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Mode of Protein Complexes on Gold Nanoparticles Surface: Synthesis and Characterization of Biomaterials for Hemocompatibility and Preferential DNA Complexation

机译:金纳米粒子表面上蛋白质复合物的模式:血液相位力和优先DNA络合生物材料的合成与表征

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By using in situ synthesis of gold nanoparticles (Au NPs) in the presence of binary mixtures of cytochrome c (Cyc,c) and bovine serum albumen (BSA) model proteins, we demonstrated a new method of studying protein protein interactions on the surfaces of nanomaterials. Such interactions were simultaneously evaluated and supported by the molecular dynamics studies in terms of protein docking. Both experimental and theoretical studies collectively indicated a strong complexation among Cyc,c and BSA on the surface of Au NPs with a multipoint anchoring mechanism to Au surface. They also highlighted that the Cyc,c BSA complex exhibited much stronger surface adsorption rather than Cyc,c or BSA alone. Biofunctional Au NPs thus obtained were tested for hemocompatibility for their possible applications as drug delivery vehicles in systemic circulation by employing the hemolysis. The hemolysis was done for the Au NPs which were coated with entire mixing range of Cyc,c-BSA mixtures to explore themost appropriate mixing compositions of Cyc,c-BSA mixtures for hemocompatibility. In addition, protein coated Au NPs demonstrated strong complexation with DNA which were significantly pronounced for the Cyc,c-BSA complex coated NPs rather than Cyc,c or BSA alone coated NPs. The Cyc,c-BSA docked complex on Au NP surface behaved like a typical helix turn helix motif because of the size disparity between a much larger BSA and smaller Cyc,c protein that resulted in stronger complexation with DNA in comparison to surface adsorbed Cyc,c or BSA alone. These finding bear important relevance in biotechnology in terms of gene expression and transcription factors.
机译:通过在细胞色素C(Cyc,C)和牛血清蛋白(BSA)模型蛋白的二元混合物存在下使用金纳米颗粒(Au NPS)的原位合成,我们证明了一种研究蛋白质蛋白质相互作用的新方法纳米材料。通过在蛋白质对接方面的分子动力学研究同时评估这些相互作用。实验和理论研究均共同表明Cyc,C和BSA在Au NPS表面上具有强烈络合,具有对Au表面的多点锚定机构。他们还强调了Cyc,C BSA复合物单独表现出更强烈的表面吸附而不是Cyc,C或BSA。通过采用溶血测试,测试如此获得的用于血液相成的血液相容性,以作为药物循环中的药物递送载体。对于Au NPS进行的溶血,其涂覆有Cyc,C-BSA混合物的整个混合范围,以探索Cyc的适当混合组合物,C-BSA混合物用于血液相位性。此外,蛋白质涂覆的Au NPS与DNA表现出强烈的络合,所述DNA对于CYC,C-BSA复合涂覆的NPS而不是Cyc,C或BSA单独涂覆的NPS。 Au NP表面上的CYC,C-BSA对接复合物表现得像典型的螺旋转向螺旋图样,因为较大的BSA和较小的CYC,C蛋白与DNA相比,与表面吸附的CYC相比,导致DNA的尺寸差异相比,仅C或BSA。在基因表达和转录因子方面,这些发现在生物技术中具有重要相关性。

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