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粒子在行动:纳米多孔聚合物粒子的细胞内运输和不对称有丝分裂分配。

Particles on the move: intracellular trafficking and asymmetric mitotic partitioning of nanoporous polymer particles.

机构信息

Department of Chemical and Biomolecular Engineering, The University of Melbourne, Parkville, Victoria 3010, Australia.

出版信息

ACS Nano. 2013 Jun 25;7(6):5558-67. doi: 10.1021/nn401800u. Epub 2013 May 28.

DOI:10.1021/nn401800u
PMID:23713907
Abstract

Nanoporous polymer particles (NPPs) prepared by mesoporous silica templating show promise as a new class of versatile drug/gene delivery vehicles owning to their high payload capacity, functionality, and responsiveness. Understanding the cellular dynamics of such particles, including uptake, intracellular trafficking, and distribution, is an important requirement for their development as therapeutic carriers. Herein, we examine the spatiotemporal map of the cellular processing of submicrometer-sized disulfide-bonded poly(methacrylic acid) (PMASH) NPPs in HeLa cells using both flow cytometry and fluorescence microscopy. The data show that the PMASH NPPs are transported from the early endosomes to the lysosomes within a few minutes. Upon cell division, the lysosome-enclosed PMASH NPPs are distributed asymmetrically between two daughter cells. Statistical analysis of cells during cytokinesis suggests that partitioning of particles is biased with an average segregation deviation of 60%. Further, two-dimensional difference gel electrophoresis (2D-DIGE) analysis reveals that 127 out of 3059 identified spots are differentially regulated upon exposure to the PMASH NPPs. Pathway analysis of the proteomics data suggests that ubiquitylation, a reversible modification of cellular proteins with ubiquitin, plays a central role in overall cellular responses to the particles. These results provide important insights into the cellular dynamics and heterogeneity of NPPs, as well as the mechanisms that regulate the motility of these particles within cells, all of which have important implications for drug susceptibility characteristics in cancer cells using particle-based carriers.

摘要

介孔硅模板制备的纳米多孔聚合物颗粒(NPPs)由于其高载药能力、多功能性和响应性,有望成为一类新型的多功能药物/基因传递载体。了解这些颗粒的细胞动力学,包括摄取、细胞内运输和分布,是将其开发为治疗载体的重要要求。在此,我们使用流式细胞术和荧光显微镜研究了亚微米级二硫键键合的聚(甲基丙烯酸)(PMASH)NPP 在 HeLa 细胞中的细胞处理的时空图谱。数据表明,PMASH NPP 可在几分钟内从早期内体转运到溶酶体。在细胞分裂过程中,溶酶体封闭的 PMASH NPP 不均匀地分布在两个子细胞之间。有丝分裂过程中细胞的统计分析表明,粒子的分配具有偏倚性,平均分离偏差为 60%。此外,二维差异凝胶电泳(2D-DIGE)分析表明,在暴露于 PMASH NPP 后,3059 个鉴定斑点中有 127 个发生差异调节。蛋白质组学数据分析的途径分析表明,泛素化,即细胞蛋白的可逆修饰,在颗粒对细胞的整体反应中起着核心作用。这些结果为 NPP 的细胞动力学和异质性以及调节这些颗粒在细胞内运动的机制提供了重要的见解,这对于使用基于颗粒的载体的癌细胞中的药物敏感性特征具有重要意义。

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