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Cationic Nanoliposomes Meet mRNA: Efficient Delivery of Modified mRNA Using Hemocompatible and Stable Vectors for Therapeutic Applications

机译:阳离子纳米脂质体符合mRNA:使用可用于治疗应用的血液相容性和稳定载体有效地传递修饰的mRNA

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摘要

Synthetically modified mRNA is a unique bioactive agent, ideal for use in therapeutic applications, such as cancer vaccination or treatment of single-gene disorders. In order to facilitate mRNA transfections for future therapeutic applications, there is a need for the delivery system to achieve optimal transfection efficacy, perform with durable stability, and provide drug safety. The objective of our study was to comprehensively analyze the use of 3β-[N-(N',N'-dimethylaminoethane) carbamoyl](DC-Cholesterol)/dioleoylphosphatidylethanolamine (DOPE) liposomes as a potential transfection agent for modified mRNAs. Our cationic liposomes facilitated a high degree of mRNA encapsulation and successful cell transfection efficiencies. More importantly, no negative effects on cell viability or immune reactions were detected posttransfection. Notably, the liposomes had a long-acting transfection effect on cells, resulting in a prolonged protein production of alpha-1-antitrypsin (AAT). In addition, the stability of these mRNA-loaded liposomes allowed storage for 80 days, without the loss of transfection efficacy. Finally, comprehensive analysis showed that these liposomes are fully hemocompatible with fresh human whole blood. In summary, we present an extensive analysis on the use of DC-cholesterol/DOPE liposomes as mRNA delivery vehicles. This approach provides the basis of a safe and efficient therapeutic strategy in the development of successful mRNA-based drugs.
机译:合成修饰的mRNA是一种独特的生物活性剂,非常适合用于治疗应用,例如癌症疫苗接种或单基因疾病的治疗。为了促进mRNA转染用于未来的治疗应用,需要递送系统以实现最佳的转染功效,具有持久的稳定性并提供药物安全性。我们研究的目的是全面分析3β-[N-(N',N'-二甲基氨基乙烷)氨基甲酰基](DC-胆固醇)/油酰磷脂酰乙醇胺(DOPE)脂质体作为修饰的mRNA的潜在转染剂的用途。我们的阳离子脂质体促进了高度的mRNA封装和成功的细胞转染效率。更重要的是,转染后未检测到对细胞活力或免疫反应的负面影响。值得注意的是,脂质体对细胞具有长效转染作用,导致α-1-抗胰蛋白酶(AAT)的蛋白质产生时间延长。此外,这些装有mRNA的脂质体的稳定性可以保存80天,而不会损失转染效果。最后,全面分析表明,这些脂质体与新鲜的人类全血具有完全的血液相容性。总之,我们对使用DC胆固醇/ DOPE脂质体作为mRNA传递载体进行了广泛的分析。这种方法为成功开发基于mRNA的药物提供了安全有效的治疗策略的基础。

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