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阳离子脂质体 - DNA复合物作为基因传递载体:对类骨细胞的研究进展及作用机制

Cationic liposome-DNA complexes as gene delivery vectors: Development and behaviour towards bone-like cells.

作者信息

Oliveira A C, Ferraz M P, Monteiro F J, Simões S

机构信息

Instituto de Engenharia Biomédica, Porto, Portugal.

出版信息

Acta Biomater. 2009 Jul;5(6):2142-51. doi: 10.1016/j.actbio.2009.02.019. Epub 2009 Feb 20.

DOI:10.1016/j.actbio.2009.02.019
PMID:19332382
Abstract

Modulation of the biological pathways responsible for fracture repair and osteogenisis may accelerate regeneration. Gene therapy is an alternative method for the release of osteogenisis-stimulating proteins into tissues. The development of vectors for gene release is still a problem in terms of ethics and techniques. In this work we evaluated whether cationic liposomes constitute a valuable strategy for the release of genetic material into bone tissue cells as non-viral vectors. Liposomes were prepared with 1,2-dioleoyl-3-trimethylammonium propane (DOTAP)-2-dioleoyl-sn-glycero-3-phosphatidylethanolamine and DOTAP-cholesterol, and characterized according to their size, zeta potential, DNA protection capacity and cytotoxicity. Transfection studies were also carried out using pCMVbeta-gal plasmid in two osteoblastic cell lines (MG63 and MC3T3-E1) and in the 294T line, varying the charge ratio and the applied DNA dose. Inclusion of transferrin to increase the expression was also tested. The results suggest that there is great dependency between the transfection activity and the lipid formulation, the charge ratios of the complexes, the applied DNA dose and the cell type. There were even some differences concerning both osteoblastic lines under study. The cells of the MC3T3-E1 line present greater expression levels than the cells of the MG-63 line. The conjugation of the transferrin with the complexes contributes to the increase in transfection levels, possibly due to an increase in internalization of complexes. It is thus a good strategy for inducing the expression of specific genes in osteoblast-like cells.

摘要

调节负责骨折修复和成骨的生物学途径可能会加速再生。基因治疗是一种将成骨刺激蛋白释放到组织中的替代方法。就伦理和技术而言,用于基因释放的载体的开发仍然是一个问题。在这项工作中,我们评估了阳离子脂质体作为非病毒载体将遗传物质释放到骨组织细胞中是否是一种有价值的策略。用1,2 - 二油酰基 - 3 - 三甲基铵丙烷(DOTAP)-2 - 二油酰基 - sn - 甘油 - 3 - 磷脂酰乙醇胺和DOTAP - 胆固醇制备脂质体,并根据其大小、zeta电位、DNA保护能力和细胞毒性进行表征。还使用pCMVβ - gal质粒在两种成骨细胞系(MG63和MC3T3 - E1)以及294T细胞系中进行转染研究,改变电荷比和应用的DNA剂量。还测试了加入转铁蛋白以增加表达。结果表明,转染活性与脂质制剂、复合物的电荷比、应用的DNA剂量和细胞类型之间存在很大的依赖性。在所研究的两种成骨细胞系之间甚至存在一些差异。MC3T3 - E1细胞系的细胞比MG - 63细胞系的细胞呈现出更高的表达水平。转铁蛋白与复合物的结合有助于提高转染水平,这可能是由于复合物内化增加所致。因此,它是在成骨样细胞中诱导特定基因表达的良好策略。

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