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利用阳离子脂质体载体优化体外和体内实现mRNA介导的肿瘤细胞转染的方法。

Optimization of methods to achieve mRNA-mediated transfection of tumor cells in vitro and in vivo employing cationic liposome vectors.

作者信息

Lu D, Benjamin R, Kim M, Conry R M, Curiel D T

机构信息

Gene Therapy Program, UAB Comprehensive Cancer Center, University of Alabama at Birmingham 35294, USA.

出版信息

Cancer Gene Ther. 1994 Dec;1(4):245-52.

PMID:7627814
Abstract

Direct in vivo transfection of tumor nodules in situ via liposome-DNA complexes has been employed as a strategy to accomplish antitumor immunization. To circumvent the potential safety hazards associated with systemic localization of delivered DNA, the utility of mRNA transcript-mediated gene delivery was explored. Capped, polyadenylated mRNA transcripts encoding the firefly luciferase and Escherichia coli lacZ reporter genes were derived by in vitro transcription. Transfection of the human breast cancer cell line MDA-MB-435 in vitro was accomplished employing cationic liposome-mRNA complexes. Evaluation of a panel of cationic liposome preparations demonstrated significant differences in the capacity of the various preparations to accomplish mRNA-mediated transfection. Quantitative evaluation of in vitro transfection demonstrated that target cells could be transfected at a high level of efficiency. The mRNA liposome-complexes were evaluated for in vivo transfection of tumor nodules in human xenografts in athymic nude mice. It could be demonstrated the liposome-mRNA complexes were comparable in efficacy to liposome-DNA complexes in accomplishing in situ tumor transfection. Thus, mRNA may be considered as an alternative to plasmid DNA as a gene transfer vector for genetic immunopotentiation applications.

摘要

通过脂质体 - DNA复合物对肿瘤结节进行直接体内原位转染已被用作实现抗肿瘤免疫的一种策略。为了规避与递送DNA的全身定位相关的潜在安全风险,人们探索了mRNA转录本介导的基因递送的效用。通过体外转录获得了编码萤火虫荧光素酶和大肠杆菌lacZ报告基因的加帽、聚腺苷酸化的mRNA转录本。利用阳离子脂质体 - mRNA复合物在体外完成了对人乳腺癌细胞系MDA - MB - 435的转染。对一组阳离子脂质体制剂的评估表明,各种制剂在实现mRNA介导的转染能力方面存在显著差异。体外转染的定量评估表明,靶细胞能够以高效率被转染。对无胸腺裸鼠人异种移植瘤中的肿瘤结节进行了体内转染评估,结果表明脂质体 - mRNA复合物在原位肿瘤转染方面的功效与脂质体 - DNA复合物相当。因此,mRNA可被视为质粒DNA的替代品,作为用于基因免疫增强应用的基因转移载体。

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