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载紫杉醇和柚皮素的固体脂质纳米粒经环肽表面修饰后,提高了在多形性胶质母细胞瘤中的肿瘤靶向能力。

Paclitaxel and naringenin-loaded solid lipid nanoparticles surface modified with cyclic peptides with improved tumor targeting ability in glioblastoma multiforme.

机构信息

Department of Neurology, Tangshan Workers' Hospital, Tangshan, Hebei 063000, China.

Department of Oncological Radiotherapy, The People's Hospital of Zhangqiu, No.1920 Huiquan Road, Mingshui, Jinan, Shandong Province 250200, China.

出版信息

Biomed Pharmacother. 2021 Jun;138:111461. doi: 10.1016/j.biopha.2021.111461. Epub 2021 Mar 9.

DOI:10.1016/j.biopha.2021.111461
PMID:33706131
Abstract

The present work describes the systematic development of paclitaxel and naringenin-loaded solid lipid nanoparticles (SLNs) for the treatment of glioblastoma multiforme (GBM). So far only temozolomide therapy is available for the GBM treatment, which fails by large amount due to poor brain permeability of the drug and recurrent metastasis of the tumor. Thus, we investigated the drug combination containing paclitaxel and naringenin for the treatment of GBM, as these drugs have individually demonstrated significant potential for the management of a wide variety of carcinoma. A systematic product development approach was adopted where risk assessment was performed for evaluating the impact of various formulation and process parameters on the quality attributes of the SLNs. I-optimal response surface design was employed for optimization of the dual drug-loaded SLNs prepared by micro-emulsification method, where Percirol ATO5 and Dynasan 114 were used as the solid lipid and surfactant, while Lutrol F188 was used as the stabilizer. Drug loaded-SLNs were subjected to detailed in vitro and in vivo characterization studies. Cyclic RGD peptide sequence (Arg-Gly-Asp) was added to the formulation to obtain the surface modified SLNs which were also evaluated for the particle size and surface charge. The optimized drug-loaded SLNs exhibited particle size and surface charge of 129 nm and 23 mV, drug entrapment efficiency >80% and drug loading efficiency >7%. In vitro drug release study carried out by micro dialysis bag method indicated more than 70% drug was release observed within 8 h time period. In vivo pharmacokinetic evaluation showed significant improvement (p < 0.05) in drug absorption parameters (C and AUC) from the optimized SLNs over the free drug suspension. Cytotoxicity evaluation on U87MG glioma cells indicated SLNs with higher cytotoxicity as compared to that of the free drug suspension (p < 0.05). Evaluation of uptake by florescence measurement indicated superior uptake of SLNs tagged with dye over the plain dye solution. Overall, the dual drug-loaded SLNs showed better chemoprotective effect over the plain drug solution, thus construed superior anticancer activity of the developed nanoformulation in the management of glioblastoma multiforme.

摘要

本工作描述了紫杉醇和柚皮素负载固体脂质纳米粒(SLNs)用于治疗多形性胶质母细胞瘤(GBM)的系统开发。迄今为止,GBM 的治疗仅可采用替莫唑胺疗法,但由于药物在大脑中的渗透性差和肿瘤的复发性转移,该疗法的效果并不理想。因此,我们研究了包含紫杉醇和柚皮素的药物组合用于 GBM 的治疗,因为这些药物在单独使用时都表现出了对多种癌的显著治疗潜力。采用系统产品开发方法,对各种制剂和工艺参数对 SLNs 质量属性的影响进行风险评估。采用 I-最优响应面设计对微乳液法制备的双载药 SLNs 进行优化,其中使用 Percirol ATO5 和 Dynasan 114 作为固体脂质和表面活性剂,Lutrol F188 作为稳定剂。对载药 SLNs 进行了详细的体外和体内特性研究。在配方中添加环肽序列(精氨酸-甘氨酸-天冬氨酸),以获得表面修饰的 SLNs,并对其粒径和表面电荷进行评估。优化后的载药 SLNs 的粒径和表面电荷分别为 129nm 和 23mV,药物包封效率>80%,药物载量效率>7%。通过微透析袋法进行的体外药物释放研究表明,在 8 小时内观察到超过 70%的药物释放。体内药代动力学评价显示,与游离药物混悬液相比,优化后的 SLNs 使药物吸收参数(C 和 AUC)有显著改善(p<0.05)。对 U87MG 神经胶质瘤细胞的细胞毒性评价表明,SLNs 的细胞毒性高于游离药物混悬液(p<0.05)。荧光测量的摄取评估表明,与普通染料溶液相比,标记染料的 SLNs 具有更好的摄取能力。总体而言,与普通药物溶液相比,双载药 SLNs 显示出更好的化学保护作用,因此推断所开发的纳米制剂在管理多形性胶质母细胞瘤方面具有更高的抗癌活性。

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