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Ondansetron-loaded chitosan microspheres for nasal antiemetic drug delivery: an alternative approach to oral and parenteral routes.

机译:装载恩丹西酮的壳聚糖微球用于鼻止吐药物的递送:口服和肠胃外途径的另一种方法。

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BACKGROUND: The aim of this study was to develop chitosan microspheres for nasal delivery of ondansetron hydrochloride (OND). METHOD: Microspheres were prepared with spray-drying method using glutaraldehyde as the crosslinking agent. Microspheres were characterized in terms of morphology, particle size, zeta potential, production yield, drug content, encapsulation efficiency, and in vitro drug release. RESULTS: All microspheres were spherical in shape with smooth surface and positively charged. Microspheres had also high encapsulation efficiency and the suitable particle size for nasal administration. In vitro studies indicated that all crosslinked microspheres had a significant burst effect, and sustained drug release pattern was observed until 24 hours following burst drug release. Nasal absorption of OND from crosslinked chitosan microspheres was evaluated in rats, and pharmacokinetic parameters of OND calculated from nasal microsphere administration were compared with those of both nasal and parenteral administration of aqueous solutions of OND. In vivo data also supported that OND-loaded microspheres were also able to attain a sustained plasma profile and significantly larger area under the curve values with respect to nasal aqueous solution of OND. CONCLUSION: Based on in vitro and in vivo data, it could be concluded that crosslinked chitosan microspheres are considered as a nasal delivery system of OND.
机译:背景:这项研究的目的是开发壳聚糖微球用于盐酸恩丹西酮(OND)的鼻腔输送。方法:以戊二醛为交联剂,采用喷雾干燥法制备微球。根据形态,粒度,ζ电势,产量,药物含量,包封效率和体外药物释放来表征微球。结果:所有微球均为球形,表面光滑,带正电。微球还具有高的包封效率和适合鼻腔给药的粒径。体外研究表明,所有交联的微球均具有显着的猝发作用,并且观察到持续的药物释放模式,直到猝发药物释放后24小时为止。在大鼠中评估了从交联的壳聚糖微球在鼻腔中吸收OND的情况,并将通过鼻微球给药计算出的OND的药代动力学参数与经鼻和肠胃外给药的OND水溶液进行了比较。体内数据还支持装载OND的微球相对于OND的鼻腔水溶液也能够获得持续的血浆分布和曲线值下明显更大的面积。结论:基于体外和体内数据,可以得出结论,交联的壳聚糖微球被认为是OND的鼻腔给药系统。

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