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首页> 外文期刊>Bioconjugate Chemistry >Dual Site-Selective Presentation of Functional Handles on Protein-Engineered Cowpea Chlorotic Mottle Virus-Like Particles
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Dual Site-Selective Presentation of Functional Handles on Protein-Engineered Cowpea Chlorotic Mottle Virus-Like Particles

机译:蛋白质工程豇豆氯化斑块病毒样颗粒上功能手柄的双位点选择性呈现

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摘要

Protein cages hold much promise as carrier systems in nanomedicine, due to their well-defined size, cargo-loading capacity, and inherent biodegradability. In order to make them suitable for drug delivery, they have to be stable under physiological conditions. In addition, often surface modifications are required, for example, to improve cell targeting or reduce the particle immunogenicity by PEGylation. For this purpose, we investigated the functionalization capacity of the capsid of cowpea chlorotic mottle virus (CCMV), modified at the interior with a stabilizing elastinlike polypeptide (ELP) tag, by employing a combination of protein engineering and bio-orthogonal chemistry. We first demonstrated the accessibility of the native cysteine residue in ELP-CCMV as a site-selective surface-exposed functional handle, which was not available in the native CCMV capsid. An additional bio-orthogonal functional handle was introduced by incorporation of the noncanonical amino acid, azido-phenylalanine (AzF), using the amber suppression mechanism. Dual site-selective presentation of both a cell-penetrating TAT peptide and a fluorophore to track the particles was demonstrated successfully in HeLa cell uptake studies.
机译:由于其定义明确尺寸,货物负载能力和固有的生物降解性,蛋白质笼子作为纳米医生的承载系统承担了许多承担得多。为了使它们适合药物递送,它们必须在生理条件下保持稳定。另外,例如,需要通过聚乙二醇化改善细胞靶向或减少颗粒免疫原性的表面修饰。为此目的,我们研究了豇豆氯化斑块病毒(CCMV)的胶囊的官能化能力,通过采用蛋白质工程和生物正交化学的组合来在内部修饰。我们首先证明了ELP-CCMV本地半胱氨酸残基的可及性作为位点选择性表面暴露的功能手柄,其在天然CCMV衣壳中不可用。通过使用琥珀抑制机制掺入非甘露糖氨基酸,氮杂苯丙氨酸(AZF)来引入另外的生物正交功能手柄。在HeLa细胞摄取研究中成功地证明了一种细胞穿透Tat肽和荧光团的双位点选择性呈递追踪颗粒。

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