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PCL-Isocyanate: A New, Degradable. Macromolecular Synthon for the Synthesis of Polymeric Bioconjugates

机译:PCL-异氰酸酯:一种新的,可降解的。高分子合成子合成高分子生物共轭物

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摘要

A new route to poly(epsilon-caprolactone) (PCL) conjugates is described. It is based on successive reactions: the formation of a polycarboxylated PCL via an anionic carboxylation of PCL, the activation of the carboxylic acid group via an acyl chloride group, the conversion of the acyl chloride group to an azide group and finally the formation of an isocyanate group by the Curtius rearrangement. The various steps were monitored using FTIR spectroscopy. To exemplify the potential of the method, isocyanated poly(epsilon-caprolactone) was reacted with UV-absorbing, model, alcohol- and amine-bearing small molecules that were bound to the PCL skeleton via carbamate or urea bonds, respectively. FTIR spectroscopy, SEC with refractometric/photodiode-array double detection, and H-1 NMR spectroscopy were used to assess the effective binding of the drug models on the polymeric backbone. The thermal transitions of the conjugates were characterized using DSC.
机译:描述了一种新的聚(ε-己内酯)(PCL)结合物的方法。它基于以下连续反应:通过PCL的阴离子羧化反应形成多羧化PCL,通过酰氯基团活化羧酸基团,酰氯基团转化为叠氮基团,最后形成异氰酸酯基团经库尔修斯重排。使用FTIR光谱法监测各个步骤。为了证明该方法的潜力,使异氰酸酯化的聚(ε-己内酯)与分别通过氨基甲酸酯或脲键结合到PCL骨架上的吸收紫外线的,模型化的,带有醇和胺的小分子反应。 FTIR光谱,具有折射/光电二极管阵列双重检测的SEC和H-1 NMR光谱用于评估药物模型在聚合物主链上的有效结合。使用DSC表征缀合物的热转变。

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