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Tracking and quantifying polymer therapeutic distribution on a cellular level using 3D dSTORM

机译:使用3D dSTORM在细胞水平上跟踪和量化聚合物治疗分布

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摘要

We used a single-molecule localization technique called direct stochastic optical reconstruction microscopy (dSTORM) to quantify both colocalization and spatial distribution on a cellular level for two conceptually different N-(2-hydroxypropyl)methacrylamide (HPMA) copolymer conjugates. Microscopy images were acquired of entire cells with resolutions as high as 25 nm revealing the nanoscale distribution of the fluorescently labeled therapeutic components. Drug-free macromolecular therapeutics consisting of two self-assembling nanoconjugates showed slight increase in nanoclusters on the cell surface with time. Additionally, dSTORM provided high resolution images of the nanoscale organization of the self-assembling conjugates at the interface between two cells. A conjugate designed for treating ovarian cancer showed that the model drug (Cy3) and polymer bound to Cy5 were colocalized at an early time point before the model drug was enzymatically cleaved from the polymer. Using spatial descriptive statistics it was found that the drug was randomly distributed after 24 h while the polymer bound dye remained in clusters. Four different fluorescent dyes were used and two different therapeutic systems were tested to demonstrate the versatility and possible general applicability of dSTORM for use in studying drug delivery systems.
机译:我们使用一种称为直接随机光学重建显微镜(dSTORM)的单分子定位技术在两个概念上不同的N-(2-羟丙基)甲基丙烯酰胺(HPMA)共聚物共轭物的细胞水平上量化共定位和空间分布。以高达25 nm的分辨率获取整个细胞的显微镜图像,揭示了荧光标记的治疗成分的纳米级分布。由两种自组装的纳米共轭物组成的无药物大分子疗法显示,随着时间的推移,细胞表面的纳米团簇略有增加。此外,dSTORM在两个细胞之间的界面处提供了自组装结合物的纳米级组织的高分辨率图像。设计用于治疗卵巢癌的缀合物显示,在从聚合物酶促裂解模型药物之前,模型药物(Cy3)和与Cy5结合的聚合物在早期被共定位。使用空间描述统计,发现该药物在24小时后随机分布,而聚合物结合的染料仍保持簇状。使用了四种不同的荧光染料,并测试了两种不同的治疗系统,以证明dSTORM的多功能性和可能的​​普遍适用性,用于研究药物输送系统。

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