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Protein capsules assembled via isobutyramide grafts: Sequential growth, biofunctionalization, and cellular uptake

机译:通过异丁酰胺移植物组装的蛋白胶囊:顺序生长,生物功能化和细胞摄取

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We report the sequential assembly of proteins via the alternating physical adsorption of human serum albumin (HSA) and chemical grafting with isobutyramide (IBAM) or bromoisobutyramide (BrIBAM) groups. This approach, performed on silica template particles, leads to the formation of noncovalent protein films with controlled growth at the nanometer scale. Further, after template removal, hollow protein capsules with tunable wall thicknesses and high mechanical stability are obtained. The use of BrIBAM, compared to IBAM grafts, leads to significantly thicker capsule walls, highlighting the influence of the bromine atoms in the assembly process, which is discussed in terms of a theoretical model of noncovalent interactions. Another feature of the process is the possibility to functionalize the HSA capsules with other biologically active macromolecules, including enzymes, polysaccharides, or DNA plasmids, demonstrating the versatility of this approach. We also report that BrIBAM-HSA and IBAM-HSA capsules display negligible cytotoxicity in vitro with HeLa cells and that their cellular uptake is dependent on the thickness of the capsule walls. These findings support the potential use of these protein capsules in tailored biological applications such as drug delivery.
机译:我们报告通过人类血清白蛋白(HSA)的交替物理吸附和异丁酰胺(IBAM)或溴异丁酰胺(BrIBAM)基团的化学嫁接对蛋白质进行的顺序组装。在二氧化硅模板颗粒上执行的此方法导致形成非共价蛋白膜,并在纳米级控制生长。此外,在除去模板后,获得了具有可调壁厚和高机械稳定性的中空蛋白胶囊。与IBAM移植物相比,BrIBAM的使用导致胶囊壁明显增厚,突出了组装过程中溴原子的影响,这是根据非共价相互作用的理论模型进行讨论的。该方法的另一个特点是可以用其他具有生物活性的大分子功能化HSA胶囊,包括酶,多糖或DNA质粒,这证明了这种方法的多功能性。我们还报告说,BrIBAM-HSA和IBAM-HSA胶囊在体外对HeLa细胞显示的细胞毒性微不足道,并且它们的细胞摄取取决于胶囊壁的厚度。这些发现支持了这些蛋白质胶囊在特定的生物学应用中的潜在用途,例如药物递送。

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