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Synthesis and in vivo pharmacokinetic evaluation of degradable shell cross-linked polymer nanoparticles with poly(carboxybetaine) versus poly(ethylene glycol) surface-grafted coatings

机译:具有聚羧基甜菜碱与聚乙二醇表面接枝涂层的可降解壳交联聚合物纳米粒子的合成及体内药代动力学评价

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摘要

Nanoparticles with tunable pharmacokinetics are desirable for various biomedical applications. Poly(ethylene glycol) (PEG) is well-known to create "stealth" effects to stabilize and extend the blood circulation of nanoparticles. In this work, poly(carboxybetaine) (PCB), a new nonfouling polymer material, was incorporated as surface-grafted coatings, conjugated onto degradable shell cross-linked knedel-like nanoparticles (dSCKs) composed of poly(acrylic acid)-based shells and poly(lactic acid) cores, to compare the in vivo pharmacokinetics to their PEG-functionalized analogues. A series of five dSCKs was prepared from amphiphilic block copolymers, having different numbers and lengths of either PEG or PCB grafts, by supramolecular assembly in water followed by shell cross-linking, and then studied by a lactate assay to confirm their core hydrolytic degradabilities. Each dSCK was also conjugated with 1,4,7,10-tetraazacyclododecane-1,4,7,10-tetraacetic acid macrocyclic chelators and tyramine moieties to provide for~ (64)Cu and/or radiohalogen labeling. The high specific activity of~ (64)Cu radiolabeling ensured nanogram administration of dSCKs for in vivo evaluation of their pharmacokinetics. Biodistribution studies demonstrated comparable in vivo pharmacokinetic profiles of PCB-grafted dSCKs to their PEG-conjugated counterparts. These results indicated that PCB-functionalized dSCKs have great potential as a theranostic platform for translational research.
机译:具有可调药代动力学的纳米颗粒是各种生物医学应用所需要的。众所周知,聚乙二醇(PEG)具有“隐形”效果,可以稳定和延长纳米颗粒的血液循环。在这项工作中,聚(羧基甜菜碱)(PCB),一种新的防污聚合物材料,作为表面接枝涂料被掺入,并共轭到可降解的壳交联的类似聚苯胺的纳米颗粒(dSCKs)上,该纳米颗粒由基于聚丙烯酸的壳组成和聚乳酸核心,以将体内药代动力学与其PEG官能化类似物进行比较。由具有不同数目和长度的PEG或PCB接枝物的两亲嵌段共聚物,通过在水中的超分子组装,然后进行壳交联,制备一系列五个dSCK,然后通过乳酸盐测定法进行研究,以确认其核心水解降解能力。每个dSCK还与1,4,7,10-四氮杂环十二烷-1,4,7,10-四乙酸大环螯合剂和酪胺部分缀合以提供〜(64)Cu和/或放射性卤素标记。 〜(64)Cu放射性标记的高比活度确保了dSCK的纳克级给药,可用于体内评估其药代动力学。生物分布研究表明,PCB接枝的dSCKs的体内药代动力学特征与PEG缀合的对应物相当。这些结果表明,PCB功能化的dSCK作为翻译研究的治疗论平台具有巨大潜力。

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