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Drug-Loaded, Bivalent-Bottle-Brush Polymers by Graft-through ROMP

机译:通过移植物宽且曲折的药物装载的二价瓶刷子聚合物

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摘要

Graft through ring-opening metathesis polymerization (ROMP) using ruthenium N heterocyclic carbene catalysts has enabled the synthesis of bottle-brush polymers with unprecedented ease and control Here we report the first bivalent-brush polymers, these materials were prepared by graft through ROMP of drug-loaded poly(ethylene glycol) (PEG) based macromonomers (MMs) Anticancer drugs doxorubicin (DOX) and camptothecin (CT) were attached to a norbornene alkyne-PEG MM via a photocleavable linker ROMP of either or both drug loaded MMs generated brush homo and copolymers with low polydispersities and defined molecular weights. Release of free DOX and CT from these materials was initiated by exposure to 365 nm light All of the CT and DOX polymers were at least 10 fold more toxic to human cancer cells after photoinitiated drug release while a copolymer carrying both CT and DOX displayed 30-fold increased toxicity upon irradiation Graft through ROMP of drug loaded macromonomers provides a general method for the systematic study of structure function relationships for stimuli responsive polymers in biological systems.
机译:使用钌N杂环卡宾催化剂通过开环复分解聚合(ROMP)进行的接枝反应使瓶刷聚合物的合成变得前​​所未有的容易和可控。在这里,我们报道了首批二价刷聚合物,这些材料是通过将药物通过ROMP接枝制备的。载有聚乙二醇(PEG)的大分子单体(MM)将抗癌药阿霉素(DOX)和喜树碱(CT)通过一个或两个载药MM产生的刷均质的光裂解接头ROMP与降冰片烯炔PEG MM连接低多分散性和确定分子量的共聚物。通过暴露在365 nm光线下,从这些材料中释放出游离的DOX和CT,所有这些CT和DOX聚合物在光引发药物释放后对人癌细胞的毒性至少是其十倍,而同时携带CT和DOX的共聚物显示出30-辐照后毒性增加两倍载药大分子单体通过ROMP接枝提供了用于系统研究生物系统中刺激反应性聚合物结构功能关系的一般方法。

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  • 年度 2011
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