首页> 外文期刊>Biochimica et biophysica acta. Gene structure and expression >Polymer chemical structure is a key determinant of physicochemical and colloidal properties of polymer-DNA complexes for gene delivery
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Polymer chemical structure is a key determinant of physicochemical and colloidal properties of polymer-DNA complexes for gene delivery

机译:聚合物化学结构是决定基因传递的聚合物-DNA复合物的物理化学和胶体性质的关键决定因素

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Polyplexes are now emerging as potentially useful vectors for gene therapy. To improve our understanding of how the chemical structure of the polymer affects the properties of these systems, a series of structurally related polymers, the linear poly(amidoamine)s (PAAs), have been examined for their abilities to form complexes with DNA. Structure-dependent differences in DNA binding are shown by gel electrophoretic retardation of DNA and thermal transition analyses. Two PAAs, NG28 and NG30, stand out as having high affinity DNA binding characteristics, similar to the model homopolypeptide, poly-L-lysine. In addition, differences in complex formation, particle size and surface charge are displayed for the different polymer-DNA systems. Electron microscopy studies showed that the polymers condensed DNA into similar unit structures but only complexes with NG30 did not undergo agglomeration. This was attributed to an excess of complexed polymer forming a shell of uncomplexed polymer chain segments around a condensed DNA-polymer core. The transfection activities of these polymer complexes differ greatly, and some of these differences can be explained in a multifactorial way by the physicochemical and colloidal properties. It is concluded that polymer chemical structure dictates the apparent affinity of DNA binding, and also several of the important colloidal characteristics of the resulting complexes.
机译:如今,复合物正在成为基因治疗的潜在有用载体。为了更好地理解聚合物的化学结构如何影响这些系统的性能,已经研究了一系列结构相关的聚合物,即线性聚(氨基胺)(PAA)与DNA形成复合物的能力。 DNA结合的凝胶电泳阻滞和热转变分析显示了DNA结合的结构依赖性差异。两种PAA NG28和NG30具有高亲和力DNA结合特性,与模型同型多肽poly-L-赖氨酸相似。此外,对于不同的聚合物-DNA系统,在复合物的形成,粒径和表面电荷方面也存在差异。电子显微镜研究表明,聚合物将DNA浓缩成相似的单元结构,但只有与NG30的复合物不会发生团聚。这归因于过量的络合聚合物在缩合的DNA-聚合物核周围形成未络合的聚合物链段的壳。这些聚合物复合物的转染活性差异很大,其中一些差异可以通过理化和胶体性质以多因素的方式解释。结论是,聚合物的化学结构决定了DNA结合的表观亲和力,也决定了所得复合物的几个重要的胶体特性。

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