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纤维蛋白原与沸石纳米颗粒的分子相互作用。

Molecular interaction of fibrinogen with zeolite nanoparticles.

机构信息

Nano Drug Delivery Research Center, Kermanshah University of Medical Sciences, Kermanshah, Iran.

Pharmacutical Sciences Research Center, Kermanshah University of Medical Sciences, Kermanshah, Iran.

出版信息

Sci Rep. 2019 Feb 7;9(1):1558. doi: 10.1038/s41598-018-37621-4.

Abstract

Fibrinogen is one of the key proteins that participate in the protein corona composition of many types of nanoparticles (NPs), and its conformational changes are crucial for activation of immune systems. Recently, we demonstrated that the fibrinogen highly contributed in the protein corona composition at the surface of zeolite nanoparticles. Therefore, understanding the interaction of fibrinogen with zeolite nanoparticles in more details could shed light of their safe applications in medicine. Thus, we probed the molecular interactions between fibrinogen and zeolite nanoparticles using both experimental and simulation approaches. The results indicated that fibrinogen has a strong and thermodynamically favorable interaction with zeolite nanoparticles in a non-cooperative manner. Additionally, fibrinogen experienced a substantial conformational change in the presence of zeolite nanoparticles through a concentration-dependent manner. Simulation results showed that both E- and D-domain of fibrinogen are bound to the EMT zeolite NPs via strong electrostatic interactions, and undergo structural changes leading to exposing normally buried sequences. D-domain has more contribution in this interaction and the C-terminus of γ chain (γ), located in D-domain, showed the highest level of exposure compared to other sequences/residues.

摘要

纤维蛋白原是参与许多类型纳米粒子(NPs)的蛋白质冠组成的关键蛋白质之一,其构象变化对于免疫系统的激活至关重要。最近,我们证明了纤维蛋白原在沸石纳米粒子表面的蛋白质冠组成中高度贡献。因此,更详细地了解纤维蛋白原与沸石纳米粒子的相互作用可以为它们在医学中的安全应用提供启示。因此,我们使用实验和模拟方法研究了纤维蛋白原与沸石纳米粒子之间的分子相互作用。结果表明,纤维蛋白原与沸石纳米粒子以非协同的方式具有强烈且热力学有利的相互作用。此外,纤维蛋白原在沸石纳米粒子存在下通过浓度依赖性方式经历了实质性的构象变化。模拟结果表明,纤维蛋白原的 E 结构域和 D 结构域均通过强静电相互作用与 EMT 沸石 NPs 结合,并发生结构变化,导致通常埋藏的序列暴露。D 结构域在这种相互作用中贡献更多,γ 链(γ)的 C 末端位于 D 结构域,与其他序列/残基相比,显示出最高的暴露水平。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c205/6367512/5f999ab148db/41598_2018_37621_Fig1_HTML.jpg

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