Key Laboratory of Functional Polymer Materials, Ministry of Education, and Institute of Polymer Chemistry, Nankai University, Tianjin, People's Republic of China.
Int J Nanomedicine. 2013;8:4229-46. doi: 10.2147/IJN.S51566. Epub 2013 Nov 5.
Polyethylene glycol (PEG)-ylation is a widely used strategy to fabricate nanocarriers with a long blood circulation time. Further elaboration of the contribution of the surface PEGylation pattern to biodistribution is highly desirable. We fabricated a series of polyion complex (PIC) micelles PEGylated with different ratios (PEG2k and PEG550). The plasma protein adsorption, murine macrophage uptake, and in vivo biodistribution with iodine-125 as the tracer were systematically studied to elucidate the impact of PEGylation patterns on the biodistribution of micelles. We demonstrated that the PEGylated micelles with short hydrophilic PEG chains mixed on the surface were cleared quickly by the reticuloendothelial system (RES), and the single PEG2k PEGylated micelles could efficiently prolong the blood circulation time and increase their deposition in tumor sites. The present study extends the understanding of the PEGylation strategy to further advance the development of ideal nanocarriers for drug delivery and imaging applications.
聚乙二醇(PEG)化是一种广泛使用的策略,用于制备具有长血液循环时间的纳米载体。进一步阐述表面 PEG 化模式对生物分布的贡献是非常需要的。我们制备了一系列聚离子复合物(PIC)胶束,用不同比例的 PEG2k 和 PEG550 进行 PEG 化。系统研究了血浆蛋白吸附、小鼠巨噬细胞摄取和体内碘-125 示踪剂的生物分布,以阐明 PEG 化模式对胶束生物分布的影响。我们证明,表面混合有短亲水性 PEG 链的 PEG 化胶束很快被网状内皮系统(RES)清除,而单 PEG2k PEG 化胶束能够有效地延长血液循环时间并增加其在肿瘤部位的沉积。本研究扩展了对 PEG 化策略的理解,以进一步推进用于药物输送和成像应用的理想纳米载体的发展。
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