Membrane fusogenic high-density lipoprotein nanoparticles |
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Authors: | Hyungjin Kim Tomohiro Nobeyama Shinnosuke Honda Kaori Yasuda Nobuhiro Morone Tatsuya Murakami |
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Abstract: | ![]() 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. |
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Keywords: | Corresponding author at: Department of Biotechnology, Graduate School of Engineering, Toyama Prefectural University, 5180 Kurokawa, Imizu, Toyama 939-0398, Japan. apoA-I apolipoprotein A-I CHEMS cholesteryl hemisuccinate Chol cholesterol CPP cell-penetrating peptide DOPC DOPE DOPS DPH 1,6-diphenyl-1,3,5-hexatriene DPPC EM electron microscopy FRET förster resonance energy transfer 340 generalized polarization NBD-DPPE RhoB octadecyl rhodamine B chloride Rho-DPPE SOPC TAT a cell-penetrating peptide of human immunodeficiency virus Tat protein Lipoproteins Cell-penetrating peptide Lipid mixing Mildly acidic pH |
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