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嵌合单 α-螺旋结构域作为刚性融合蛋白连接子在蛋白质纳米技术和结构生物学中的应用。

Chimeric single α-helical domains as rigid fusion protein connections for protein nanotechnology and structural biology.

机构信息

Laboratory of Nanoscale Biology, Division of Biology and Chemistry, Paul Scherrer Institute, 5232 Villigen PSI, Switzerland; Department of Biology, ETH Zürich, 8093 Zürich, Switzerland.

Laboratory of Nanoscale Biology, Division of Biology and Chemistry, Paul Scherrer Institute, 5232 Villigen PSI, Switzerland.

出版信息

Structure. 2022 Jan 6;30(1):95-106.e7. doi: 10.1016/j.str.2021.09.002. Epub 2021 Sep 28.

Abstract

Chimeric fusion proteins are essential tools for protein nanotechnology. Non-optimized protein-protein connections are usually flexible and therefore unsuitable as structural building blocks. Here we show that the ER/K motif, a single α-helical domain (SAH), can be seamlessly fused to terminal helices of proteins, forming an extended, partially free-standing rigid helix. This enables the connection of two domains at a defined distance and orientation. We designed three constructs termed YFPnano, T4Lnano, and MoStoNano. Analysis of experimentally determined structures and molecular dynamics simulations reveals a certain degree of plasticity in the connections that allows the adaptation to crystal contact opportunities. Our data show that SAHs can be stably integrated into designed structural elements, enabling new possibilities for protein nanotechnology, for example, to improve the exposure of epitopes on nanoparticles (structural vaccinology), to engineer crystal contacts with minimal impact on construct flexibility (for the study of protein dynamics), and to design novel biomaterials.

摘要

嵌合融合蛋白是蛋白质纳米技术的重要工具。未经优化的蛋白-蛋白连接通常是灵活的,因此不适合作为结构构建块。在这里,我们表明 ER/K 基序(单个α-螺旋结构域(SAH))可以无缝融合到蛋白质的末端螺旋上,形成一个扩展的、部分独立的刚性螺旋。这使得两个结构域可以在特定的距离和方向上连接。我们设计了三种称为 YFPnano、T4Lnano 和 MoStoNano 的构建体。对实验确定的结构和分子动力学模拟的分析表明,连接具有一定的可塑性,允许适应晶体接触机会。我们的数据表明,SAH 可以稳定地整合到设计的结构元件中,为蛋白质纳米技术提供新的可能性,例如,提高纳米颗粒上表位的暴露度(结构疫苗学),在对构建体灵活性影响最小的情况下设计晶体接触(用于研究蛋白质动力学),以及设计新型生物材料。

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