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聚乙二醇化聚氨基酸封端介孔硅纳米粒用于榄香烯在实体瘤中靶向线粒体的递送

PEGylated polyaminoacid-capped mesoporous silica nanoparticles for mitochondria-targeted delivery of celastrol in solid tumors.

机构信息

College of Pharmacy, Yeungnam University, 214-1, Dae-dong, Gyeongsan, 712-749, South Korea.

Department of Pharmaceutical Engineering, Dankook University, 119 Dandae-ro, Cheonan, 31116, South Korea.

出版信息

Colloids Surf B Biointerfaces. 2018 May 1;165:56-66. doi: 10.1016/j.colsurfb.2018.02.015. Epub 2018 Feb 11.

DOI:10.1016/j.colsurfb.2018.02.015
PMID:29453086
Abstract

The major goal of cancer chemotherapy is to maximize the therapeutic efficacy of anticancer drugs, while minimizing their associated side effects. Celastrol (CST), which is extracted from the traditional Chinese medicinal plant Tripterygium wilfordii, has been reported to exhibit significant anticancer effects in various in vitro and in vivo cancer models. Nanoparticulate drug delivery systems could be employed to preserve and enhance the pharmacological effects of CST in cancer cells. Among these, mesoporous silica nanoparticles (MSNs) are one of the most promising drug delivery systems. MSNs possess the capability of passive accumulation within solid tumors, and could efficiently transport anticancer drugs to such tumors in a site-specific manner. In this study, PEGylated polyaminoacid-capped CST-loaded MSN (CMSN-PEG) showed controlled in vitro drug release behavior, and exhibited high in vitro cytotoxicity in different cancer cells. Compared to treatment with free CST, treatment with CMSN-PEG resulted in the increased expression of the apoptosis protein HIF-1α and proteins corresponding to mitochondrial apoptosis pathway. Importantly, CMSN-PEG remarkably reduced tumor burden with no toxicity to healthy cells in the SCC7 tumor-bearing xenograft model. Our results clearly demonstrate a promising potential of CMSN-PEG for the treatment of solid tumors.

摘要

癌症化疗的主要目标是最大限度地提高抗癌药物的治疗效果,同时最大限度地降低其相关副作用。从传统中药雷公藤中提取的雷公藤红素(CST)已被报道在各种体外和体内癌症模型中具有显著的抗癌作用。纳米药物递送系统可用于保护和增强 CST 在癌细胞中的药理作用。其中,介孔硅纳米粒子(MSNs)是最有前途的药物递送系统之一。MSNs 具有在实体瘤中被动积累的能力,并能够以特定部位的方式将抗癌药物高效地输送到这些肿瘤中。在这项研究中,PEG 化聚氨基酸封端 CST 负载的 MSN(CMSN-PEG)表现出可控的体外药物释放行为,并在不同的癌细胞中表现出高体外细胞毒性。与游离 CST 治疗相比,用 CMSN-PEG 治疗导致凋亡蛋白 HIF-1α 和线粒体凋亡途径相关蛋白的表达增加。重要的是,CMSN-PEG 在 SCC7 荷瘤异种移植模型中显著降低了肿瘤负担,而对健康细胞没有毒性。我们的研究结果清楚地表明,CMSN-PEG 具有治疗实体瘤的巨大潜力。

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