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Thin-Shelled PEGylated Perfluorooctyl Bromide Nanocapsules for Tumor-Targeted Ultrasound Contrast Agent

机译:薄壳聚乙二醇化全氟辛基溴化物纳米胶囊的肿瘤靶向超声造影剂。

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摘要

Shell thickness determines the acoustic response of polymer-based perfluorooctyl bromide (PFOB) nanocapsule ultrasound contrast agents. PEGylation provides stealth property and arms for targeting moieties. We investigated a modulation in the polymer formulation of carboxy-terminated poly(d,l-lactide-co-glycolide) (PLGA) and poly(d,l-lactide-co-glycolide)-block-polyethylene glycol (PLGA-b-PEG) to produce thin-shelled PFOB nanocapsules while keeping its echogenicity, stealth property, and active targeting potential. Polymer formulation contains 40% PLGA-PEG that yields the PEGylated PFOB nanocapsules of approximately 150 nm size with average thickness-to-radius ratio down to 0.15, which adequately hindered phagocytosis. Functionalization with antibody enables in vitro tumor-specific targeting. Despite the acoustic response improvement, the in vivo tumor accumulation was inadequate to generate an observable acoustic response to the ultrasound power at the clinical level. The use of PLGA and PLGA-PEG polymer blend allows the production of thin-shelled PFOB nanocapsules with echogenicity improvement while maintaining its potential for specific targeting.
机译:壳的厚度决定了基于聚合物的全氟辛基溴(PFOB)纳米胶囊超声造影剂的声学响应。聚乙二醇化为目标部分提供了隐形属性和武器。我们研究了羧基末端聚(d,l-丙交酯-乙交酯)(PLGA)和聚(d,l-丙交酯-乙交酯)-嵌段-聚乙二醇(PLGA-b- PEG)来生产薄壳PFOB纳米胶囊,同时保持其回声性,隐身性和主动靶向潜力。聚合物配方中包含40%的PLGA-PEG,可产生约150μnm大小的PEG化PFOB纳米胶囊,平均厚度/半径比低至0.15,这充分地阻止了吞噬作用。抗体功能化可实现体外肿瘤特异性靶向。尽管声音响应有所改善,但体内肿瘤的积累不足以在临床水平上产生对超声功率的可观察到的声音响应。 PLGA和PLGA-PEG聚合物共混物的使用可以生产具有回声性的薄壳PFOB纳米胶囊,同时保持其潜在的特异性靶向能力。

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