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Membrane fusogenic high-density lipoprotein nanoparticles

机译:膜致密性高密度脂蛋白纳米粒子

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摘要

Membrane fusion under mildly acidic pH occurs naturally during viral infection in cells and has been exploited in the field of nanoparticle-mediated drug delivery to circumvent endosomal entrapment of the cargo. Herein, we aimed to confer virus-like fusogenic activity to HDL in the form of a ca. 10-nm disc comprising a discoidal lipid bilayer and two copies of a lipid-binding protein at the edge. A series of HDL mutants were prepared with a mixture of three lipids and a cell-penetrating peptide (TAT, penetratin, or Arg8) fused to the protein. In a lipid-mixing assay with anionic liposomes at pH 5.5, one HDL mutant showed the fusogenic activity higher than known fusogenic liposomes. In live mammalian cells, this HDL mutant showed high plasma membrane-binding activity in the presence of serum independent of pH. In the absence of serum, a mildly acidic pH dependency for binding to the plasma membrane and the subsequent lipid mixing between them was observed for this mutant. We propose a novel strategy to develop HDL-based drug carriers by taking advantage of the HDL lipid/protein composite structure.
机译:在细胞病毒感染期间在轻微酸性pH下自然地发生膜融合,并且已经在纳米粒子介导的药物递送的领域中被利用,以避免货物的内体抑制。在此,我们旨在以CA的形式赋予病毒样致致致致致致致致沉菌活性至HDL。 10-nm圆盘,包括盘形脂质双层和在边缘处的脂质结合蛋白的两份拷贝。用三种脂质的混合物和融合到蛋白质的细胞穿透肽(TAT,Pepetratin或Arg8)的混合物制备一系列HDL突变体。在pH5.5的阴离子脂质体的脂混合测定中,一个HDL突变体显示出比已知的富含血糖体脂质体高的致融合活性。在活哺乳动物细胞中,该HDL突变体在血清含有与pH无血清存在下的高血浆膜结合活性。在没有血清的情况下,对于该突变体,观察到对血浆膜结合的温和酸性pH依赖性以及它们之间的随后的脂质混合。我们提出了一种通过利用HDL脂/蛋白质复合结构来开发基于HDL的药物载体的新策略。

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