首页> 外文期刊>International Journal of Nanomedicine >Dual-drug nanomedicine with hydrophilic F127-modified magnetic nanocarriers assembled in amphiphilic gelatin for enhanced penetration and drug delivery in deep tumor tissue
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Dual-drug nanomedicine with hydrophilic F127-modified magnetic nanocarriers assembled in amphiphilic gelatin for enhanced penetration and drug delivery in deep tumor tissue

机译:双药纳米胺,具有亲水性F127-改性的磁性纳米载体,组装在两亲性明胶中,用于增强深肿瘤组织中的渗透和药物递送

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Introduction: Deep penetration of large-sized drug nanocarriers into tumors is important to improve the efficacy of tumor therapy. Methods: In this study, we developed a size-changeable “Trojan Horse” nanocarrier (THNC) composed of paclitaxel (PTX)-loaded Greek soldiers (GSs; ~20 nm) assembled in an amphiphilic gelatin matrix with hydrophilic losartan (LST) added. Results: With amphiphilic gelatin matrix cleavage by matrix metalloproteinase-2, LST showed fast release of up to 60% accumulated drug at 6 h, but a slow release kinetic (~20%) was detected in the PTX from the GSs, indicating that THNCs enable controllable release of LST and PTX drugs for penetration into the tumor tissue. The in vitro cell viability in a 3D tumor spheroid model indicated that the PTX-loaded GSs liberated from THNCs showed deeper penetration as well as higher cytotoxicity, reducing a tumor spheroid to half its original size and collapsing the structure of the tumor microenvironment. Conclusion: The results demonstrate that the THNCs with controlled drug release and deep penetration of magnetic GSs show great potential for cancer therapy.
机译:简介:大型药物纳米载体的深入渗透到肿瘤中是重要的,以提高肿瘤治疗的功效。方法:在本研究中,我们开发了一种尺寸可变的“特洛伊木马”纳米载波(THNC),由PACLITAXEL(PTX) - 加载的希腊士兵(GSS;〜20nm)组成,组装在含有亲水性氯沙坦(LST)的两亲性明胶基质中组合。结果:通过基质金属蛋白酶-2,LST在6小时内显示出快速释放多达60%的累积药物,但在GSS的PTX中检测缓慢释放动力学(〜20%),表明THNCS使LST和PTX药物的可控释放用于渗透到肿瘤组织中。 3D肿瘤球体模型中的体外细胞活力表明,从THNC释放的PTX负载GSS显示出更深的渗透和更高的细胞毒性,将肿瘤球体降低到其原始尺寸的一半并塌陷肿瘤微环境的结构。结论:结果表明,具有受控药物释放和磁性GSS深度渗透的THNC表现出癌症治疗的巨大潜力。

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