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首页> 外文期刊>Gene therapy >Protective copolymers for nonviral gene vectors: synthesis, vector characterization and application in gene delivery.
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Protective copolymers for nonviral gene vectors: synthesis, vector characterization and application in gene delivery.

机译:非病毒基因载体的保护性共聚物:合成,载体表征以及在基因传递中的应用。

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摘要

Uncontrolled interactions of gene vectors and drug carriers in and with an in vivo environment pose serious limitations to their applicability. In order to reduce such interactions we have designed, synthesized and applied novel copolymers of poly(ethylene glycol) and reactive linkers which are derivatized with anionic peptides after copolymerization. The anionic copolymer derivatives are used to coat positively charged nonviral gene vectors by electrostatic interactions. The copolymer coat confers to polyelectrolyte colloids of DNA and polycations steric stabilization in their minimal size and prevents salt- and serum albumin-induced aggregation. Furthermore, complement activation and the interaction with serum proteins are drastically reduced or abolished in contrast to unprotected DNA complexes. The designed vectors are compatible with the intracellular steps of gene delivery and can even enhance transfection efficiency as demonstrated with various adherent and nonadherent cell lines in culture. The synthetic concept is amenable to the principles of combinatorial chemistry and the copolymeric products may be applicable beyond gene delivery in targeted drug delivery. Gene Therapy (2000) 7, 1183-1192.
机译:基因载体和药物载体在体内环境中以及在体内环境中的不受控制的相互作用严重限制了它们的适用性。为了减少这种相互作用,我们设计,合成和应用了聚乙二醇和反应性连接基的新型共聚物,它们在共聚后被阴离子肽衍生化。阴离子共聚物衍生物用于通过静电相互作用包覆带正电荷的非病毒基因载体。共聚物涂层赋予DNA和聚阳离子空间尺寸最小的聚电解质胶体稳定的功能,并防止盐和血清白蛋白诱导的聚集。此外,与未保护的DNA复合物相比,补体激活和与血清蛋白的相互作用被大大降低或消除。设计的载体与基因传递的细胞内步骤兼容,甚至可以提高转染效率,如培养中各种粘附和非粘附细胞系所证明的。合成概念适合于组合化学原理,并且共聚产物可以在靶向药物递送中适用于基因递送以外的领域。基因疗法(2000)7,1183-1192。

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