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Optimisation of chloroquine phosphate loaded nanostructured lipid carriers using Box–Behnken design and its antimalarial efficacy

机译:用Box-Behnken设计优化氯喹磷酸氯化纳米结构脂质携带者及其抗疟药性能

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Chloroquine was once the most widely used antimalarial for nearly eight decades for its safety, efficiency, stability, low cost and finally for its less toxic nature. But its use and efficacy got slowly decreased with the increase of chloroquine resistant strains of Plasmodium species throughout the world. Lipid based nanodrug delivery systems have been very popular in the recent times as they are very less toxic, have drug targeting capabilities and also reduces the dosing frequency by increasing efficacy of the drug. In the present research work, response surface methodology was employed to optimise chloroquine phosphate (CQ) loaded nanostructured lipid carriers (NLCs) using a modified double emulsion technique. The optimised CQ loaded NLC showed a particle size of 66.50 ± 1.21 nm, PDI of 0.210 ± 0.016, ZP of +38.4 ± 1.44 and EE of 78.2 ± 1.2%, respectively. The in vitro and in vivo antimalarial studies of CQ loaded NLCs showed an enhanced antimalarial efficacy of the nanoformulation with a better suppression of parasitemia and with an increased efficacy of more than 23% in comparison to pure drug. This study demonstrated that by loading a drug into an NLCs system can help in overcoming the problems associated with the present antimalarials available. ? 2017 Informa UK Limited, trading as Taylor & Francis Group.
机译:氯喹是一旦其安全,效率,稳定性,低成本近八十年的最广泛使用的抗疟情况。但它的使用和功效随着世界各地的疟原虫物种的氯喹抗性菌株的增加而缓慢下降。基于脂质的纳米树脂递送系统在近期在近期非常受欢迎,因为它们非常不那么含量较小,具有药物靶向能力,并且通过提高药物的功效来降低给药频率。在本研究工作中,使用响应面方法使用改性的双乳液技术优化氯喹磷酸盐(CQ)负载的纳米结构脂质载体(NLC)。优化的CQ加载的NLC显示粒度为66.50±1.21nm,PDI为0.210±0.016,ZP分别为78.2±1.2%。对CQ负载的NLC的体外和体内抗疟性研究表明,与纯药物相比,占血症患者的抑制性和抑制血症的疗效增加超过23%的疗效增强了抗疟药。该研究表明,通过将药物加载到NLCS系统中,系统可以有助于克服与​​现有抗疟情况相关的问题。还2017年Informa UK Limited,贸易为泰勒&弗朗西斯集团。

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