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首页> 外文期刊>Colloids and Surfaces, B. Biointerfaces >Honokiol nanosuspensions: Preparation, increased oral bioavailability and dramatically enhanced biodistribution in the cardio-cerebro-vascular system
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Honokiol nanosuspensions: Preparation, increased oral bioavailability and dramatically enhanced biodistribution in the cardio-cerebro-vascular system

机译:厚朴酚纳米悬浮液:制备,增加的口服生物利用度和在心脑血管系统中的生物分布显着增强

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摘要

Honokiol is a phytochemical component with multiple pharmacological activities, but Honokiol's wider use has been restricted by its poor solubility. Using bovine serum albumin and polyvinylpyrrolidone as stabilisers in a solvent precipitation-ultrasonication method, Honokiol nanosuspensions were prepared with a mean particle size of 116.2 nm (±2nm), a zeta potential of -44.7 mV (±1.7 mV) and a high drug payload of 50.4 ± 0.6% (w/w). X-ray powder diffraction and differential scanning calorimetry indicated that Honokiol was in an amorphous state in the nanosuspensions, in contrast with bulk Honokiol powder. Honokiol was released faster in vitro from nanosuspensions with no burst release, and the highest 98% cumulative release was after 60 h. Honokiol nanosuspensions improved the oral bioavailability of Honokiol in in vivo studies in rats with a 3.94-fold C_(max) and a 2.2-fold AUC_((0-t)). Remarkably, in contrast to oral administration, intraperitoneal administration of Honokiol nanosuspensions could dramatically alter the biodistribution of Honokiol, resulting in a much higher drug level and tissue bioavailability in the blood, heart and brain, benefitting the treatment of cardio-cerebro-vascular diseases.
机译:厚朴酚是一种具有多种药理活性的植物化学成分,但是厚朴酚的广泛使用受到其不良溶解性的限制。使用牛血清白蛋白和聚乙烯吡咯烷酮作为溶剂沉淀-超声法中的稳定剂,制得厚朴酚纳米悬浮液,其平均粒径为116.2 nm(±2 nm),ζ电位为-44.7 mV(±1.7 mV),药物有效载荷高为50.4±0.6%(w / w)。 X射线粉末衍射和差示扫描量热法表明,厚朴酚粉与厚朴酚粉相反,厚朴酚在纳米悬浮液中处于非晶态。厚朴酚在体外从纳米悬浮液中释放得更快,没有爆发释放,最高的98%累积释放是在60小时后。厚朴酚纳米悬浮液在大鼠体内研究中,厚朴酚的口服生物利用度提高了3.94倍C_(max)和2.2倍AUC _((0-t))。值得注意的是,与口服给药相比,厚朴酚纳米悬浮液的腹膜内给药可以显着改变厚朴酚的生物分布,从而导致血液,心脏和大脑中更高的药物水平和组织生物利用度,从而有益于心脑血管疾病的治疗。

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