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首页> 外文期刊>International Journal of Pharmaceutics >Chitosan/o-carboxymethyl chitosan nanoparticles for efficient and safe oral anticancer drug delivery: In vitro and in vivo evaluation
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Chitosan/o-carboxymethyl chitosan nanoparticles for efficient and safe oral anticancer drug delivery: In vitro and in vivo evaluation

机译:壳聚糖/邻羧甲基壳聚糖纳米颗粒用于有效和安全的口服抗癌药物递送:体外和体内评估

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The present study investigated the ability of a polyelectrolyte complex (CS/CMCS-NPs), composed of chitosan (CS) and o-carboxymeymethy chitosan (CMCS) as a pH responsive carrier for oral delivery of doxorubicin hydrochloride (DOX). The obtained CS/CMCS-NPs were characterized for various parameters including morphology, particle size, zeta potential, entrapment efficiency and stability under the simulated GI tract conditions. The pH responsive stability of the DOX-loaded CS/CMCS nanoparticles (DOX:CS/CMCS-NPs) determined the drug release rate, which was lower in acidic pH than the neutral. Ex vivo intestinal adhesion and permeation indicated DOX:CS/CMCS-NGs were able to enhance absorption of DOX throughout the entire small intestine, especially in jejunum and ileum. Oral administration of DOX:CS/CMCS-NPs was effective to deliver DOX into blood, giving an absolute bioavailability of 42%. The tissue distribution and toxicity of DOX:CS/CMCS-NPs in rats showed low level of DOX in heart and kidney, and obviously decreased cardiac and renal toxicities. These results indicated CS/CMCS-NPs were highly efficient and safe as an oral delivery system for DOX.
机译:本研究调查了由壳聚糖(CS)和邻羧甲基甲基壳聚糖(CMCS)组成的聚电解质复合物(CS / CMCS-NPs)作为pH响应型阿霉素盐酸盐(DOX)的pH响应载体的能力。在模拟的胃肠道条件下,对获得的CS / CMCS-NPs的各种参数进行了表征,包括形态,粒径,ζ电势,包封效率和稳定性。载有DOX的CS / CMCS纳米颗粒(DOX:CS / CMCS-NPs)的pH响应稳定性决定了药物释放速率,该释放速率在酸性pH中低于中性。离体肠粘连和渗透表明DOX:CS / CMCS-NGs能够增强整个小肠对DOX的吸收,尤其是在空肠和回肠中。口服DOX:CS / CMCS-NPs可有效将DOX输送到血液中,绝对生物利用度为42%。大鼠体内DOX:CS / CMCS-NPs的组织分布和毒性显示心脏和肾​​脏中的DOX水平较低,并且明显降低了心脏和肾脏的毒性。这些结果表明,CS / CMCS-NP作为DOX的口服给药系统是高效且安全的。

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