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细胞外环在[具体物种]外膜蛋白X(OmpX)折叠中的作用 。(原文中“of.”后面缺少具体内容)

The Role of Extracellular Loops in the Folding of Outer Membrane Protein X (OmpX) of .

作者信息

Hermansen Simen, Ryoo David, Orwick-Rydmark Marcella, Saragliadis Athanasios, Gumbart James C, Linke Dirk

机构信息

Section for Genetics and Evolutionary Biology, Department of Biosciences, University of Oslo, Oslo, Norway.

Interdisciplinary Bioengineering Graduate Program, Georgia Institute of Technology, Atlanta, GA, United States.

出版信息

Front Mol Biosci. 2022 Jul 14;9:918480. doi: 10.3389/fmolb.2022.918480. eCollection 2022.

Abstract

The outer membrane of Gram-negative bacteria acts as an additional diffusion barrier for solutes and nutrients. It is perforated by outer membrane proteins (OMPs) that function most often as diffusion pores, but sometimes also as parts of larger cellular transport complexes, structural components of the cell wall, or even as enzymes. These OMPs often have large loops that protrude into the extracellular environment, which have promise for biotechnological applications and as therapeutic targets. Thus, understanding how modifications to these loops affect OMP stability and folding is critical for their efficient application. In this work, the small outer membrane protein OmpX was used as a model system to quantify the effects of loop insertions on OMP folding and stability. The insertions were varied according to both hydrophobicity and size, and their effects were determined by assaying folding into detergent micelles by SDS-PAGE and by isolating the outer membrane of cells expressing the constructs. The different insertions were also examined in molecular dynamics simulations to resolve how they affect OmpX dynamics in its native outer membrane. The results indicate that folding of OMPs is affected by both the insert length and by its hydrophobic character. Small insertions sometimes even improved the folding efficiency of OmpX, while large hydrophilic inserts reduced it. All the constructs that were found to fold could also do so in their native environment. One construct that could not fold was transported to the OM , but remained unfolded. Our results will help to improve the design and efficiency of recombinant OMPs used for surface display.

摘要

革兰氏阴性菌的外膜充当溶质和营养物质的额外扩散屏障。它被外膜蛋白(OMPs)穿孔,这些外膜蛋白通常作为扩散孔发挥作用,但有时也作为更大的细胞转运复合物的一部分、细胞壁的结构成分,甚至作为酶。这些外膜蛋白通常有大的环突出到细胞外环境中,这在生物技术应用和作为治疗靶点方面具有前景。因此,了解这些环的修饰如何影响外膜蛋白的稳定性和折叠对于它们的有效应用至关重要。在这项工作中,小外膜蛋白OmpX被用作模型系统来量化环插入对外膜蛋白折叠和稳定性的影响。插入物根据疏水性和大小而变化,其影响通过SDS-PAGE分析其折叠到去污剂胶束中的情况以及通过分离表达构建体的细胞的外膜来确定。还在分子动力学模拟中检查了不同的插入物,以解析它们如何影响OmpX在其天然外膜中的动力学。结果表明,外膜蛋白的折叠受插入长度及其疏水特性的影响。小的插入物有时甚至提高了OmpX的折叠效率,而大的亲水性插入物则降低了它。所有被发现能折叠的构建体在其天然环境中也能折叠。一个不能折叠的构建体被转运到外膜,但仍未折叠。我们的结果将有助于提高用于表面展示的重组外膜蛋白的设计和效率。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3a87/9329534/5e3760289933/fmolb-09-918480-g001.jpg

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