Setyawati Damai Ria, Azzahra Khairunnisa, Mardliyati Etik, Maharani Bismi Yasinta
Research Center for Vaccine and Drugs, National Research and Innovation Agency, Jakarta, Indonesia.
Department of Pharmacy, Faculty of Health and Sciences, Universitas Islam Negeri Syarif Hidayatullah, Jakarta, Indonesia; Nano Center Indonesia, South Tangerang 15314, Indonesia.
Biochim Biophys Acta Gen Subj. 2024 Nov;1868(11):130705. doi: 10.1016/j.bbagen.2024.130705. Epub 2024 Aug 22.
Cationic liposomes represent a promising non-viral carrier platform for gene delivery. The successful intracellular delivery of genes to the target cell is highly influenced by lipid compositions in the liposomal formulation. In the present study, a Box-Behnken design was applied to investigate the optimal lipid composition for the liposome-based transfection agent.
The concentrations of DOTAP, DSPE-PEG, and cholesterol were set as independent factors. A total of 15 lipid compositions were generated and tested for specific responses, including particle size, encapsulation efficiency, cell viability, and cell transfection. The data were then analyzed to predict the optimal composition using response surface methodology (RSM).
The results for particle size, encapsulation efficiency, cell viability and fluorescence intensity ranged from 158.7 to 2064 nm, 48.19-95.72%, 81.50-122.67%, and 0.0-9.08, respectively. Compositions of liposome-based transfection agent without DOTAP, those without cholesterol, and those containing DSPE-PEG2000 with a molar ratio equal to or greater than that of cholesterol tended to exhibit low encapsulation efficiency. The ability of the liposome to complex DNA, as determined through electrophoresis gel retardation assay, showed that the composition without DOTAP produced DNA bands, indicating that the prepared liposomes had a less ability to complex DNA. The cytotoxicity test results indicated that all lipid compositions were considered non-toxic, as they exhibited >80% cell viability. The cell transfection assay demonstrated that the lipid composition containing a combination of DOTAP and cholesterol was able to transfect DNA into cells. According to response analysis, RSM predicted that the optimal lipid composition consisted of 2.75 μmol DOTAP and 0.91 μmol cholesterol, with a desirability value of 0.85.
Although the equation model is still acceptable for predicting the optimal lipid composition, further study is needed to obtain a model with higher desirability, such as by using more lipid compositions, increased replications, and different variable responses.
阳离子脂质体是一种很有前景的非病毒基因递送载体平台。基因成功递送至靶细胞内受到脂质体制剂中脂质组成的高度影响。在本研究中,采用Box-Behnken设计来研究基于脂质体的转染剂的最佳脂质组成。
将DOTAP、DSPE-PEG和胆固醇的浓度设定为独立因素。共生成15种脂质组成,并测试其特定反应,包括粒径、包封率、细胞活力和细胞转染。然后使用响应面法(RSM)分析数据以预测最佳组成。
粒径、包封率、细胞活力和荧光强度的结果分别为158.7至2064nm、48.19 - 95.72%、81.50 - 122.67%和0.0 - 9.08。不含DOTAP的基于脂质体的转染剂组成、不含胆固醇的组成以及含有摩尔比等于或大于胆固醇的DSPE-PEG2000的组成往往表现出低包封率。通过电泳凝胶阻滞试验测定的脂质体与DNA复合的能力表明,不含DOTAP的组成产生了DNA条带,表明所制备的脂质体与DNA复合的能力较低。细胞毒性测试结果表明,所有脂质组成均被认为无毒,因为它们的细胞活力>80%。细胞转染试验表明,含有DOTAP和胆固醇组合的脂质组成能够将DNA转染到细胞中。根据响应分析,RSM预测最佳脂质组成为2.75μmol DOTAP和0.91μmol胆固醇,可取性值为0.85。
尽管该方程模型在预测最佳脂质组成方面仍然可以接受,但需要进一步研究以获得具有更高可取性的模型,例如通过使用更多脂质组成、增加重复次数和不同的变量响应。
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