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PEG-epirubicin Conjugates with High Drug Loading

机译:PEG-厄比霉素与高载药量结合

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PEG is used as a polymeric carrier for low molecular weight drugs,but limitations arise from the fact that only one or two hydroxyl residues are on each polymer.Therefore,the synthesis of dendrimeric structures,based on amino adipic acid or beta-glutamic acid,as a branching molecule,built on a PEG diol of Mw 10,000 Da was investigated.The large polycyclic drug epirubicin molecule was chosen as a model to investigate the influence of structure branching and drug steric hindrance during coupling reactions.Several derivatives with increased numbers of drug molecules linked to each PEG chain were synthesized and their physical,chemical and biological properties were studied.The use of specific amino bicarboxylic acids (amino adipic acid or beta-glutamic acid),as the branching moiety for the dendrimer synthesis,allowed linking the hindered molecule epirubicin to multibranched PEG.Most drug loaded conjugates only dissolve in water following dissolution in DMSO.This solubility problem was solved by adding a hydrophilic peptide linker between the drug and the polymer.The conjugates,synthesized in good yield and purity,showed better stability than free epirubicin in different pH buffers and in plasma as well as prolonged residence time in blood.Dynamic light scattering investigation showed that these products have a high tendency to aggregate forming stable micelles.
机译:PEG用作低分子量药物的聚合物载体,但局限性在于每个聚合物上只有一个或两个羟基残基。因此,基于氨基己二酸或β-谷氨酸的树枝状结构的合成,以分子量为10,000 Da的PEG二醇为支链分子作为研究对象,选择了大型多环药物表柔比星分子作为模型,研究了结构支化和药物位阻对偶联反应的影响。合成了与每个PEG链连接的分子,并研究了它们的物理,化学和生物学特性。使用特定的氨基双羧酸(氨基己二酸或β-谷氨酸)作为树枝状聚合物合成的支链部分,可以连接受阻分子表柔比星到多支PEG。大多数负载药物的结合物仅在DMSO中溶解后才溶于水。通过在药物和聚合物之间添加亲水性肽接头,合成的共轭物在不同的pH缓冲液和血浆中比游离的表柔比星具有更好的稳定性,并且在血液中的停留时间更长。动态光散射研究结果表明这些产品极有可能聚集形成稳定的胶束。

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