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A simple protocol for preparation of a liposomal vesicle with encapsulated plasmid DNA that mediate high accumulation and reporter gene activity in tumor tissue

机译:用封装的质粒DNA制备脂质体囊泡的简单方案该质粒DNA介导肿瘤组织中的高积累和报道基因活性

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摘要

The systemic delivery of gene therapeutics by non-viral methods has proven difficult. Transfection systems that are performing well in vitro have been reported to have disadvantageous properties such as rapid clearance and short circulation time often resulting in poor transfection efficiency when applied in vivo. Large unilaminary vesicles (LUV) with encapsulated nucleic acids designated stabilized-plasmid-lipo-particle (SPLP) have showed promising results in terms of systemic stability and accumulation in tumor tissue due to the enhanced permeability and retention effect (EPR). We have developed a simple protocol for the research-scale preparation of SPLPs from commercially available reagents with high amounts of encapsulated plasmid DNA. The SPLPs show properties of promising accumulation in tumor tissue in comparison to other organs when intravenously injected into xenograft tumor-bearing nude mice. Although transcriptionally targeted suicide gene therapy was not achieved, the SPLPs were capable of mediating reporter gene transfection in subcutaneous flank tumors originating from human small cell lung cancer.
机译:已经证明通过非病毒方法全身递送基因治疗剂是困难的。据报道,在体外运行良好的转染系统具有不利的特性,例如清除速度快和循环时间短,当在体内应用时通常导致较差的转染效率。由于增强的通透性和保留效应(EPR),具有被包封的核酸的大的单囊泡(LUV)被称为稳定的质粒脂质颗粒(SPLP),在系统稳定性和在肿瘤组织中的积累方面已显示出令人鼓舞的结果。我们已经开发了一种简单的方案,用于从具有大量封装质粒DNA的市售试剂中大规模制备SPLP。与其他器官相比,SPLPs在静脉注射到异种移植荷瘤裸鼠中时显示出在肿瘤组织中有希望积累的特性。尽管未实现转录靶向自杀基因治疗,但SPLP能够介导源自人类小细胞肺癌的皮下胁腹肿瘤中的报告基因转染。

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