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具有支链连接子的可电离脂质增强mRNA疫苗的递送。

Ionizable Lipids with Branched Linkers Enhance the Delivery of mRNA Vaccines.

作者信息

Liu Jiwei, Sun Wenjing, Xiao Bing, Xu Haoran, Fan Jiaqi, Shi Xueying, Pan Yixuan, Wei Qi, Li Ruoshui, Wang Huimin, Piao Ying, Xiang Jiajia, Shao Shiqun, Zhou Zhuxian, Shen Youqing, Tang Jianbin

机构信息

Zhejiang Key Laboratory of Smart Biomaterials, College of Chemical and Biological Engineering, Zhejiang University, Hangzhou, Zhejiang 310058, P. R. China.

ZJU-Hangzhou Global Scientific and Technological Innovation Center, Zhejiang University, Hangzhou, Zhejiang 311200, P. R. China.

出版信息

ACS Appl Mater Interfaces. 2025 Mar 5;17(9):13552-13564. doi: 10.1021/acsami.4c21289. Epub 2025 Feb 20.

Abstract

The emergence of mRNA vaccines has heralded an epoch in disease prevention and treatment. Safe and efficient mRNA delivery systems are highly desired for the widespread application of mRNA therapeutics. Herein, we have designed a facile synthetic pathway for producing ionizable lipids featuring various branched linkers. These lipids have been integrated into lipid nanoparticles (LNPs) to improve the delivery of mRNA vaccines. The influence of linker structure on lipids and LNPs is currently underreported, yet it undeniably exerts a substantial impact on the outcomes. Through systematic screening and formulation optimization, we have identified that LNPs comprising ionizable lipids with a branched β-isobutylglutarate linker (bLNPs) exhibited superior transfection capabilities. In preclinical cancer prevention and treatment models, mRNA vaccines delivered by bLNPs (mRNA-bLNPs) have shown significant efficacy without causing systemic toxicity, highlighting the potential of bLNPs for clinical translation. Our synthetic strategy facilitates the expansion of the LNP library and provides valuable insights into the relationship between linker structures and delivery efficiency, thereby propelling the advancement of LNP technology.

摘要

mRNA疫苗的出现开创了疾病预防和治疗的新纪元。安全高效的mRNA递送系统对于mRNA疗法的广泛应用至关重要。在此,我们设计了一种简便的合成途径,用于生产具有各种支链连接子的可电离脂质。这些脂质已被整合到脂质纳米颗粒(LNPs)中,以改善mRNA疫苗的递送。连接子结构对脂质和LNPs的影响目前报道较少,但它无疑对结果产生重大影响。通过系统筛选和配方优化,我们发现包含具有支链β-异丁基戊二酸连接子的可电离脂质的LNPs(bLNPs)表现出卓越的转染能力。在临床前癌症预防和治疗模型中,由bLNPs递送的mRNA疫苗(mRNA-bLNPs)已显示出显著疗效,且不会引起全身毒性,凸显了bLNPs临床转化的潜力。我们的合成策略有助于扩大LNP文库,并为连接子结构与递送效率之间的关系提供有价值的见解,从而推动LNP技术的进步。

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