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琥珀酰化聚亚乙基亚胺衍生物极大地提高了聚合物复合物的血清稳定性和体外基因转染效率。

Succinylated Polyethylenimine Derivatives Greatly Enhance Polyplex Serum Stability and Gene Delivery In Vitro.

出版信息

Biomacromolecules. 2018 Nov 12;19(11):4348-4357. doi: 10.1021/acs.biomac.8b01248. Epub 2018 Nov 1.

Abstract

Polymeric materials provide particularly attractive scaffolds for the creation of supramolecular bioconjugates for the delivery of nucleic acids but typically lack the efficiency and biocompatibility to be clinically relevant. To address both issues, we produced zwitterion-like derivatives of polyethylenimine via succinylation of primary and secondary amines (zPEI). Polymers were generated with 9-55% of the amines modified (zPEI X, where X indicates the percentage of amines succinylated). Characterization of polymer/DNA interactions revealed that the presence of succinyl groups decreased the protonation constant of zPEI, resulting in both a decreased buffering capacity and polyplexes that dissociated in the presence of lower amounts of a competing counteranion compared to unmodified PEI. zPEI polyplexes also exhibited decreased aggregation in the presence of serum proteins. In the absence of serum, transfections with zPEI/DNA polyplexes exhibited similar or slightly improved transgene expression compared to unmodified PEI/DNA polyplexes. More importantly, zPEI 9-25 increased transgene expression up to 51-fold upon transfection in the presence of serum compared to PEI/DNA, while higher succinylation decreased gene delivery activity. Gene delivery mediated by zPEI 9/DNA polyplexes in the presence of serum was equal to or greater than unmodified PEI/DNA polyplexes in the absence of serum. The data suggest that succinylation increased gene transfection by decreasing polymer/DNA interaction strength, which may allow for more facile polyplex unpackaging, and/or increased stability of polyplex size and inhibition of aggregation in the presence of serum. However, it appears there exists a balance between the positive effects of succinylation and the need for sufficient polymer/DNA binding to condense and protect the cargo.

摘要

聚合物材料为构建用于核酸递送的超分子生物缀合物提供了特别有吸引力的支架,但通常缺乏效率和生物相容性,无法达到临床相关的水平。为了解决这两个问题,我们通过对伯胺和仲胺进行琥珀酰化,制备了类似两性离子的聚亚乙基亚胺衍生物(zPEI)。聚合物的胺基有 9-55%被修饰(zPEI X,其中 X 表示被琥珀酰化的胺的百分比)。聚合物/DNA 相互作用的特性表明,琥珀酰基的存在降低了 zPEI 的质子化常数,导致其缓冲能力降低,并且与未修饰的 PEI 相比,在存在较少竞争抗衡阴离子的情况下,多聚物更容易解离。zPEI 多聚物在存在血清蛋白的情况下也表现出较低的聚集。在没有血清的情况下,与未修饰的 PEI/DNA 多聚物相比,zPEI/DNA 多聚物的转染显示出相似或略微改善的转基因表达。更重要的是,与 PEI/DNA 相比,在有血清存在的情况下,zPEI 9-25 的转染可将转基因表达提高 51 倍,而更高的琥珀酰化程度则降低了基因传递活性。在有血清存在的情况下,zPEI 9/DNA 多聚物介导的基因传递与无血清时未修饰的 PEI/DNA 多聚物的基因传递相当或更高。数据表明,琥珀酰化通过降低聚合物/DNA 相互作用强度来增加基因转染,这可能允许更方便地解包多聚物,和/或增加多聚物大小的稳定性并抑制在血清存在下的聚集。然而,琥珀酰化的积极作用和聚合物/DNA 结合以浓缩和保护货物的必要性之间似乎存在平衡。

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