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Injectable phenytoin loaded polymeric microspheres for the control of temporal lobe epilepsy in rats

机译:注射苯妥英钠负载的聚合物微球用于控制大鼠颞叶癫痫

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摘要

Epilepsy is a prevalent neurological disorder with a high frequency of drug resistance. While significant advancements have been made in drug delivery systems to overcome anti-epileptic drug resistance, efficacies of materials in biological systems have been poorly studied. The purpose of the study was to evaluate the anti-epileptic effects of injectable poly(epsiloncaprolactone) (PCL) microspheres for controlled release of an anticonvulsant, phenytoin (PHT), in an animal model of epilepsy. Methods: PHT-PCL and Blank-PCL microspheres formulated using an oil-in-water (O/W) emulsion solvent evaporation method were evaluated for particle size, encapsulation efficiency, surface morphology and in-vitro drug release profile. Microspheres with the most suitable morphology and release characteristics were subsequently injected into the hippocampus of a rat tetanus toxin model of temporal lobe epilepsy. Electrocorticography (ECoG)from the cerebral cortex were recorded for all animals. The number of seizure events, severity of seizures, and seizure duration were then compared between the two treatment groups. Results: We have shown that small injections of drug-loaded microspheres are biologically tolerated and released PHT can control seizures for the expected period of time that is in accord with in-vitro release data. Conclusion: The study demonstrated the feasibility of polymer-based delivery systems in controlling focal seizures.
机译:癫痫病是一种普遍的神经系统疾病,耐药性高发。尽管在药物输送系统中已经取得了很大的进步,以克服抗癫痫药的耐药性,但生物系统中材料的功效研究却很少。该研究的目的是评估可注射的聚ε-己内酯(PCL)微球在癫痫动物模型中控制释放的抗惊厥药苯妥英(PHT)的抗癫痫作用。方法:使用水包油(O / W)乳剂溶剂蒸发法配制的PHT-PCL和Blank-PCL微球的粒径,包封效率,表面形态和体外药物释放曲线均经过评估。随后将具有最合适的形态和释放特性的微球注射到颞叶癫痫大鼠破伤风毒素模型的海马中。记录所有动物的大脑皮层的脑电图(ECoG)。然后比较两个治疗组的癫痫发作次数,癫痫发作严重程度和癫痫发作持续时间。结果:我们已经表明,小剂量载药微球的注射具有生物学耐受性,释放的PHT可以在预期的时间内控制癫痫发作,这与体外释放数据一致。结论:该研究证明了基于聚合物的递送系统在控制局灶性癫痫发作中的可行性。

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