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蛋白质冠层的结合功能与结构组织分析

An Analysis of the Binding Function and Structural Organization of the Protein Corona.

作者信息

Zhang Yuwei, Wu Jamie L Y, Lazarovits James, Chan Warren C W

机构信息

Department of Chemistry, University of Toronto, 80 St. George Street, Toronto, Ontario M5S 3H6, Canada.

Institute of Biomaterials and Biomedical Engineering, University of Toronto, 164 College Street, Toronto, Ontario M5S 3G9, Canada.

出版信息

J Am Chem Soc. 2020 May 13;142(19):8827-8836. doi: 10.1021/jacs.0c01853. Epub 2020 Apr 28.

Abstract

Blood proteins adsorb onto the surface of nanoparticles after intravenous injection to form a protein corona. The underlying organization and binding function of these adsorbed proteins remain unclear. This can impact how the corona mediates cell and tissue interactions. Here, we investigated the function and structural organization of the protein corona using an immunoassay approach. We discovered that only 27% of the adsorbed proteins examined are functional for binding to their target protein. This is because the corona architecture is not a monolayer, but an assembly of proteins that are bound to each other. We further demonstrated that we can control the binding functionality of a protein by changing the organization of proteins in the assembly. We show that manipulation of the corona protein composition and assembly can influence their interactions with macrophage cells in culture. This study provides detailed functional and structural insights into the protein corona on nanomaterials and offers a new strategy to manipulate it for controlled interactions with the biological system.

摘要

静脉注射后,血液中的蛋白质吸附到纳米颗粒表面,形成蛋白质冠层。这些吸附蛋白的潜在组织和结合功能尚不清楚。这可能会影响蛋白质冠层介导细胞和组织相互作用的方式。在这里,我们使用免疫测定方法研究了蛋白质冠层的功能和结构组织。我们发现,所检测的吸附蛋白中只有27% 具有与其靶蛋白结合的功能。这是因为蛋白质冠层结构不是单层的,而是由相互结合的蛋白质组成的集合体。我们进一步证明,通过改变集合体中蛋白质的组织方式,可以控制蛋白质的结合功能。我们表明,对蛋白质冠层的组成和组装进行操纵,可以影响其与培养中的巨噬细胞的相互作用。这项研究提供了关于纳米材料上蛋白质冠层的详细功能和结构见解,并提供了一种新策略来操纵它,以实现与生物系统的可控相互作用。

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