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Bacteriophage PRD1 as a nanoscaffold for drug loading

机译:噬菌体PRD1 nanoscaffold作为药物加载

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Viruses are very attractive biomaterials owing to their capability as nanocarriers of genetic material. Efforts have been made to functionalize self-assembling viral protein capsids on their exterior or interior to selectively take up different payloads. PRD1 is a double-stranded DNA bacteriophage comprising an icosahedral protein outer capsid and an inner lipidic vesicle. Here, we report the three-dimensional structure of PRD1 in complex with the antipsychotic drug chlorpromazine (CPZ) by cryo-electron microscopy. We show that the jellyrolls of the viral major capsid protein P3, protruding outwards from the capsid shell, serve as scaffolds for loading heterocyclic CPZ molecules. Additional X-ray studies and molecular dynamics simulations show the binding modes and organization of CPZ molecules when complexed with P3 only and onto the virion surface. Collectively, we provide a proof of concept for the possible use of the lattice-like organisation and the quasi-symmetric morphology of virus capsomers for loading heterocyclic drugs with defined properties.
机译:病毒生物材料由于是非常具有吸引力的他们的功能基因的人们材料。自组装病毒蛋白质衣壳上外部或内部有选择地吸收不同的载荷。噬菌体组成一个二十面体蛋白质外层衣壳和内部油脂的泡。我们报告PRD1的三维结构在复杂的抗精神病药物氯丙嗪(CPZ)低温电子显微镜。我们表明,病毒主要的果冻卷衣壳蛋白P3,向外突出衣壳壳,作为支架使用装载杂环CPZ分子。研究和分子动力学模拟显示CPZ的绑定模式和组织当包裹着P3和分子病毒粒子表面。可能使用的概念以格状组织和quasi-symmetric形态学的病毒衣壳体加载杂环药物与定义的属性。

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