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靶向再循环内体以增强 mRNA 脂质纳米颗粒。

Targeting Recycling Endosomes to Potentiate mRNA Lipid Nanoparticles.

机构信息

Department of Molecular Physiology and Biological Physics, University of Virginia, 480 Ray C. Hunt Drive, Charlottesville, 22903 Virginia, United States.

Department of Molecular Medicine, UF Scripps Biomedical Research, 130 Scripps Way, Jupiter, 33458 Florida, United States.

出版信息

Nano Lett. 2024 May 1;24(17):5104-5109. doi: 10.1021/acs.nanolett.3c04415. Epub 2024 Apr 19.

Abstract

mRNA lipid nanoparticles (LNPs) have emerged as powerful modalities for gene therapies to control cancer and infectious and immune diseases. Despite the escalating interest in mRNA-LNPs over the past few decades, endosomal entrapment of delivered mRNAs vastly impedes therapeutic developments. In addition, the molecular mechanism of LNP-mediated mRNA delivery is poorly understood to guide further improvement through rational design. To tackle these challenges, we characterized LNP-mediated mRNA delivery using a library of small molecules targeting endosomal trafficking. We found that the expression of delivered mRNAs is greatly enhanced via inhibition of endocytic recycling in cells and in live mice. One of the most potent small molecules, endosidine 5 (ES5), interferes with recycling endosomes through Annexin A6, thereby promoting the release and expression of mRNA into the cytoplasm. Together, these findings suggest that targeting endosomal trafficking with small molecules is a viable strategy to potentiate the efficacy of mRNA-LNPs.

摘要

mRNA 脂质纳米颗粒(LNPs)已成为控制癌症、传染病和免疫疾病的基因治疗的强大手段。尽管在过去几十年中,mRNA-LNPs 的兴趣不断增加,但内体捕获递送的 mRNAs 极大地阻碍了治疗的发展。此外,LNP 介导的 mRNA 递送的分子机制了解甚少,无法通过合理设计进行进一步改进。为了解决这些挑战,我们使用针对内体运输的小分子文库来表征 LNP 介导的 mRNA 递送。我们发现,通过抑制细胞和活体小鼠中的内吞再循环,递送的 mRNAs 的表达大大增强。最有效的小分子之一,内索丁 5(ES5),通过 Annexin A6 干扰再循环内体,从而促进 mRNA 释放到细胞质中并表达。总之,这些发现表明,用小分子靶向内体运输是增强 mRNA-LNP 疗效的可行策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/81d0/11066955/70e9c6cbe9e3/nl3c04415_0001.jpg

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