Cytotoxicity and anti-inflammatory activity of cyclosporine A loaded PLGA nanoparticles for ocular use.

K. Hermans, D. van den Plas, E. Schreurs, W. Weyenberg, A. Ludwig
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引用次数: 11

Abstract

Cyclosporine A loaded poly(lactide-co-glycolide) nanoparticles were prepared using the o/w emulsification solvent evaporation method and the effect of four preparation parameters on particle size and zeta potential was investigated. Release properties of the nanoparticles were examined and in vitro experiments were performed in order to evaluate the cytotoxicity and anti-inflammatory activity of the nanoparticles developed. Particle sizes varied between 191 and 303 nm depending on the different preparation parameters and all nanoparticle dispersions were monodisperse. The nanoparticles showed negative zeta potential values varying between -16 and -35 mV and 57 to 70 % of the amount of loaded cyclosporine A was released after 24 h. None of the nanoparticle formulations showed significant cytotoxicity compared to the negative control using human epithelial cells (HaCaT). Cyclosporine A incorporated in the various nanoparticle formulations retained its anti-inflammatory activity as significant suppression of interleukine-2 secretion in concanavalin A stimulated Jurkat T cells was measured. As the overall influence of the freeze-drying process on the characteristics of nanoparticles was limited, trehalose and carnitine should be preferred as cryoprotectants in ocular formulations for treatment of dry eye disease.
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眼用环孢素A负载PLGA纳米颗粒的细胞毒性和抗炎活性。
采用0 /w乳化溶剂蒸发法制备了负载环孢素A的聚丙交酯-羟基乙酸酯纳米颗粒,考察了4个制备参数对颗粒大小和zeta电位的影响。研究了纳米颗粒的释放特性,并进行了体外实验,以评价纳米颗粒的细胞毒性和抗炎活性。根据不同的制备参数,纳米颗粒的粒径在191 ~ 303 nm之间变化,并且所有的纳米颗粒分散体都是单分散的。纳米颗粒的zeta电位值在-16和-35 mV之间变化,24小时后释放了负载量的57 - 70%的环孢素A。与使用人上皮细胞(HaCaT)的阴性对照相比,没有纳米颗粒制剂显示出显著的细胞毒性。环孢素A掺入到各种纳米颗粒制剂中,其抗炎活性得到了显著抑制,在刀豆蛋白A刺激的Jurkat T细胞中,白细胞介素2的分泌得到了显著抑制。由于冷冻干燥过程对纳米颗粒特性的整体影响有限,因此在治疗干眼病的眼部配方中,海藻糖和肉碱应优先作为冷冻保护剂。
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