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Plug-and-Display: decoration of Virus-Like Particles via isopeptide bonds for modular immunization

机译:即插即用:通过异肽键修饰病毒样颗粒以进行模块化免疫

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摘要

Virus-like particles (VLPs) are non-infectious self-assembling nanoparticles, useful in medicine and nanotechnology. Their repetitive molecularly-defined architecture is attractive for engineering multivalency, notably for vaccination. However, decorating VLPs with target-antigens by genetic fusion or chemical modification is time-consuming and often leads to capsid misassembly or antigen misfolding, hindering generation of protective immunity. Here we establish a platform for irreversibly decorating VLPs simply by mixing with protein antigen. SpyCatcher is a genetically-encoded protein designed to spontaneously form a covalent bond to its peptide-partner SpyTag. We expressed in E. coli VLPs from the bacteriophage AP205 genetically fused to SpyCatcher. We demonstrated quantitative covalent coupling to SpyCatcher-VLPs after mixing with SpyTag-linked to malaria antigens, including CIDR and Pfs25. In addition, we showed coupling to the VLPs for peptides relevant to cancer from epidermal growth factor receptor and telomerase. Injecting SpyCatcher-VLPs decorated with a malarial antigen efficiently induced antibody responses after only a single immunization. This simple, efficient and modular decoration of nanoparticles should accelerate vaccine development, as well as other applications of nanoparticle devices.
机译:病毒样颗粒(VLP)是非感染性的自组装纳米颗粒,可用于医学和纳米技术。其重复的分子定义架构对工程多价具有吸引力,尤其是疫苗接种。然而,通过基因融合或化学修饰用靶抗原修饰VLP很费时,并且经常导致衣壳错装或抗原错折叠,从而阻碍了保护性免疫的产生。在这里,我们建立了一个平台,简单地通过与蛋白质抗原混合即可不可逆地修饰VLP。 SpyCatcher是一种基因编码的蛋白质,旨在与其肽伙伴SpyTag自发形成共价键。我们在大肠杆菌VLP中表达了与SpyCatcher基因融合的噬菌体AP205。在与链接到疟疾抗原(包括CIDR和Pfs25)的SpyTag混合后,我们证明了与SpyCatcher-VLP定量共价偶联。此外,我们显示了与表皮生长因子受体和端粒酶与癌症相关的肽与VLP的偶联。仅注射一次免疫后,注射装饰有疟疾抗原的SpyCatcher-VLP即可有效诱导抗体反应。纳米粒子的这种简单,有效和模块化的装饰应加快疫苗的开发以及纳米粒子设备的其他应用。

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