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首页> 外文期刊>Journal of Controlled Release: Official Journal of the Controlled Release Society >The origin of neural stem cells impacts their interactions with targeted-lipid nanocapsules: Potential role of plasma membrane lipid composition and fluidity
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The origin of neural stem cells impacts their interactions with targeted-lipid nanocapsules: Potential role of plasma membrane lipid composition and fluidity

机译:神经干细胞的起源会影响它们与靶向脂质纳米胶囊的相互作用:血浆膜脂质组合物和流动性的潜在作用

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摘要

The adsorption of a peptide (NFL-TBS.40-63 peptide (NFL)) known to induce neural stem cells (NSC) differentiation in vitro, at the surface of lipid nanocapsules (LNC) provides a targeting drug delivery system (NFL-LNC) that penetrates subventricular zone-neural stem cells (SVZ-NSC) but not central canal-NSC (CC-NSC). We hypothesized preferential interactions could explaine, at least partially, the different properties of SVZ- and CC-NSC plasma membranes. The objective of this work was to compare SVZ- and CC-NSC plasma membrane lipid composition, fluidity and permeability. Plasma membranes of SVZ- and CC-NSC were isolated and analyzed by LC-MS for their lipid content. Membrane fluidity was evaluated by measuring the generalized polarization (GP) of Laurdan and membrane permeability by fluorescent dextran penetration. Liposomes with different lipid compositions and steady state fluidities were prepared. AGP was measured after incubation with NFL-LNC. A significantly higher proportion of cholesterol, ceramides, sphingomyelins, phosphatidylethanolamines and a lower proportion of phosphatidylcholines and sulfatides were observed in SVZ-compared to CC-NSC. Fluidity, probably more than lipid composition, drove NFL-LNC and NSC interactions, and SVZ-NSC were more sensitive to NFL permeabilization than CC-NSC. We demonstrated that NSC membrane lipid composition and fluidity depended of NSC origin and that these features could play a role in the specific interactions with NFL-LNC.
机译:已知肽(NFL-TBS.40-63肽(NFL))在脂质纳米腐植物(LNC)表面上诱导神经干细胞(NSC)分化的肽(NFL-TBS.40-63肽(NFL))提供靶向药物递送系统(NFL-LNC )渗透细分区域 - 神经干细胞(SVZ-NSC),但不是中央管道 - NSC(CC-NSC)。我们假设的优先相互作用可以至少部分地解释SVZ-和CC-NSC血浆膜的不同性质。这项工作的目的是比较SVZ和CC-NSC血浆膜脂质组合物,流动性和渗透性。分离SVZ-和CC-NSC的血浆膜,并通过LC-MS分析它们的脂质含量。通过荧光葡聚糖渗透测量劳丹的广义极化(GP)和膜渗透率来评价膜流动性。制备具有不同脂质组合物和稳态流动性的脂质体。与NFL-LNC孵育后测量AGP。与CC-NSC相比,在SVZ与CC-NSC相比,在SVZ与CC-NSC相比,观察到显着较高比例的胆固醇,神经酰胺,鞘氨酰胺,磷脂酰乙醇胺和磷脂酰胆碱和硫酸盐的较低比例。流动性,可能大于脂质组合物,驱动NFL-LNC和NSC相互作用,并且SVZ-NSC比CC-NSC更敏感。我们证明NSC膜脂质组合物和流动性依赖于NSC来源,并且这些特征可以在与NFL-LNC的特定相互作用中发挥作用。

著录项

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  • 作者单位

    Catholic Univ Louvain UCLouvain Louvain Drug Res Inst Adv Drug Delivery &

    Biomat Ave E Mounier 73 B-1200 Brussels Belgium;

    Catholic Univ Louvain UCLouvain Louvain Drug Res Inst Cellular &

    Mol Pharmacol Ave E Mounier 73 B-1200 Brussels Belgium;

    Catholic Univ Louvain UCLouvain Louvain Drug Res Inst Bioanal &

    Pharmacol Bioact Lipids Ave E Mounier 73 B-1200 Brussels Belgium;

    Catholic Univ Louvain UCLouvain Louvain Drug Res Inst Bioanal &

    Pharmacol Bioact Lipids Ave E Mounier 73 B-1200 Brussels Belgium;

    Univ Angers Unite Micro &

    Nanomed Translationelles UMR INSERM Inst Biol Sante PBH IRIS CHU Angers F-49033 Angers France;

    Univ Angers Unite Micro &

    Nanomed Translationelles UMR INSERM Inst Biol Sante PBH IRIS CHU Angers F-49033 Angers France;

    Catholic Univ Louvain UCLouvain Louvain Drug Res Inst Adv Drug Delivery &

    Biomat Ave E Mounier 73 B-1200 Brussels Belgium;

    Catholic Univ Louvain UCLouvain Louvain Drug Res Inst Bioanal &

    Pharmacol Bioact Lipids Ave E Mounier 73 B-1200 Brussels Belgium;

    Catholic Univ Louvain UCLouvain Louvain Drug Res Inst Cellular &

    Mol Pharmacol Ave E Mounier 73 B-1200 Brussels Belgium;

    Catholic Univ Louvain UCLouvain Louvain Drug Res Inst Adv Drug Delivery &

    Biomat Ave E Mounier 73 B-1200 Brussels Belgium;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 药学;
  • 关键词

    Fluidity; Lipid composition; Lipid nanocapsules; Neural stem cells; NFL-TBS.40-63; Permeability; Plasma membrane;

    机译:流动性;脂质组合物;脂质纳米胶囊;神经干细胞;NFL-TBS.40-63;渗透率;血浆膜;

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