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首页> 外文期刊>Journal of Controlled Release: Official Journal of the Controlled Release Society >A facile approach to functionalizing cell membrane-coated nanoparticles with neurotoxin-derived peptide for brain-targeted drug delivery
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A facile approach to functionalizing cell membrane-coated nanoparticles with neurotoxin-derived peptide for brain-targeted drug delivery

机译:用神经毒素衍生肽官能化细胞膜涂覆纳米粒子的容易方法,用于脑靶向药物递送

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AbstractThe blood brain barrier separates the circulating blood from the extracellular fluid in the central nervous system and thus presents an essential obstacle to brain transport of therapeutics. Herein, we report on an effective brain-targeted drug delivery system that combines a robust red blood cell membrane-coated nanoparticle (RBCNP) with a unique neurotoxin-derived targeting moiety. The RBCNPs retain the complex biological functions of natural cell membranes while exhibiting physicochemical properties that are suitable for effective drug delivery. CDX peptide is derived from candoxin and shows high binding affinity with nicotinic acetylcholine receptors (nAChRs) expressed on the surface of brain endothelial cells. Through a facile yet robust approach, we successfully incorporateDCDX peptides onto the surface of RBCNPs without compromising the peptide's brain targeting ability. The resultingDCDX-RBCNPs show promising brain targeting efficiency bothin vitroandin vivo. Using a glioma mouse model, we demonstrate that doxorubicin-loadedDCDX-RBCNPs have superior therapeutic efficacy and markedly reduced toxicity as compared to the nontargeted drug formulations. While RBCNPs are used as a model system to evaluate the surface modification approach, the reported method can be readily generalized to various types of cell membrane-derived nanocarriers for broad medical applications.
机译:<![cdata [ 抽象 血脑屏障将循环血液与中枢神经系统中的细胞外液分开,从而提出了一个必要的障碍脑脑运输治疗。在此,我们报告了一种有效的脑靶向药物递送系统,其将稳健的红细胞膜涂覆的纳米颗粒(RBCNP)与独特的神经毒素衍生的靶向部分结合在一起。 RBCNPS保留了天然细胞膜的复杂生物功能,同时表现出适合有效药物递送的物理化学性质。 CDX肽衍生自Candoxin,并在脑内皮细胞表面表达的烟碱乙酰胆碱受体(NACHR)具有高结合亲和力。通过易于较强的方法,我们成功地将 d cdx肽在RBCNPS的表面上并不损害肽的脑靶向能力。得到的 d cdx-rbcnps显示有前途的脑靶向效率在体外在vivo < / ce:斜体>。使用胶质瘤小鼠模型,我们证明了加载了多柔比蛋白的 D cdx-rbcnps具有优异的治疗效果,并且与不靶向药物制剂相比显着降低毒性。虽然RBCNP用作型号系统以评估表面改性方法,但是报告的方法可以容易地广泛地推广到广泛的医疗应用的各种类型的细胞膜衍生的纳米载体。

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