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Improvement of Pain Relief of Fentanyl Citrate Drug Encapsulated in Nanostructured Lipid Carrier: Drug Formulation, Parameter Optimization, in vitro and in vivo Studies

机译:纳米结构脂质载体中芬太尼柠檬酸盐药物疼痛缓解的改善:药物制剂,参数优化,体外和体内研究

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Introduction: In this study, the encapsulation of fentanyl citrate as an opioid drug with hydrophobic nature in the nanostructured lipid carrier (NLC) is performed. Methods: For encapsulation of fentanyl citrate drug, hot homogenization method is used. The pharmacokinetics of encapsulated fentanyl citrate for pain relief of rats are investigated. The influence of important variables such as the ratio of liquid lipid to the total amount of lipids, surfactant type and concentration on the particle size is investigated using response surface method. Results: Results show that the optimal NLC size is about 90 nm with PDI value around 0.2 and zeta potential of ? 25± 4.01 mV. Characterization analysis of optimal nanostructure shows successful encapsulation of the drug in nanostructure with a spherical morphology of the NLC structure. Results of drug release from commercial fentanyl citrate ampoule and NLC form indicate a control drug release from the NLC within 72 hours in comparison to the commercial ampoule. In vivo studies show that fentanyl citrate-loaded NLC not only has the potential to relieve pain in doses equal to commercial drug but also it can reduce the dose of the drug about 50%. Conclusion: In conclusion, NLC form of fentanyl citrate can increase the efficacy of the drug by appropriate drug distribution in the body and can reduce the risks of overdose.
机译:介绍:在本研究中,进行柠檬酸亚氧化亚锡作为阿片类药物的封装,纳米结构脂质载体(NLC)中具有疏水性质。方法:对于柠檬酸芬太尼药物的封装,使用热均化方法。研究了柠檬酸盐包封的芬太尼的药代动力学,用于大鼠疼痛缓解。研究诸如液体脂质与脂质总量的总脂质,表面活性剂型和粒度浓度的影响,采用响应表面法研究。结果:结果表明,最佳NLC尺寸约为90nm,PDI值约为0.2和Zeta潜力? 25±4.01 mV。最佳纳米结构的表征分析显示了NLC结构的球形形态的纳米结构中药物的成功包封。商业芬太尼柠檬酸亚锡和NLC形式的药物释放结果表明与商业安瓿相比,在72小时内从NLC的对照药物释放。在体内研究表明,柠檬酸芬太尼的NLC不仅有可能缓解等于商业药物的剂量疼痛,而且还可以将药物剂量减少约50%。结论:总之,柠檬酸亚锡的NLC形式可以通过身体中的适当药物分布增加药物的功效,可以降低过量的风险。

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