首页> 外文期刊>Journal of Controlled Release: Official Journal of the Controlled Release Society >PEG-based block catiomers possessing DNA anchoring and endosomal escaping functions to form polyplex micelles with improved stability and high transfection efficacy
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PEG-based block catiomers possessing DNA anchoring and endosomal escaping functions to form polyplex micelles with improved stability and high transfection efficacy

机译:具有DNA锚定和内体逃逸功能的基于PEG的嵌段复合物形成具有改善的稳定性和高转染效率的多聚体胶束

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摘要

For the development of polyplex systems showing a high transfection efficacy without a large excess of polycations, a lysine (Lys) unit as a DNA anchoring moiety was introduced into the amino acid sequence in poly(ethylene glycol)-b-cationic poly(N-substituted asparagine) with a flanking N-(2-aminoethyl)-2-aminoethyl group (PEG-b-Asp(DET)) resulting in PEG-b-P[Lys/Asp(DET)], in which the Asp(DET) unit acts as a buffering moiety inducing endosomal escape with minimal cytotoxicity. PEG-b-P[Lys/Asp(DET)]/DNA polyplexes exhibited a narrow size distribution of similar to 90 nm without secondary aggregates at the stoichiometric N/P 1, suggesting the formation of PEG-shielded polyplex micelles. The introduction of Lys units into the catiomer sequence facilitated cellular uptake and a 100-fold higher level of gene expression with PEG-b-P [Lys/Asp(DET)]/DNA polyplex micelles prepared even at a lowered N/P 2, possibly due to the enhanced association power of the anchoring Lys units. (c) 2007 Elsevier B.V All rights reserved.
机译:为了开发在没有大量过量阳离子的情况下显示高转染效率的多聚体系统,将赖氨酸(Lys)单元作为DNA锚定部分引入了聚(乙二醇)-b-阳离子聚(N-侧翼的N-(2-氨基乙基)-2-氨基乙基(PEG-b-Asp(DET))取代了天冬酰胺),得到PEG-bP [Lys / Asp(DET)],其中Asp(DET)单元作为诱导内体逃逸的缓冲部分,具有最小的细胞毒性。 PEG-b-P [Lys / Asp(DET)] / DNA复合物在化学计量比N / P 1处显示出类似于90 nm的窄尺寸分布,而没有次级聚集体,表明形成了PEG保护的复合物胶束。将Lys单位引入Catiomer序列有助于细胞摄取,并且即使在较低的N / P 2下制备的PEG-bP [Lys / Asp(DET)] / DNA复合胶束也能使细胞表达提高100倍。增强了锚定Lys单位的关联能力。 (c)2007 Elsevier B.V保留所有权利。

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