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阳离子脂质介导的自扩增复制子RNA向树突状细胞的递送

Self-Amplifying Replicon RNA Delivery to Dendritic Cells by Cationic Lipids.

作者信息

Englezou Pavlos C, Sapet Cedric, Démoulins Thomas, Milona Panagiota, Ebensen Thomas, Schulze Kai, Guzman Carlos-Alberto, Poulhes Florent, Zelphati Olivier, Ruggli Nicolas, McCullough Kenneth C

机构信息

Institute of Virology and Immunology (IVI), Mittelhäusern 3147, Switzerland.

OZ Biosciences, Case 922, Marseille, France.

出版信息

Mol Ther Nucleic Acids. 2018 Sep 7;12:118-134. doi: 10.1016/j.omtn.2018.04.019. Epub 2018 May 4.

Abstract

Advances in RNA technology during the past two decades have led to the construction of replication-competent RNA, termed replicons, RepRNA, or self-amplifying mRNA, with high potential for vaccine applications. Cytosolic delivery is essential for their translation and self-replication, without infectious progeny generation, providing high levels of antigen expression for inducing humoral and cellular immunity. Synthetic nanoparticle-based delivery vehicles can both protect the RNA molecules and facilitate targeting of dendritic cells-critical for immune defense development. Several cationic lipids were assessed, with RepRNA generated from classical swine fever virus encoding nucleoprotein genes of influenza A virus. The non-cytopathogenic nature of the RNA allowed targeting to dendritic cells without destroying the cells-important for prolonged antigen production and presentation. Certain lipids were more effective at delivery and at promoting translation of RepRNA than others. Selection of particular lipids provided delivery to dendritic cells that resulted in translation, demonstrating that delivery efficiency could not guarantee translation. The observed translation in vitro was reproduced in vivo by inducing immune responses against the encoded influenza virus antigens. Cationic lipid-mediated delivery shows potential for promoting RepRNA vaccine delivery to dendritic cells, particularly when combined with additional delivery elements.

摘要

在过去二十年中,RNA技术的进步促使了具有复制能力的RNA的构建,这种RNA被称为复制子、RepRNA或自我扩增mRNA,在疫苗应用方面具有很高的潜力。胞质递送对于它们的翻译和自我复制至关重要,且不会产生感染性后代,能提供高水平的抗原表达以诱导体液免疫和细胞免疫。基于合成纳米颗粒的递送载体既能保护RNA分子,又有助于靶向树突状细胞——这对免疫防御发展至关重要。研究评估了几种阳离子脂质,用编码甲型流感病毒核蛋白基因的经典猪瘟病毒产生RepRNA。RNA的非细胞致病性使得其能够靶向树突状细胞而不破坏细胞——这对于延长抗原产生和呈递很重要。某些脂质在递送和促进RepRNA翻译方面比其他脂质更有效。选择特定脂质可实现向树突状细胞的递送并导致翻译,这表明递送效率并不能保证翻译。通过诱导针对编码流感病毒抗原的免疫反应,在体内重现了体外观察到的翻译情况。阳离子脂质介导的递送显示出促进RepRNA疫苗递送至树突状细胞的潜力,特别是与其他递送元件结合时。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/842d/6023837/e52e0909b2f3/gr1.jpg

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