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基于空间稳定化BGTC的脂质体复合物:结构特征及体内转染小鼠气道基因

Sterically stabilized BGTC-based lipoplexes: structural features and gene transfection into the mouse airways in vivo.

作者信息

Pitard B, Oudrhiri N, Lambert O, Vivien E, Masson C, Wetzer B, Hauchecorne M, Scherman D, Rigaud J L, Vigneron J P, Lehn J M, Lehn P

机构信息

UMR 7001, CNRS/ENSCP/Aventis Gencell, Vitry-sur-Seine, France.

出版信息

J Gene Med. 2001 Sep-Oct;3(5):478-87. doi: 10.1002/jgm.211.

Abstract

BACKGROUND

Colloidal stability of lipid/DNA aggregates is a major requirement for cationic lipid-mediated transfection which is particularly difficult to fulfil at the high DNA concentrations used for in vivo gene delivery. Thus, we have investigated the potential of poly(ethyleneglycol) (PEG) conjugates for steric stabilization of lipoplexes formed by bis(guanidinium)-tren-cholesterol/dioleoyl phosphatidylethanolamine (BGTC/DOPE) liposomes, a class of cationic liposomes we have developed over the past few years.

METHODS AND RESULTS

We demonstrate that adequate lipophilic PEG derivatives can stabilize BGTC/DOPE lipoplexes formed at high DNA concentration. We also report the results of cryotransmission electron microscopy studies indicating that PEG-stabilized lipoplexes form DNA-coated structures which assemble into clusters exhibiting various complex morphologies. Finally, we report data from in vivo transfection experiments suggesting that PEG-mediated colloidal stabilization of concentrated lipoplex solutions may allow enhanced transfection of the mouse airways via intranasal administration.

CONCLUSION

Our results represent an important step towards the design of multimodular BGTC-based systems for improved in vivo gene transfection.

摘要

背景

脂质/DNA聚集体的胶体稳定性是阳离子脂质介导的转染的主要要求,而在用于体内基因递送的高DNA浓度下尤其难以实现。因此,我们研究了聚乙二醇(PEG)缀合物对由双(胍基)-三亚乙基四胺-胆固醇/二油酰磷脂酰乙醇胺(BGTC/DOPE)脂质体形成的脂质体复合物进行空间稳定的潜力,这是我们在过去几年中开发的一类阳离子脂质体。

方法与结果

我们证明了适当的亲脂性PEG衍生物可以稳定在高DNA浓度下形成的BGTC/DOPE脂质体复合物。我们还报告了低温透射电子显微镜研究的结果,表明PEG稳定的脂质体复合物形成了DNA包被的结构,这些结构组装成具有各种复杂形态的簇。最后,我们报告了体内转染实验的数据,表明PEG介导的浓缩脂质体复合物溶液的胶体稳定可能允许通过鼻内给药增强对小鼠气道的转染。

结论

我们的结果代表了朝着设计用于改善体内基因转染的多模块BGTC基系统迈出的重要一步。

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