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首页> 外文期刊>Biomacromolecules >Degradable Copolymer Nanoparticles from Radical Ring-Opening Copolymerization between Cyclic Ketene Acetals and Vinyl Ethers
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Degradable Copolymer Nanoparticles from Radical Ring-Opening Copolymerization between Cyclic Ketene Acetals and Vinyl Ethers

机译:可降解共聚物纳米颗粒来自环氯烯缩醛和乙烯基醚之间的自由基开环共聚

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摘要

2-Methylene-1,3-dioxepane (MDO) and different vinyl ether (VE) monomers were successfully copolymerized by free-radical radical ring-opening copolymerization (rROP) to yield P(MDO-co-VE) copolymers with M-n = 7 000-13 000 g.mol(-1) and high molar fractions of MDO (F-MDO = 0.7-0.9). By using VE derivatives of different aqueous solubilities or by grafting PEG chains onto the copolymers by "click" chemistry via azide-containing VE units, hydrophobic, amphiphilic and water-soluble copolymers were obtained. The different copolymers were then formulated into nanoparticles by nanoprecipitation using Pluronics for hydrophobic copolymers, without surfactant for amphiphilic copolymers, or blended with PMDO for water-soluble copolymers. Most of the copolymers led to nanoparticles with average diameters in the 130-250 nm with narrow particle size distributions and satisfying colloidal stability for a period of at least 1-2 weeks and up to 6 months. The copolymers were successfully degraded under accelerated, hydrolytic or enzymatic conditions. Hydrophobic copolymers led to degradation kinetics in PBS similar to that of PCL and complete degradation (-95% in M-n decrease) was observed in the presence of enzymes (lipases). Preliminary cytotoxicity assays were performed on endothelial cells (HUVEC) and macrophages (J774.A1) and revealed high cell viabilities at 0.1 mg-mL(-1).
机译:通过自由基自由基开环共聚(RROP)成功共聚2-亚甲基-1,3-二氧烯(MDO)和不同的乙烯基醚(Ve)单体,得到P(MDO-CO-VE)与Mn = 7的共聚物000-13 000 G.MOL(-1)和MDO的高摩尔分数(F-MDO = 0.7-0.9)。通过使用不同水溶性的VE衍生物或通过通过含叠氮化物的VE单元,疏水,两亲性和水溶性共聚物将PEG链移植到共聚物上。然后使用Pluronics使用Pluronics用于疏水性共聚物的Purronics将不同的共聚物配制成纳米粒子,没有用于两亲共聚物的表面活性剂,或与PMDO混合用于水溶性共聚物。大多数共聚物导致纳米颗粒,在130-250nm中具有平均直径,粒径窄,胶体稳定性至少为1-2周,最多6个月。在加速,水解或酶促条件下成功降解共聚物。在酶(脂肪酶)存在下观察到与PCL类似的PBS中的疏水性共聚物导致与PCL的降解动力学相似,并在酶(脂肪酶)存在下观察到的完全降解(M-N减少)。在内皮细胞(HUVEC)和巨噬细胞(J774.A1)上进行初步细胞毒性测定,并揭示了0.1mg-mL(-1)的高细胞活性。

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  • 来源
    《Biomacromolecules》 |2019年第1期|共13页
  • 作者单位

    Univ Paris Saclay Univ Paris Sud Fac Pharm Inst Galien Paris Sud UMR CNRS 8612 5 Rue Jean Baptiste Clement F-92296 Chatenay Malabry France;

    Univ Paris Saclay Univ Paris Sud Fac Pharm Inst Galien Paris Sud UMR CNRS 8612 5 Rue Jean Baptiste Clement F-92296 Chatenay Malabry France;

    Univ Paris Saclay Univ Paris Sud Fac Pharm Inst Galien Paris Sud UMR CNRS 8612 5 Rue Jean Baptiste Clement F-92296 Chatenay Malabry France;

    Aix Marseille Univ CNRS Inst Chim Radicalaire UMR 7273 F-13397 Marseille France;

    Aix Marseille Univ CNRS Inst Chim Radicalaire UMR 7273 F-13397 Marseille France;

    Aix Marseille Univ CNRS Inst Chim Radicalaire UMR 7273 F-13397 Marseille France;

    Univ Paris Saclay Univ Paris Sud Fac Pharm Inst Galien Paris Sud UMR CNRS 8612 5 Rue Jean Baptiste Clement F-92296 Chatenay Malabry France;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 分子生物学;
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