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在模板化复合纳米结构中稳定病毒蛋白笼的见解:二硫键的作用。

Insights into stabilization of a viral protein cage in templating complex nanoarchitectures: roles of disulfide bonds.

机构信息

Suzhou Key Laboratory of Nanomedical Characterization, Division of Nanobiomedicine and i-Lab, Suzhou Institute of Nano-Tech and Nano-Bionics, Chinese Academy of Sciences, Suzhou, 215123, China.

出版信息

Small. 2014 Feb 12;10(3):536-43. doi: 10.1002/smll.201300860. Epub 2013 Sep 9.

Abstract

As a typical protein nanostructure, virus-based nanoparticle (VNP) of simian virus 40 (SV40), which is composed of pentamers of the major capsid protein of SV40 (VP1), has been successfully employed in guiding the assembly of different nanoparticles (NPs) into predesigned nanostructures with considerable stability. However, the stabilization mechanism of SV40 VNP remains unclear. Here, the importance of inter-pentamer disulfide bonds between cysteines in the stabilization of quantum dot (QD)-containing VNPs (VNP-QDs) is comprehensively investigated by constructing a series of VP1 mutants of cysteine to serine. Although the presence of a QD core can greatly enhance the assembly and stability of SV40 VNPs, disulfide bonds are vital to stability of VNP-QDs. Cysteine at position 9 (C9) and C104 contribute most of the disulfide bonds and play essential roles in determining the stability of SV40 VNPs as templates to guide assembly of complex nanoarchitectures. These results provide insightful clues to understanding the robustness of SV40 VNPs in organizing suprastructures of inorganic NPs. It is expected that these findings will help guide the future design and construction of protein-based functional nanostructures.

摘要

作为一种典型的蛋白质纳米结构,猿猴病毒 40(SV40)的病毒纳米颗粒(VNP)由 SV40 主要衣壳蛋白(VP1)的五聚体组成,已成功用于引导不同纳米颗粒(NPs)组装成具有相当稳定性的预定纳米结构。然而,SV40 VNP 的稳定机制仍不清楚。在这里,通过构建一系列半胱氨酸到丝氨酸的 VP1 突变体,全面研究了半胱氨酸之间的五聚体二硫键在含量子点的 VNP(VNP-QD)稳定中的重要性。尽管 QD 核的存在可以极大地增强 SV40 VNP 的组装和稳定性,但二硫键对于 VNP-QD 的稳定性至关重要。位置 9(C9)和 C104 的半胱氨酸贡献了大部分二硫键,并在确定 SV40 VNP 作为指导组装复杂纳米结构的模板的稳定性方面发挥着重要作用。这些结果为理解 SV40 VNP 在组织无机 NPs 的超结构方面的稳健性提供了有见地的线索。预计这些发现将有助于指导未来基于蛋白质的功能性纳米结构的设计和构建。

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