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Engineering multifunctional protein nanoparticles by in vitro disassembling and reassembling of heterologous building blocks

机译:通过体外拆卸和重新组装异源构建块的工程多功能蛋白纳米粒子

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The engineering of protein self-assembling at the nanoscale allows the generation of functional and biocompatible materials, which can be produced by easy biological fabrication. The combination of cationic and histidine-rich stretches in fusion proteins promotes oligomerization as stable protein-only regular nanoparticles that are composed by a moderate number of building blocks. Among other applications, these materials are highly appealing as tools in targeted drug delivery once empowered with peptidic ligands of cell surface receptors. In this context, we have dissected here this simple technological platform regarding the controlled disassembling and reassembling of the composing building blocks. By applying high salt and imidazole in combination, nanoparticles are disassembled in a process that is fully reversible upon removal of the disrupting agents. By taking this approach, we accomplish here the in vitro generation of hybrid nanoparticles formed by heterologous building blocks. This fact demonstrates the capability to generate multifunctional and/or multiparatopic or multispecific materials usable in nanomedical applications.
机译:蛋白自组装在纳米级的工程允许的功能性和生物相容的材料,其可以通过简单的生物制造来制造的产生。阳离子和富含组氨酸的绵延的融合蛋白相结合,促进齐聚作为由中等数量的积木组成的稳定的蛋白质,只有经常纳米粒子。在其它应用中,这些材料都非常吸引人,如靶向给药工具,一旦与细胞表面受体的配体肽授权。在此背景下,我们在这里解剖关于受控分解和合成积木的重组这个简单的技术平台。通过在组合施加高盐和咪唑,纳米颗粒被分解在一个过程,是在移除所述破坏剂的完全可逆的。通过这种方法,我们在这里完成在体外产生异源积木形成混合纳米粒子。该事实表明,以产生多官能和/或多互补位或多特异性材料nanomedical用途中使用的能力。

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