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首页> 外文期刊>European Polymer Journal >Comparative study of enzyme-catalyzed biodegradation and crystallization behavior of PCL-PTEGMA amphiphilic hypergraft copolymers
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Comparative study of enzyme-catalyzed biodegradation and crystallization behavior of PCL-PTEGMA amphiphilic hypergraft copolymers

机译:酶催化生物降解和PCL-PTEGMA两亲草锆二氯联合体的结晶行为的比较研究

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摘要

This work aims to systematically elucidate the biodegradation and crystallization behaviors of the model hypergraft systems made of poly(epsilon-caprolactone) (PCL) and poly[tri(ethylene glycol) methyl ether acrylate] (PTEGMA) blocks. A series of hyperbranched PCL (HB-PCLn) with varied subchain lengths were synthesized using AB(2)-type macromonomers with different degrees of polymerization (DPs). The HB-PCLs were grafted with linear PTEGMA chains to prepare amphiphilic hypergraft copolymers (HB-PCLn-g-PTEGMA(m)) to eventually get self-assembled structures through micellization. The DP of PTEGMA was also varied to get two sets of samples with varied sub-chain lengths of the hyperbranched core and the linear corona within each individual set to systematically study the crystallization and biodegradation behaviors of PCL. Differential scanning calorimetric (DSC) measurements of both hypergrafts and linear precursors were compared in order to get insights into the crystallization pattern of PCL. We found that the degree of crystallization in PCL can be controlled from similar to 0 (lowest limit) to similar to 52% (highest limit) by structural regulation. Biodegradation studies were performed in aqueous medium with Lipase from Pseudomonas using dynamic light scattering (DLS). A model was proposed to correlate the sub-chain length of core, the chain length of corona with the biodegradation rate of PCL, which reveals that an increase of PCL content in HB-PCLn-g-PTEGMA(m) increases the crystallinity while decreases the rate of biodegradation in a predictable manner.
机译:该工作旨在系统地阐明由聚(ε-己内酯)(PCL)和聚[三(乙二醇)甲基醚丙烯酸酯](PTEGMA)嵌段制成的模型高血流动系统的生物降解和结晶行为。使用具有不同聚合程度(DPS)的AB(2)型大分子单体合成具有多种子链长的一系列超支化PCL(HB-PCLN)。将Hb-PCLS与线性PTEGMA链接枝以制备两亲血液过度移植共聚物(HB-PCLN-G-PTEGMA(M)),以最终通过胶束进行自组装的结构。 PTEGMA的DP也变化,以获得两组具有超支核心的多种子链长度的样品,并且在每个单独的核心内的线性电晕设置为系统地研究PCL的结晶和生物降解行为。比较差分扫描量热(DSC)对二氯联合物和线性前体的测量,以便在PCL的结晶模式中获得洞察。我们发现,通过结构调节,可以将PCL中的结晶度与0(最低限度)类似于52%(最高限度)。使用动态光散射(DLS),在含水培养基中在水性介质中进行生物降解研究。提出了一种模型来关联核心的子链长度,与PCL的生物降解速率的电晕的链长,显示HB-PCLN-G-PTEGMA(M)中的PCL含量的增加增加了结晶度,同时降低以可预测的方式生物降解率。

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