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Visualization of the protein corona: towards a biomolecular understanding of nanoparticlecell- interactions

机译:可视化蛋白质的电晕:走向nanoparticlecell -生物分子的理解的相互作用

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The use of nanocarriers in biology and medicine is complicated by the current need to understand how nanoparticles interact in complex biological surroundings. When nanocarriers come into contact with serum, proteins immediately adsorb onto their surface, forming a protein corona which defines their biological identity. Although the composition of the protein corona has been widely determined by proteomics, its morphology still remains unclear. In this study we show for the first time the morphology of the protein corona using transmission electron microscopy. We are able to demonstrate that the protein corona is not, as commonly supposed, a dense, layered shell coating the nanoparticle, but an undefined, loose network of proteins. Additionally, we are now able to visualize and discriminate between the soft and hard corona using centrifugation-based separation techniques together with proteomic characterization. The protein composition of the similar to 15 nm hard corona strongly depends on the surface chemistry of the respective nanomaterial, thus further affecting cellular uptake and intracellular trafficking. Large diameter protein corona resulting from pre-incubation with soft corona or Apo-A1 inhibits cellular uptake, confirming the stealth-effect mechanism. In summary, the knowledge on protein corona formation, composition and morphology is essential to design therapeutic effective nanoparticle systems.
机译:人们在生物学和医学的使用当前需要了解复杂的纳米粒子相互作用在复杂的生物环境。立即与血清蛋白质吸附到他们的表面,形成一种蛋白质电晕定义了他们的生物身份。组成蛋白质的电晕广泛由蛋白质组学,其形态仍不清楚。第一次蛋白质电晕的形态使用透射电子显微镜。能够证明蛋白质电晕不像通常认为,一个密集的、分层的壳涂层的纳米颗粒,但未定义,松了网络的蛋白质。能够想象和区分软、硬使用centrifugation-based电晕分离技术与蛋白质组学鉴定。类似的努力15 nm电晕强烈依赖各自的表面化学纳米材料,从而进一步影响细胞吸收和胞内走私。直径电晕产生的蛋白质与软电晕或Apo-A1 pre-incubation抑制细胞吸收,确认stealth-effect机制。蛋白质形成电晕,知识成分和形态设计至关重要治疗有效的纳米系统。

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