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Design, syntheses, and Transfection biology of novel non-cholesterol-based guanidinylated cationic lipids

机译:新型非胆固醇基胍基化阳离子脂质的设计,合成和转染生物学

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摘要

The design of efficacious cationic transfection lipids with guanidinium headgroups is an actively pursued area of research in nonviral gene delivery. Herein, we report on the design, syntheses, and gene transfection properties of six novel non-cholesterol-based cationic amphiphiles (1-6) with a single guanidinium headgroup in transfecting CHO, COS-1, MCF-7, A549, and HepG2 cells. The in vitro gene transfer efficiencies of lipids 1-6 were evaluated using both the reporter gene and the whole cell histochemical X-gal staining assays. The efficiencies of lipids 1-3, in particular, were found to be about 2- to 4-fold higher than that of commercially available LipofectAmine in transfecting COS-1, CHO, A-549, and MCF-7 cells. However, the relative transfection efficiencies of lipids 1-3 and LipofectAmine were found to be comparable in HepG2 cells. Cholesterol was found to be a more efficacious co-lipid than dioleoyllphosphatidyl ethanolamine (DOPE). In general, lipids 1-3 containing the additional quaternized centers were observed to be more transfection efficient than lipids 4-6 with less positive headgroups. MTT-assay-based cell viability measurements in representative CHO cells revealed high (>75%) cell viabilities of lipids 1-6 across the lipid/DNA charge ratios 0.1:1 to 3:1. Electrophoretic gel patterns observed in DNase I protection experiments support the notion that enhanced degradation of DNA associated with lipoplexes of lipids 4-6 might play some role in diminishing their in vitro gene transfer efficacies. Size and global surface charge measurement by a dynamic laser light scattering instrument equipped with xi-sizing capacity revealed the nanosizes and surface potentials of both the transfection efficient and the incompetent lipoplexes to be within the range of 200-600 nm and +3.4 to -34 mV, respectively. To summarize, given the feasibility of a wide range of structural manipulations in the headgroup regions of non-cholesterol-based cationic amphiphiles, our present findings are expected to broaden the potential of cationic amphiphiles with guanidinium headgroups for use in nonviral gene therapy.
机译:具有胍基头基的有效阳离子转染脂质的设计是非病毒基因递送研究的一个积极追求的领域。在这里,我们报告的设计,合成和基因转染特性的六个新颖的非胆固醇基阳离子两亲物(1-6)与单个胍基头基团在转染CHO,COS-1,MCF-7,A549和HepG2中细胞。使用报告基因和全细胞组织化学X-gal染色法评估了脂质1-6的体外基因转移效率。特别是,在转染COS-1,CHO,A-549和MCF-7细胞中,脂质1-3的效率比市售LipofectAmine约高2-4倍。然而,发现脂质1-3和LipofectAmine的相对转染效率在HepG2细胞中相当。发现胆固醇比二油基磷脂酰乙醇胺(DOPE)更有效的共脂质。通常,观察到含有额外季铵化中心的脂质1-3比具有较少阳性首基的脂质4-6具有更高的转染效率。在代表性的CHO细胞中,基于MTT分析的细胞活力测定显示,脂质1-6在脂质/ DNA电荷比为0.1:1至3:1时具有高(> 75%)的细胞活力。在DNase I保护实验中观察到的电泳凝胶模式支持以下观念,即与脂质4-6的脂质复合物相关的DNA降解增强可能在降低其体外基因转移效率中起一定作用。通过配备xi-sizing容量的动态激光散射仪进行大小和整体表面电荷测量,发现转染效率和不适合的脂质复合物的纳米尺寸和表面电势均在200-600 nm和+3.4至-34范围内mV,分别。综上所述,鉴于在非胆固醇类阳离子两亲物的头基区域进行广泛的结构操作的可行性,我们目前的发现有望扩大具有胍基头基的阳离子两亲物在非病毒基因治疗中的潜力。

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