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用于评价埃达福林脂质纳米粒肠道吸收的体外肠共培养细胞模型。

In vitro intestinal co-culture cell model to evaluate intestinal absorption of edelfosine lipid nanoparticles.

机构信息

Department of Pharmaceutics and Pharmaceutical Technology, School of Pharmacy, University of Navarra, C/Irunlarrea 1, E-31080 Pamplona, Spain.

出版信息

Curr Top Med Chem. 2014;14(9):1124-32. doi: 10.2174/1568026614666140329225340.

Abstract

Nanotechnology is providing a new therapeutic paradigm by enhancing drug efficacy and preventing side-effects. Edelfosine is a synthetic ether lipid analogue of platelet activating factor with high antitumor activity. The encapsulation of this potent antitumor drug in lipid nanoparticles increases its oral bioavailability; moreover, it prevents the hemolytic and gastrointestinal side-effects of the free drug. The literature points towards lymphatic absorption of lipid nanoparticles after oral administration, and previous in vitro and in vivo studies stress the protection against toxicity that these nanosystems provide. The present study is intended to assess the permeability of lipid nanoparticles across the intestinal barrier. Caco-2 monoculture and Caco-2/Raji co-culture were used as in vitro models of enterocytes and Microfold cells respectively. Results showed that free drug is internalized and possibly metabolized in enterocytes. These results do not correlate with those observed in vivo when edelfosine-lipid nanoparticles were administered orally in mice, which suggests that the microfold model is not a good model to study the absorption of edelfosine-lipid nanoparticles across the intestinal barrier in vitro.

摘要

纳米技术通过提高药物疗效和预防副作用,提供了一种新的治疗范例。埃德尔福辛是血小板激活因子的合成醚脂类似物,具有很高的抗肿瘤活性。将这种强效抗肿瘤药物包封在脂质纳米粒中可以提高其口服生物利用度;此外,还可以防止游离药物的溶血和胃肠道副作用。文献指出,脂质纳米粒经口服给药后会被淋巴吸收,以前的体外和体内研究强调了这些纳米系统提供的毒性保护作用。本研究旨在评估脂质纳米粒穿过肠屏障的通透性。Caco-2 单层培养和 Caco-2/Raji 共培养分别用作肠细胞和微褶皱细胞的体外模型。结果表明,游离药物在肠细胞内被内化并可能被代谢。这些结果与埃德尔福辛脂质纳米粒在小鼠口服给药时在体内观察到的结果不一致,这表明微褶皱模型不是体外研究埃德尔福辛脂质纳米粒穿过肠屏障吸收的良好模型。

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