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用于转染的DNA-阳离子脂质体复合物的形成方式和结构特征。

Mode of formation and structural features of DNA-cationic liposome complexes used for transfection.

作者信息

Gershon H, Ghirlando R, Guttman S B, Minsky A

机构信息

Department of Organic Chemistry, Weizmann Institute of Science, Rehovot, Israel.

出版信息

Biochemistry. 1993 Jul 20;32(28):7143-51. doi: 10.1021/bi00079a011.

Abstract

Complexes formed between cationic liposomes and nucleic acids represent a highly efficient vehicle for delivery of DNA and RNA molecules into a large variety of eukaryotic cells. By using fluorescence, gel electrophoresis, and metal-shadowing electron microscopy techniques, the factors that affect the, yet unclear, interactions between DNA and cationic liposomes as well as the structural features of the resulting complexes have been elucidated. A model is suggested according to which cationic liposomes bind initially to DNA molecules to form clusters of aggregated vesicles along the nucleic acids. At a critical liposome density, two processes occur, namely, DNA-induced membrane fusion, indicated by lipid mixing studies, and liposome-induced DNA collapse, pointed out by the marked cooperativity of the encapsulation processes, by their modulations by DNA-condensing agents, and also by their conspicuous independence upon DNA length. The DNA collapse leads to the formation of condensed structures which can be completely encapsulated within the fused lipid bilayers in a fast, highly cooperative process since their exposed surface is substantially smaller than that of extended DNA molecules. The formation of the transfecting DNA-liposome complexes in which the nucleic acids are fully encapsulated within a positively-charged lipid bilayer is proposed, consequently, to be dominated by mutual effects exerted by the DNA and the cationic liposomes, leading to interrelated lipid fusion and DNA collapse.

摘要

阳离子脂质体与核酸形成的复合物是一种将DNA和RNA分子高效递送至多种真核细胞的载体。通过荧光、凝胶电泳和金属投影电子显微镜技术,影响DNA与阳离子脂质体之间尚不明确的相互作用以及所得复合物结构特征的因素已得到阐明。提出了一个模型,根据该模型,阳离子脂质体最初与DNA分子结合,沿着核酸形成聚集囊泡簇。在临界脂质体密度下,会发生两个过程,即脂质混合研究表明的DNA诱导的膜融合,以及封装过程的显著协同性、DNA凝聚剂对其的调节以及它们对DNA长度的明显独立性所指出的脂质体诱导的DNA塌陷。DNA塌陷导致形成凝聚结构,由于其暴露表面比伸展的DNA分子小得多,这些凝聚结构可以在快速、高度协同的过程中完全封装在融合的脂质双层内。因此,核酸完全封装在带正电荷的脂质双层中的转染性DNA-脂质体复合物的形成被认为主要受DNA和阳离子脂质体相互作用的影响,导致相关的脂质融合和DNA塌陷。

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