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脂质体、金纳米颗粒和硒纳米颗粒中包封的环糊精对细胞培养基中siRNA稳定性的影响。

Effect of Cyclodextrins Formulated in Liposomes and Gold and Selenium Nanoparticles on siRNA Stability in Cell Culture Medium.

作者信息

Castillo Cruz Betzaida, Chinapen Barletta Sandra, Ortiz Muñoz Bryan G, Benitez-Reyes Adriana S, Amalbert Perez Omar A, Cardona Amador Alexander C, Vivas-Mejia Pablo E, Barletta Gabriel L

机构信息

Department of Chemistry, University of Puerto Rico at Humacao, Humacao 00791, Puerto Rico.

Department of Physiology/Pathology, San Juan Bautista School of Medicine, Caguas 00725, Puerto Rico.

出版信息

Pharmaceuticals (Basel). 2024 Oct 8;17(10):1344. doi: 10.3390/ph17101344.

Abstract

BACKGROUND

Encapsulation of siRNA fragments inside liposome vesicles has emerged as an effective method for delivering siRNAs in vitro and in vivo. However, the liposome's fluid-phospholipid bilayer of liposomes allows siRNA fragments to diffuse out of the liposome, decreasing the dose concentration and therefore the effectiveness of the carrier. We have previously reported that β-cyclodextrins formulated in liposomes help increase the stability of siRNAs in cell culture medium. Here, we continued that study to include α, γ, methyl-β-cyclodextrins and β-cyclodextrin-modified gold and selenium nanoparticles.

METHODS

We used Isothermal Titration Calorimetry to study the binding thermodynamics of siRNAs to the cyclodextrin-modified nanoparticles and to screen for the best adamantane derivative to modify the siRNA fragments, and we used gel electrophoresis to study the stabilization effect of siRNA by cyclodextrins and the nanoparticles.

RESULTS

We found that only β- and methyl-β-cyclodextrins increased siRNA serum stability. Cyclodextrin-modified selenium nanoparticles also stabilize siRNA fragments in serum, and siRNAs chemically modified with an adamantane moiety (which forms inclusion complexes with the cyclodextrin-modified-nanoparticles) show a strong stabilization effect.

CONCLUSIONS

β-cyclodextrins are good additives to stabilize siRNA in cell culture medium, and the thermodynamic data we generated of the interaction between cyclodextrins and adamantane analogs (widely used in drug delivery studies), should serve as a guide for future studies where cyclodextrins are sought for the delivery and solvation of small organic molecules.

摘要

背景

将小干扰RNA(siRNA)片段包裹在脂质体囊泡内已成为一种在体外和体内递送siRNA的有效方法。然而,脂质体的流体磷脂双分子层会使siRNA片段从脂质体中扩散出来,降低剂量浓度,进而降低载体的有效性。我们之前报道过,脂质体中配制的β-环糊精有助于提高siRNA在细胞培养基中的稳定性。在此,我们继续该研究,将α-、γ-、甲基-β-环糊精以及β-环糊精修饰的金和硒纳米颗粒纳入研究范围。

方法

我们使用等温滴定量热法研究siRNA与环糊精修饰纳米颗粒的结合热力学,并筛选出最佳的金刚烷衍生物来修饰siRNA片段;同时使用凝胶电泳研究环糊精和纳米颗粒对siRNA的稳定作用。

结果

我们发现只有β-环糊精和甲基-β-环糊精能提高siRNA在血清中的稳定性。环糊精修饰的硒纳米颗粒也能在血清中稳定siRNA片段,并且用金刚烷部分化学修饰的siRNA(其与环糊精修饰的纳米颗粒形成包合物)显示出很强的稳定作用。

结论

β-环糊精是在细胞培养基中稳定siRNA的良好添加剂,我们生成的环糊精与金刚烷类似物(广泛用于药物递送研究)之间相互作用的热力学数据,应为未来寻求环糊精用于小分子有机化合物递送和溶剂化的研究提供指导。

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