Department of Bioengineering, University of Pennsylvania, Philadelphia, Pennsylvania 19104, United States.
Bioconjug Chem. 2011 Oct 19;22(10):2021-9. doi: 10.1021/bc200214g. Epub 2011 Sep 20.
Block copolymer-based vesicles have recently garnered a great deal of interest as nanoplatforms for drug delivery and molecular imaging applications due to their unique structural properties. These nanovesicles have been shown to direct their cargo to disease sites either through enhanced permeability and retention or even more efficiently via active targeting. Here, we show that the efficacy of nanovesicle targeting can be significantly improved when prepared from polymer-lipid blends compared with block copolymer alone. Polymer-lipid hybrid nanovesicles were produced from the aqueous coassembly of the diblock copolymer, poly(ethylene oxide)-block-polybutadiene (PEO-PBD), and the phospholipid, hydrogenated soy phosphatidylcholine (HSPC). The PEG-based vesicles, 117 nm in diameter, were functionalized with either folic acid or anti-HER2/neu affibodies as targeting ligands to confer specificity for cancer cells. Our results revealed that nanovesicles prepared from polymer-lipid blends led to significant improvement in cell binding compared to nanovesicles prepared from block copolymer alone in both in vitro cell studies and murine tumor models. Therefore, it is envisioned that nanovesicles composed of polymer-lipid blends may constitute a preferred embodiment for targeted drug delivery and molecular imaging applications.
基于嵌段共聚物的囊泡由于其独特的结构特性,最近作为药物传递和分子成像应用的纳米平台引起了极大的兴趣。这些纳米囊泡已被证明可以通过增强的通透性和保留作用,甚至通过更有效的主动靶向作用,将其货物导向疾病部位。在这里,我们表明,与单独使用嵌段共聚物相比,从聚合物-脂质混合物中制备的纳米囊泡的靶向效果可以显著提高。聚合物-脂质混合纳米囊泡是由两亲性嵌段共聚物聚(氧化乙烯)-嵌段-聚丁二烯(PEO-PBD)和磷脂氢化大豆卵磷脂(HSPC)在水相中共组装而成的。基于 PEG 的囊泡直径为 117nm,通过叶酸或抗 HER2/neu affibodies 作为靶向配体进行功能化,以赋予对癌细胞的特异性。我们的结果表明,与单独使用嵌段共聚物制备的纳米囊泡相比,聚合物-脂质混合物制备的纳米囊泡在体外细胞研究和小鼠肿瘤模型中均导致细胞结合显著改善。因此,可以预见,由聚合物-脂质混合物组成的纳米囊泡可能构成靶向药物传递和分子成像应用的首选方案。
