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Deconvoluting Lipid Nanoparticle Structure for Messenger RNA Delivery

机译:用于信使RNA递送的解促脂质纳米粒子结构

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Lipid nanoparticle (LNP) packaged mRNA vaccines have been deployed against infectious diseases such as COVID-19, yet their structural features remain unclear. Cholesterol, a major constituent within LNPs, contributes to their morphology that influences gene delivery. Herein, we examine the structure of LNPs containing cholesterol derivatives using electron microscopy, differential scanning calorimetry, and membrane fluidity assays. LNPs formulated with C24 alkyl derivatives of cholesterol show a polymorphic shape and various degrees of multilamellarity and lipid partitioning, likely due to phase separation. The addition of methyl and ethyl groups to the C24 alkyl tail of the cholesterol backbone induces multilamellarity (>50% increase compared to cholesterol), while the addition of a double bond induces lipid partitioning (>90% increase compared to cholesterol). LNPs with multilamellar and faceted structures, as well as a lamellar lipid phase, showed higher gene transfection. Unraveling the structure of mRNA-LNPs can enable their rational design toward enhanced gene delivery.
机译:脂质纳米粒子(LNP)包装的mRNA疫苗已针对Covid-19等传染病部署,但它们的结构特征仍然尚不清楚。 LNPS内的主要成分胆固醇,有助于影响基因递送的形态。在此,我们使用电子显微镜,差示扫描量热法和膜流动测定来检查含有胆固醇衍生物的LNP的结构。用C24烷基衍生物配制的LNP显示出多态性形状和各种多层的多功能性和脂质分配,可能是由于相分离。将甲基和乙基添加到胆固醇骨架的C24烷基尾部诱导多层(与胆固醇相比)的多层(> 50%的增加),同时添加双键诱导脂质分配(与胆固醇相比增加90%)。 LNP具有多岩石和刻面结构,以及层状脂质阶段,显示出更高的基因转染。解开mRNA-LNP的结构可以使其合理设计趋向增强基因递送。

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