白(P-gp)的可能作用。我们制备并表征了一种先前开发的含有壳聚糖纳米凝胶的 MTX。然后,将 48 只大鼠分为四组:两组接受纳米凝胶,两组接受 MTX 溶液,其中每组的 1 只在给予 MTX 前 30 分钟接受维拉帕米剂量。然后,在四个时间点以三倍重复的方式处死大鼠,并对其血浆和大脑中的 MTX 浓度进行定量,并进行统计学比较。与简单溶液相比,静脉注射后,平均直径<200nm、Zeta 电位为 22.8±6.55mV、载药效率为 72.03±0.85%、载药能力为 1.41±0.02%的球形纳米凝胶可显著提高大脑中的浓度。此外,那些接受维拉帕米的大鼠的大脑浓度更高。似乎在药物给药后短期内(<1 小时),纳米凝胶通过提供与 BBB 接触的更高药物浓度来促进 MTX 的传递,但在更长的时间内,纳米凝胶通过 BBB 并释放其内容物。

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