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首页> 外文期刊>Carbohydrate Polymers: Scientific and Technological Aspects of Industrially Important Polysaccharides >N-Oxy lipid-based click chemistry for orthogonal coupling of mannan onto nanoliposomes prepared by microfluidic mixing: Synthesis of lipids, characterisation of mannan-coated nanoliposomes and in vitro stimulation of dendritic cells
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N-Oxy lipid-based click chemistry for orthogonal coupling of mannan onto nanoliposomes prepared by microfluidic mixing: Synthesis of lipids, characterisation of mannan-coated nanoliposomes and in vitro stimulation of dendritic cells

机译:基于氧化脂质的甘露甘露脂合酶在微流体混合制备的纳米脂质上的正交耦合:脂质的合成,甘露植物纳米脂质体的表征和树突细胞的体外刺激

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摘要

New synthetic aminooxy lipid was designed and synthesized as a building block for the formulation of functionalised nanoliposomes (presenting onto the outer surface of aminooxy groups) by microfluidic mixing. Orthogonal binding of cellular mannan (Candida glabrata (CCY 26-20-1) onto the outer surface of functionalised nanoliposomes was modified by orthogonal binding of reducing termini of mannans to oxime lipids via a click chemistry reaction based on aminooxy coupling (oxime ligation). The aminooxy lipid was proved as a suitable active component for preparation of functionalised nanoliposomes by the microfluidic mixing method performed with the instrument NanoAssemblr T. This "on-chip technology" can be easily scaled-up. The structure of mannan-liposomes was visualized by transmission and scanning electron microscopy, including immunogold staining of recombinant mannan receptor bound onto mannosylated-liposomes. The observed structures are in a good correlation with data obtained by DLS, NTA, and TPRS methods. In vitro experiments on human and mouse dendritic cells demonstrate selective internalisation of fluorochrome-labelled mannan-liposomes and their ability to stimulate DC comparable to lipopolysaccharide. We describe a potentially new drug delivery platform for mannan receptor-targeted antimicrobial drugs as well as for immunotherapeutics. Furthermore, the platform based on mannans bound orthogonally onto the surface of nanoliposomes represents a self-adjuvanted carrier for construction of liposome-based recombinant vaccines for both systemic and mucosal routes of administration.
机译:设计并合成了新的合成氨基氧基脂质,作为通过微流体混合制定官能化纳米脂质(呈上氨基氧基外表道)的结构嵌段。通过基于氨基氧基偶联的氨氧基偶联(Oxime连接)通过咔哒化化学反应将甘露出的末端与肟脂质的正交结合进行正交结合来改变细胞甘露群(Cycya Glabrata(Ccy 26-20-1)的正交结合。被证明氨基氧基脂质作为合适的活性组分,通过用仪器纳米可融合方法进行微流体混合方法制备官能化的纳米体。这种“片上技术”可以很容易地缩放。甘露脂质体的结构被视为透射和扫描电子显微镜,包括将重组甘露聚糖受体的免疫染色染色在甘露糖苷化 - 脂质体上。观察到的结构与DLS,NTA和TPRS方法获得的数据具有良好的相关性。人和小鼠树突细胞的体外实验表明选择性荧光染料标记的甘露脂质体的内化及其刺激直流比较T的能力o脂多糖。我们描述了甘露受体靶向抗微生物药物以及免疫治疗的潜在新的药物递送平台。此外,基于正交结合的甘露甘油族在纳米脂质表面上结合到纳米脂质的表面的平台代表了用于构建脂质体的重组疫苗的自佐载体,用于全身和粘膜给药途径。

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