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两性离子聚合物功能化脂质纳米颗粒用于 mRNA 的雾化递药。

Zwitterionic Polymer-Functionalized Lipid Nanoparticles for the Nebulized Delivery of mRNA.

机构信息

Department of Chemical Engineering, Massachusetts Institute of Technology, Cambridge, Massachusetts 02139, United States.

David H Koch Institute for Integrative Cancer Research, Massachusetts Institute of Technology, Cambridge, Massachusetts 02139, United States.

出版信息

J Am Chem Soc. 2024 Nov 27;146(47):32567-32574. doi: 10.1021/jacs.4c11347. Epub 2024 Nov 13.

Abstract

Lipid nanoparticles (LNPs) have great potential to enable inhaled delivery of mRNA to treat pulmonary diseases. However, this potential has been limited by the challenge of nebulizing the LNPs. Nebulization of LNPs can cause LNPs to aggregate and release encapsulated mRNA, limiting their delivery efficacy. To overcome this challenge, LNPs are developed whereby the PEG-lipid is fully replaced with a zwitterionic polymer (ZIP)-lipid conjugate to greatly enhance the nebulizer stability. LNPs formulated with ZIP-lipids (ZIP-LNPs) were stable to nebulization across a wide range of formulation parameters. The optimized ZIP-LNP formulation, containing reduced cholesterol content relative to traditional PEG-lipid LNPs, demonstrated improved inhaled mRNA delivery in both healthy and mucoobstructed mouse lungs. Repeat administration of the optimized ZIP-LNP formulation was well tolerated and did not result in pulmonary inflammation. This study demonstrates the potential of zwitterionic polymer-lipid conjugates for improving the performance of inhaled mRNA-LNP formulations.

摘要

脂质纳米颗粒(LNPs)具有将 mRNA 递送至肺部疾病部位的巨大潜力。然而,这一潜力受到了将 LNPs 雾化的挑战的限制。LNPs 的雾化会导致 LNPs 聚集并释放包裹的 mRNA,从而限制了它们的递药效果。为了克服这一挑战,开发了 LNPs,其中 PEG 脂质完全被两性离子聚合物(ZIP)-脂质缀合物取代,以极大地增强雾化器稳定性。ZIP-脂质(ZIP-LNP)包封的 LNPs 在广泛的制剂参数范围内都具有稳定的雾化性。与传统的 PEG-脂质 LNPs 相比,含有降低胆固醇含量的优化 ZIP-LNP 制剂在健康和粘液阻塞的小鼠肺部中显示出改善的吸入 mRNA 递药效果。优化的 ZIP-LNP 制剂的重复给药具有良好的耐受性,并且不会导致肺部炎症。本研究证明了两性离子聚合物-脂质缀合物在改善吸入 mRNA-LNP 制剂性能方面的潜力。

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