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Peptide-Functionalized Poly(ethylene glycol) Star Polymers: DNA Delivery Vehicles with Multivalent Molecular Architecture

机译:肽官能化的聚乙二醇星形聚合物:具有多价分子结构的DNA传递载体

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摘要

Exploring the development of nonviral nucleic acid delivery vectors with progressive, specific, and novel designs in molecular architecture is a fundamental way to investigate how aspects of chemical and physical structure impact the transfection process. In this study, macromolecules comprised of a four-arm star poly(ethylene glycol) and termini modified with one of five different heparin binding peptides have been investigated for their ability to bind, compact, and deliver DNA to mammalian cells in vitro. These new delivery vectors combine a PEG-derived stabilizing moiety with peptides that exhibit unique cell-surface binding ability in a molecular architecture that permits multivalent presentation of the cationic peptides. Five peptide sequences of varying heparin binding affinity were studied; each was found to sufficiently bind heparin for biological application. Additionally, the macromolecules were able to bind and compact DNA into particles of proper size for endocytosis. In biological studies, the PEG-star peptides displayed a range of toxicity and transfection efficiency dependent on the peptide identity. The vectors equipped with peptides of highest heparin binding affinity were found to bind DNA tightly, increase levels of cellular internalization, and display the most promising transfection qualities. Our results suggest heparin binding peptides with specific sequences hold more potential than nonspecific cationic polymers to optimize transfection efficiency while maintaining cell viability. Furthermore, the built-in multivalency of these macromolecules may allow simultaneous binding of both DNA at the core of the polyplex and heparan sulfate on the surface of the cell. This scheme may facilitate a bridging transport mechanism, tethering DNA to the surface of the cell and subsequently ushering therapeutic nucleic acids into the cell. This multivalent star shape is therefore a promising architectural feature that may be exploited in the design of future polycationic gene delivery vectors.
机译:探索分子结构中具有渐进,特异性和新颖设计的非病毒核酸递送载体的开发,是研究化学和物理结构各方面如何影响转染过程的基本方法。在这项研究中,已经研究了由四臂星形聚乙二醇和末端修饰的大分子组成的五种不同的肝素结合肽之一,它们具有体外结合,压缩并向哺乳动物细胞递送DNA的能力。这些新的递送载体将PEG衍生的稳定部分与在分子结构中表现出独特的细胞表面结合能力的肽相结合,从而允许阳离子肽的多价呈递。研究了五种不同肝素结合亲和力的肽序列;发现每种都可以充分结合肝素以用于生物学应用。此外,大分子能够将DNA结合并压缩成适当大小的颗粒,以进行内吞。在生物学研究中,PEG-star肽显示出一系列毒性和转染效率,具体取决于肽的同一性。发现具有最高肝素结合亲和力的肽的载体紧密地结合DNA,增加细胞内在化的水平,并显示出最有希望的转染质量。我们的结果表明,具有特定序列的肝素结合肽比非特异性阳离子聚合物具有更大的潜力,可以优化转染效率,同时保持细胞活力。此外,这些大分子的内在多价性可允许多聚体核心处的DNA与细胞表面上的硫酸乙酰肝素同时结合。该方案可以促进架桥运输机制,将DNA束缚到细胞表面,然后将治疗性核酸引入细胞。因此,这种多价星形形状是一种有前途的建筑特征,可以在未来的聚阳离子基因传递载体的设计中加以利用。

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