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Influence of molecular weight on kinetics release of metronidazole from proline-based polymers prepared by RAFT polymerization

机译:分子量对筏衍生脯氨酸基聚合物动力学释放的影响

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In the current study, the influence of polymer molecular weight on the release of metronidazole (MTZ) as a drug model from synthesized proline-based polymers was studied. Using reversible-addition fragmentation chain transfer (RAFT) polymerization, amino acid-based polymers based on N-acryloyl-L-proline (A-L-Pro-OH) with various molecular weights were prepared with relatively high conversions (55-98%, as measured by H-1 NMR spectroscopy). The polymerization process was done at different ratios of [monomer](0)/[CTA](0)/[AIBN](0). Proline-based polymers with pre-determined molecular weights (M-n = 6000-22 600 in methylated forms) and low polydispersities (M-w/M-n = 1.30-1.37) were utilized for the immobilization of metronidazole. The kinetics release studies of the polymer-MTZ adducts were done at various pH values: 2.0, 7.4, and 8.5 phosphate buffer solutions. The obtained results proved that the hydrolytic behaviors of polymeric prodrugs robustly relied on the molecular weight of the polymer and the pH of the release media. The kinetics of the release process were described using Higuchi and Korsmeyer's models to explain the drug release mechanism.
机译:在目前的研究中,研究了聚合物分子量对甲硝唑(MTZ)释放作为来自合成的脯氨酸基聚合物的药物模型的影响。使用可逆添加的碎片链转移(筏)聚合,基于N-丙烯酰基-L-脯氨酸(Al-Pro-OH)的氨基酸基聚合物,相对较高的转换(55-98%)制备各种分子量(55-98%通过H-1 NMR光谱测量)。聚合方法以[单体](0)/ [CTA](0)/ [AIBN](0)的不同比例进行。使用具有预定分子量的脯氨酸基聚合物(甲基化形式的M-N = 6000-22 600)和低多分散性(M-W / M-N = 1.30-1.37)用于固定甲硝唑。聚合物-MTZ加合物的动力学释放研究以各种pH值进行:2.0,7.4和8.5次磷酸盐缓冲溶液。所得结果证明,聚合物前药的水解行为鲁棒地依赖于聚合物的分子量和释放介质的pH。使用Higuchi和Korsmeyer的模型描述了释放过程的动力学来解释药物释放机制。

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  • 来源
    《RSC Advances 》 |2016年第76期| 共7页
  • 作者单位

    Tanta Univ Dept Chem Fac Sci Tanta 31527 Egypt;

    Tanta Univ Dept Chem Fac Sci Tanta 31527 Egypt;

    Yamagata Univ Grad Sch Sci &

    Engn Dept Polymer Sci &

    Engn 4-3-16 Jonan Yonezawa Yamagata 9928510 Japan;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 化学 ;
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