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探究金纳米粒子-β-乳球蛋白冠复合物的调制形成及其应用。

Probing the modulated formation of gold nanoparticles-beta-lactoglobulin corona complexes and their applications.

机构信息

State Key Laboratory of Oncology in South China, Collaborative Innovation Center for Cancer Medicine, Sun Yat-sen University Cancer Center, Guangzhou 510060, China.

出版信息

Nanoscale. 2017 Nov 23;9(45):17758-17769. doi: 10.1039/c7nr02999c.

Abstract

Understanding the interactions between proteins and nanoparticles (NPs) along with the underlying structural and dynamic information is of utmost importance to exploit nanotechnology for biomedical applications. Upon adsorption onto a NP surface, proteins form a well-organized layer, termed the corona, that dictates the identity of the NP-protein complex and governs its biological pathways. Given its high biological relevance, in-depth molecular investigations and applications of NPs-protein corona complexes are still scarce, especially since different proteins form unique corona patterns, making identification of the biomolecular motifs at the interface critical. In this work, we provide molecular insights and structural characterizations of the bio-nano interface of a popular food-based protein, namely bovine beta-lactoglobulin (β-LG), with gold nanoparticles (AuNPs) and report on our investigations of the formation of corona complexes by combined molecular simulations and complementary experiments. Two major binding sites in β-LG were identified as being driven by citrate-mediated electrostatic interactions, while the associated binding kinetics and conformational changes in the secondary structures were also characterized. More importantly, the superior stability of the corona led us to further explore its biomedical applications, such as in the smartphone-based point-of-care biosensing of Escherichia coli (E. coli) and in the computed tomography (CT) of the gastrointestinal (GI) tract through oral administration to probe GI tolerance and functions. Considering their biocompatibility, edible nature, and efficient excretion through defecation, AuNPs-β-LG corona complexes have shown promising perspectives for future in vitro and in vivo clinical settings.

摘要

了解蛋白质与纳米粒子(NPs)之间的相互作用以及潜在的结构和动态信息对于利用纳米技术进行生物医学应用至关重要。在吸附到 NP 表面后,蛋白质会形成一层组织良好的层,称为冠,它决定了 NP-蛋白质复合物的身份,并控制其生物途径。鉴于其高度的生物学相关性,对 NPs-蛋白质冠复合物的深入分子研究和应用仍然很少,特别是因为不同的蛋白质会形成独特的冠图案,使得识别界面处的生物分子基序至关重要。在这项工作中,我们提供了一种流行的基于食品的蛋白质,即牛β-乳球蛋白(β-LG)与金纳米粒子(AuNP)的生物-纳米界面的分子见解和结构特征,并报告了我们通过组合分子模拟和互补实验对冠复合物形成的研究。确定了β-LG 中的两个主要结合位点是由柠檬酸介导的静电相互作用驱动的,同时还对二级结构中的相关结合动力学和构象变化进行了表征。更重要的是,冠的优越稳定性促使我们进一步探索其生物医学应用,例如在智能手机的即时护理生物传感大肠杆菌(E. coli)和通过口服给药进行胃肠道(GI)的计算机断层扫描(CT)以探测 GI 耐受性和功能。考虑到它们的生物相容性、可食用性和通过粪便有效排泄,AuNP-β-LG 冠复合物在未来的体外和体内临床环境中显示出了有希望的前景。

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