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Oriented Assembly of Cell-Mimicking Nanoparticles via a Molecular Affinity Strategy for Targeted Drug Delivery

机译:通过分子亲和力策略对靶向药物递送的分子亲和力策略为定向组装纳米粒子

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摘要

Cell membrane cloaking is an emerging field in drug delivery in which specific functions of parent cells are conferred to newly formed biomimetic vehicles. A growing variety of delivery systems with diverse surface properties have been utilized for this strategy, but it is unclear whether the affinity of membrane core pairs could guarantee effective and proper camouflaging. In this study, we propose a concise and effective "molecular affinity" strategy using the intracellular domain of transmembrane receptors as "grippers" during membrane coating. Red blood cell (RBC) membranes and cationic liposomes were adopted for fabrication, and a peptide ligand derived from the cytoplasmic protein P4.2 was prepared to specifically recognize the cytoplasmic domain of band 3, a key transmembrane receptor of erythrocytes. Once anchored onto the liposome surface, the P4.2-derived peptide would interact with the isolated RBC membrane, forming a "hidden peptide button", which ensures the right-side-out orientation. The membrane-coated liposomes exhibited an appropriate size distribution around 100 nm and high stability, with superior circulation durations compared with those of conventional PEGylated liposomes. Importantly, they possessed the ability to target Candida albicans by the interaction between the pathogenic fungus and host erythrocytes and to neutralize hemotoxin secreted by the pathogenic fungi. The curative effect of the model drug was thus substantially improved. In summary, the "molecular affinity" strategy may provide a powerful and universal approach for the construction of cell membrane-coated biomaterials and nanomedicines at both laboratory and industrial scales.
机译:细胞膜粘附是药物递送中的新出现的田间,其中母细胞的特定功能被赋予新形成的仿生载体。已经利用了具有多种表面性质的多种递送系统,但是该策略已经利用,但目前尚不清楚膜芯对的亲和力是否可以保证有效和适当的伪装。在本研究中,我们提出了一种简洁有效的“分子亲和力”策略,使用跨膜受体的细胞内结构域作为膜涂层期间的“夹持器”。采用红细胞(RBC)膜和阳离子脂质体用于制造,并制备衍生自细胞质蛋白P4.2的肽配体,以特异性地识别带3的细胞质结构域,是红细胞的关键跨膜受体。一旦锚定到脂质体表面,P4.2衍生的肽就会与分离的RBC膜相互作用,形成“隐藏肽按钮”,这确保了右侧取向。膜涂覆的脂质体显示出约100nm和高稳定性的适当尺寸分布,与常规聚乙二醇化脂质体相比具有优异的循环持续时间。重要的是,它们具有通过致病性真菌和宿主红细胞之间的相互作用来靶向念珠菌醛糖的能力,并通过致病真菌分泌的血红素毒素中和。因此基本上改善了模型药物的疗效。总之,“分子亲和力”策略可以在实验室和工业尺度的构建中施工细胞膜涂层生物材料和纳米喂养的态度。

著录项

  • 来源
    《ACS nano》 |2019年第5期|共10页
  • 作者单位

    Southwest Univ Coll Pharmaceut Sci Minist Educ Key Lab Luminescent &

    Real Time Analyt Chem Chongqing 400715 Peoples R China;

    Shanghai Jiao Tong Univ Renji Hosp Sch Med Shanghai 200032 Peoples R China;

    Southwest Univ Coll Pharmaceut Sci Minist Educ Key Lab Luminescent &

    Real Time Analyt Chem Chongqing 400715 Peoples R China;

    Southwest Univ Coll Pharmaceut Sci Minist Educ Key Lab Luminescent &

    Real Time Analyt Chem Chongqing 400715 Peoples R China;

    Southwest Univ Coll Pharmaceut Sci Minist Educ Key Lab Luminescent &

    Real Time Analyt Chem Chongqing 400715 Peoples R China;

    Chongqing Gen Hosp Dept Clin Lab Chongqing 400014 Peoples R China;

    Southwest Univ Coll Pharmaceut Sci Minist Educ Key Lab Luminescent &

    Real Time Analyt Chem Chongqing 400715 Peoples R China;

    Southwest Univ Coll Pharmaceut Sci Minist Educ Key Lab Luminescent &

    Real Time Analyt Chem Chongqing 400715 Peoples R China;

    Southwest Univ Coll Pharmaceut Sci Minist Educ Key Lab Luminescent &

    Real Time Analyt Chem Chongqing 400715 Peoples R China;

    Southwest Univ Coll Pharmaceut Sci Minist Educ Key Lab Luminescent &

    Real Time Analyt Chem Chongqing 400715 Peoples R China;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 分子物理学、原子物理学;
  • 关键词

    biomimetics; red blood cell membranes; peptide ligand; targeted drug delivery; fungal infection;

    机译:生物体;红细胞膜;肽配体;靶向药物递送;真菌感染;

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