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使用带有聚酰胺胺树枝状分子的脂质制备高效基因载体:提高血清耐受性。

Preparation of efficient gene carriers using a polyamidoamine dendron-bearing lipid: improvement of serum resistance.

作者信息

Takahashi Toshinari, Harada Atsushi, Emi Nobuhiko, Kono Kenji

机构信息

Department of Applied Chemistry, Graduate School of Engineering, Osaka Prefecture University, 1-1 Gakuen-cho, Sakai, Osaka 599-8531, Japan.

出版信息

Bioconjug Chem. 2005 Sep-Oct;16(5):1160-5. doi: 10.1021/bc050012f.

Abstract

In a previous study, we developed a novel cationic lipid consisting of polyamidoamine dendron of third generation and two dodecyl chains, designated as DL-G3, which in combination with a fusogenic lipid dioleoylphosphatidylethanolamine (DOPE) achieves efficient transfection of CV1 cells by synergetic action of the proton sponge effect and membrane fusion. This study examines the effect of serum on the transfection activity of the DL-G3-DOPE-plasmid DNA lipoplexes. The transfection activity of a lipoplex with a composition optimized in the absence of serum decreased markedly in the presence of serum. However, the lipoplexes that induce efficient transfection in the presence of serum were obtainable by controlling the charge ratio of the primary amine of the DL-G3 to the phosphate group (N/P ratio) and DOPE content. The complex, which exhibited the highest transfection activity in the presence of serum, has a lower N/P ratio and higher DOPE content than that optimized in the absence of serum. Whereas disintegration of these complexes was induced by addition of heparin, which is a polysaccharide with negatively charged groups, the complex that retained transfection activity in the presence of serum required more negative charges of heparin for complex disintegration. That result implies its higher stability against negatively charged serum proteins. Comparison of the serum-resistant complex with some commercially available transfection reagents, such as Lipofectamine and SuperFect, indicates that the DL-G3 complex achieved more efficient transfection of these cells in the presence of serum.

摘要

在之前的一项研究中,我们开发了一种新型阳离子脂质,它由第三代聚酰胺胺树枝状大分子和两条十二烷基链组成,命名为DL-G3,其与促融合脂质二油酰磷脂酰乙醇胺(DOPE)组合,通过质子海绵效应和膜融合的协同作用实现对CV1细胞的高效转染。本研究考察了血清对DL-G3-DOPE-质粒DNA脂质体转染活性的影响。在无血清条件下优化组成的脂质体在有血清存在时转染活性显著降低。然而,通过控制DL-G3的伯胺与磷酸基团的电荷比(N/P比)和DOPE含量,可获得在有血清存在时能诱导高效转染的脂质体。在有血清存在时表现出最高转染活性的复合物,其N/P比比在无血清条件下优化的复合物更低,DOPE含量更高。虽然添加带负电荷基团的多糖肝素可诱导这些复合物解体,但在有血清存在时仍保留转染活性的复合物需要更多负电荷的肝素才能使复合物解体。这一结果表明其对带负电荷的血清蛋白具有更高的稳定性。将抗血清复合物与一些市售转染试剂(如Lipofectamine和SuperFect)进行比较,结果表明DL-G3复合物在有血清存在时能更有效地转染这些细胞。

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