位置:首页 >化学 >化学(综合) >ACS Nano >Use of a Lipid-Coated Mesoporous Silica Nanoparticle Platform for Synergistic Gemcitabine and Paclitaxel Delivery to Human Pancreatic Cancer in Mice

使用涂脂介孔硅纳米颗粒平台协同给药吉西他滨和紫杉醇对小鼠胰腺癌的抗肿瘤效果

Use of a Lipid-Coated Mesoporous Silica Nanoparticle Platform for Synergistic Gemcitabine and Paclitaxel Delivery to Human Pancreatic Cancer in Mice

作者:Huan Meng;Meiying Wang;Huiyu Liu;Xiangsheng Liu;Allen Situ;Bobby Wu;Zhaoxia Ji;Chong Hyun Chang;Andre E. Nel;

关键词:gemcitabine,paclitaxel,co-delivery,synergy,ratiometric,mesoporous silica nanoparticle,pancreatic cancer

DOI:https://doi.org/10.1021/acsnano.5b00510

发表时间:2015年

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摘要

最近,一种商业白蛋白结合紫杉醇(PTX)纳米载体(Abraxane)被批准作为胰腺导管腺癌近十年来的第一个新药。PTX通过抑制肿瘤基质和抑制GEM失活酶胞嘧啶脱氨酶(CDA)的表达,提高了一线胰腺癌药物吉西他滨(GEM)的药效。因此,我们在胰腺癌中开发了一种介孔硅纳米颗粒(MSNP)载体,以共同传递协同作用的GEM/PTX组合。通过定制设计的包衣脂质膜技术,实现了高药物装载,封装了计算剂量的GEM(40 wt%),利用支持的脂质双分子层(LB)。通过脂质膜的均匀涂覆使65纳米纳米颗粒纳入了少量亲脂性PTX,这可以与GEM一起共同传递到胰腺细胞和肿瘤中。我们证明了我们的LB-MSNP的比例PTX的纳入和传递可以抑制CDA表达,与PTX的协同作用的氧化应激诱导同时发生。为了证明其体内效果,携带皮下PANC-1异种移植瘤的小鼠接受了PTX/GEM-loaded LB-MSNP的静脉注射。药物共同传递提供了比GEM-loaded LB-MSNP、游离GEM或游离GEM加Abraxane更有效的肿瘤萎缩。相当的肿瘤萎缩需要共投12倍的游离Abraxane。肿瘤相关GEM代谢物的高效液相色谱分析证实,与游离GEM相比,MSNP共同传递将磷酸化的DNA互作用GEM代谢物增加了13倍,并将失活和去氨基化代谢物减少了4倍。在PANC-1原位模型中,MSNP传递的PTX/GEM的静脉注射有效地抑制了原发性肿瘤的生长并消除了转移病灶。这种双重传递载体的增强体内效果可以在没有局部或全身毒性的情况下实现。总之,我们展示了一种在胰腺癌中实现PTX/GEM协同传递的有效LB-MSNP纳米载体的开发。


Abstract

Recently, a commercial albumin-bound paclitaxel (PTX) nanocarrier (Abraxane) was approved as the first new drug for pancreatic ductal adenocarcinoma in almost a decade. PTX improves the pharmaceutical efficacy of the first-line pancreatic cancer drug, gemcitabine (GEM), through suppression of the tumor stroma and inhibiting the expression of the GEM-inactivating enzyme, cytidine deaminase (CDA). We asked, therefore, whether it was possible to develop a mesoporous silica nanoparticle (MSNP) carrier for pancreatic cancer to co-deliver a synergistic GEM/PTX combination. High drug loading was achieved by a custom-designed coated lipid film technique to encapsulate a calculated dose of GEM (40 wt %) by using a supported lipid bilayer (LB). The uniform coating of the 65 nm nanoparticles by a lipid membrane allowed incorporation of a sublethal amount of hydrophobic PTX, which could be co-delivered with GEM in pancreatic cells and tumors. We demonstrate that ratiometric PTX incorporation and delivery by our LB-MSNP could suppress CDA expression, contemporaneous with induction of oxidative stress as the operating principle for PTX synergy. To demonstrate the in vivo efficacy, mice carrying subcutaneous PANC-1 xenografts received intravenous (IV) injection of PTX/GEM-loaded LB-MSNP. Drug co-delivery provided more effective tumor shrinkage than GEM-loaded LB-MSNP, free GEM, or free GEM plus Abraxane. Comparable tumor shrinkage required coadministration of 12 times the amount of free Abraxane. High-performance liquid chromatography analysis of tumor-associated GEM metabolites confirmed that, compared to free GEM, MSNP co-delivery increased the phosphorylated DNA-interactive GEM metabolite 13-fold and decreased the inactivated and deaminated metabolite 4-fold. IV injection of MSNP-delivered PTX/GEM in a PANC-1 orthotopic model effectively inhibited primary tumor growth and eliminated metastatic foci. The enhanced in vivo efficacy of the dual delivery carrier could be achieved with no evidence of local or systemic toxicity. In summary, we demonstrate the development of an effective LB-MSNP nanocarrier for synergistic PTX/GEM delivery in pancreatic cancer.


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