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Polydopamine-Based Surface Modification of Novel Nanoparticle-Aptamer Bioconjugates for In Vivo Breast Cancer Targeting and Enhanced Therapeutic Effects

机译:基于聚多巴胺的新型纳米粒子-适体生物共轭物的表面修饰,用于体内乳腺癌靶向和增强的治疗效果

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In this study, we reported a simple polydopamine (pD)-based surface modification method to prepare novel nanoparticle-aptamer bioconjugates (Apt-pD-DTX/NPs) for in vivo tumor targeting and enhanced therapeutic effects of breast cancer. With simple preparation procedures, the new functionalized Apt-pD-DTX/NPs could maximumly increase the local effective drug concentration on tumor sites, achieving enhanced treatment effectiveness and minimizing side effects. The dopamine polymerization and aptamer conjugation barely changed the characters of NPs. Both in vitro cell experiments (i.e. endocytosis of fluorescent NPs, in vitro cellular targeting and cytotoxicity assays) and in vivo animal studies (i.e. in vivo imaging, biodistribution and antitumor effects of NPs) demonstrated that the Apt-pD-DTX/NPs could achieve significantly high targeting efficiency and enhanced therapeutic effects compared with clinical Taxotere? and NPs without functional modification. Above all, the Apt-pD-DTX/NPs showed great potential as a promising nanoformulation for in vivo breast cancer therapy and the construction of pD-modified NP-aptamer bioconjugates could be of great value in medical use.
机译:在这项研究中,我们报道了一种简单的基于聚多巴胺(pD)的表面修饰方法,以制备新型纳米粒子-适体生物共轭物(Apt-pD-DTX / NPs),用于体内靶向肿瘤和增强乳腺癌的治疗效果。通过简单的制备程序,新的功能化Apt-pD-DTX / NPs可以最大程度地增加肿瘤部位的局部有效药物浓度,从而提高治疗效果并将副作用最小化。多巴胺的聚合和适体的共轭几乎没有改变NP的特性。体外细胞实验(即荧光NP的内吞作用,体外细胞靶向和细胞毒性测定)和体内动物研究(即NP的体内成像,生物分布和抗肿瘤作用)均证明Apt-pD-DTX / NPs可以达到与临床上没有功能修饰的Taxotere ?和NPs相比,靶向作用显着提高,治疗效果增强。最重要的是,Apt-pD-DTX / NPs作为体内乳腺癌治疗的有前途的纳米制剂显示出巨大的潜力,pD修饰的NP-适体生物共轭物的构建在医学上可能具有重要的价值。

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