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Chemical Activation of Lipoplexes Formed from DNA and a Redox-Active, Ferrocene-Containing Cationic Lipid

机译:由DNA和氧化还原活性的二茂铁阳离子脂质形成的脂质体的化学活化

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We recently reported that the ferrocene-containing cationic lipid BFDMA [bis(11-ferrocenylundecyl)dimethyl-ammonium bromide] can be used to mediate cell transfection, and that levels of transfection depend critically upon the oxidation state of the ferrocenyl groups of the lipid. Here, we report that the redox activity of BFDMA can be exploited to transform lipoplexes formed from oxidized BFDMA (which do not transfect cells) to lipoplexes that are "active" (and thus mediate high levels of transgene expression) by treatment with the chemical reducing agent glutathione (GSH). We demonstrate that GSH can be used to reduce the ferrocenium groups of oxidized BFDMA rapidly both (i) in solution and (ii) in lipoplexes formed by mixing oxidized BFDMA and DNA. Lipoplexes transformed in this manner mediate levels of cell transfection in vitro that are comparable to levels of transfection mediated by lipoplexes prepared by mixing DNA and reduced BFDMA. We demonstrate further that the chemical reduction of oxidized BFDMA leads to changes in the zeta potentials of these lipoplexes (e.g., from negative to positive). Characterization of lipoplex internalization using confocal microscopy demonstrated that these changes in zeta potential correlate to differences in the extents to which these lipoplexes are internalized by cells. These results provide a framework from which to interpret differences in cell transfection mediated by reduced and oxidized BFDMA. When combined, the results of this study suggest the basis of an approach that could be used to transform lipoplexes actively or "on-demand" and provide spatial and/or temporal control over the transfection of cells in a range of different fundamental and applied contexts.
机译:我们最近报道,含二茂铁的阳离子脂质BFDMA [双(11-二茂铁基十一烷基)二甲基溴化铵]可用于介导细胞转染,转染水平关键取决于脂质中二茂铁基团的氧化态。在这里,我们报道通过化学还原处理可以利用BFDMA的氧化还原活性,将氧化的BFDMA(不转染细胞)形成的脂质复合物转化为“活跃的”(从而介导高水平的转基因表达)的脂质复合物。谷胱甘肽(GSH)。我们证明,谷胱甘肽可用于快速还原氧化的BFDMA的二茂铁基团(i)在溶液中和(ii)在通过混合氧化的BFDMA和DNA形成的脂质复合物中。以这种方式转化的脂质复合物在体外介导的细胞转染水平与通过混合DNA和还原的BFDMA制备的脂质复合物介导的转染水平相当。我们进一步证明,氧化的BFDMA的化学还原导致这些脂质复合物的ζ电势改变(例如,从负到正)。使用共聚焦显微镜对脂质体内部化的表征表明,ζ电位的这些变化与这些脂质体被细胞内化的程度的差异相关。这些结果提供了一个框架,可以用来解释由还原和氧化的BFDMA介导的细胞转染的差异。当结合在一起时,这项研究的结果表明了一种方法的基础,该方法可用于主动或“按需”转化脂质复合物,并在一系列不同的基础和应用环境中提供细胞转染的空间和/或时间控制。

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