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通过统计析因设计制备和优化 PIT 固体脂质纳米粒。

Preparation and optimization of PIT solid lipid nanoparticles via statistical factorial design.

机构信息

Department of Drug Sciences, Faculty of Pharmacy, University of Catania, Catania, Italy.

出版信息

Eur J Med Chem. 2012 Mar;49:110-7. doi: 10.1016/j.ejmech.2012.01.001. Epub 2012 Jan 4.

Abstract

The objective of this study was the preparation, physico-chemical characterization and statistical optimization of cationic solid lipid nanoparticles (SLN) prepared by the PIT method as potential carrier for gene therapy, emphasizing the application of factorial design in such a kind of studies. The preliminary screening from a physico-chemical point of view on three cationic lipids (CTAB, DDAB and DOTAP), selected on the basis of their different chemical structure and increasing lipophilicity, allowed us to select SLN with DOTAP, due to its higher zeta potential and smaller particle size. Afterward, a 2(2) full factorial experimental design was developed in order to study the effects of two independent variables (amount of DOTAP and concentration of lipid matrix) and their interaction on mean particle size and zeta potential values. The factorial planning was validated by ANOVA analysis; the correspondence between the predicted values of size and zeta and those measured experimentally confirmed the validity of the design and the equation applied for its resolution. The factorial design showed a significant influence of the independent variables on the selected parameters; in particular, a higher effect of DOTAP was observed on zeta potential value. Different dilutions of the optimized SLN containing 7% w/w of cutina CP and 1% w/w of DOTAP, with size and zeta potential values respectively of 462.9 nm and 50.8 mV, were in vitro examined to evaluate the possible cytotoxicity on two models of cell cultures: human prostate cancer androgen-non-responsive DU-145 cells and primary cultures of rat astrocytes.

摘要

本研究的目的是制备、物理化学表征和统计优化通过 PIT 法制备的阳离子固体脂质纳米粒 (SLN),作为基因治疗的潜在载体,重点强调了在这种研究中应用析因设计。基于不同的化学结构和增加的亲脂性,从物理化学角度对三种阳离子脂质(CTAB、DDAB 和 DOTAP)进行了初步筛选,选择了 DOTAP 作为 SLN 的候选材料,因为它具有更高的 Zeta 电位和更小的粒径。之后,开发了一个 2(2)完全析因实验设计,以研究两个独立变量(DOTAP 的用量和脂质基质的浓度)及其相互作用对平均粒径和 Zeta 电位值的影响。方差分析验证了析因设计的有效性;大小和 Zeta 的预测值与实验测量值之间的一致性证实了设计和应用方程的有效性。析因设计显示独立变量对所选参数有显著影响;特别是,DOTAP 对 Zeta 电位值的影响更大。不同稀释度的优化 SLN 含有 7%w/w 的角质 CP 和 1%w/w 的 DOTAP,粒径和 Zeta 电位值分别为 462.9nm 和 50.8mV,体外评估了对两种细胞培养模型(人前列腺癌雄激素非反应性 DU-145 细胞和大鼠星形胶质细胞原代培养物)的可能细胞毒性。

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