Isolation and functional analysis of phage-displayed antibody fragments targeting the staphylococcal superantigen-like proteins

IF 3.9 3区 生物学 Q2 MICROBIOLOGY MicrobiologyOpen Pub Date : 2023-07-16 DOI:10.1002/mbo3.1371
Ida Alanko, Rebecca Sandberg, Eeva-Christine Brockmann, Carla J. C. de Haas, Jos A. G. van Strijp, Urpo Lamminmäki, Outi M. H. Salo-Ahen
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Abstract

Staphylococcus aureus produces numerous virulence factors that manipulate the immune system, helping the bacteria avoid phagocytosis. In this study, we are investigating three immune evasion molecules called the staphylococcal superantigen-like proteins 1, 5, and 10 (SSL1, SSL5, and SSL10). All three SSLs inhibit vital host immune processes and contribute to S. aureus immune evasion. This study aimed to identify single-chain variable fragment (scFvs) antibodies from synthetic antibody phage libraries, which can recognize either of the three SSLs and could block the interaction between the SSLs and their respective human targets. The antibodies were isolated after three rounds of panning against SSL1, SSL5, and SSL10, and their ability to bind to the SSLs was studied using a time-resolved fluorescence-based immunoassay. We successfully obtained altogether 44 unique clones displaying binding activity to either SSL1, SSL5, or SSL10. The capability of the SSL-recognizing scFvs to inhibit the SSLs' function was tested in an MMP9 enzymatic activity assay, a P-selectin glycoprotein ligand 1 competitive binding assay, and an IgG1-mediated phagocytosis assay. We could show that one scFv was able to inhibit SSL1 and maintain MMP9 activity in a concentration-dependent manner. Finally, the structure of this inhibiting scFv was modeled and used to create putative scFv-SSL1-complex models by protein–protein docking. The complex models were subjected to a 100-ns molecular dynamics simulation to assess the possible binding mode of the antibody.

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噬菌体展示的针对葡萄球菌超抗原样蛋白的抗体片段的分离和功能分析。
金黄色葡萄球菌产生许多毒力因子,操纵免疫系统,帮助细菌避免吞噬作用。在这项研究中,我们正在研究三种被称为葡萄球菌超抗原样蛋白1、5和10(SSL1、SSL5和SSL10)的免疫逃避分子。所有三种SSLs都抑制重要的宿主免疫过程,并有助于金黄色葡萄球菌的免疫逃避。本研究旨在从合成抗体噬菌体文库中鉴定单链可变片段(scFvs)抗体,该抗体可以识别三种SSLs中的任何一种,并可以阻断SSLs与其各自人类靶点之间的相互作用。在对SSL1、SSL5和SSL10进行三轮筛选后分离抗体,并使用基于时间分辨荧光的免疫测定研究它们与SSLs结合的能力。我们总共成功地获得了44个独特的克隆,它们显示出与SSL1、SSL5或SSL10的结合活性。在MMP9酶活性测定、P-选择素糖蛋白配体1竞争性结合测定和IgG1介导的吞噬作用测定中测试了SSL识别单链抗体抑制SSLs功能的能力。我们可以表明,一种scFv能够以浓度依赖的方式抑制SSL1并维持MMP9的活性。最后,对这种抑制性scFv的结构进行了建模,并通过蛋白质-蛋白质对接用于创建推定的scFv-SSL1复合物模型。对复杂模型进行100ns的分子动力学模拟,以评估抗体的可能结合模式。
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来源期刊
MicrobiologyOpen
MicrobiologyOpen MICROBIOLOGY-
CiteScore
8.00
自引率
0.00%
发文量
78
审稿时长
20 weeks
期刊介绍: MicrobiologyOpen is a peer reviewed, fully open access, broad-scope, and interdisciplinary journal delivering rapid decisions and fast publication of microbial science, a field which is undergoing a profound and exciting evolution in this post-genomic era. The journal aims to serve the research community by providing a vehicle for authors wishing to publish quality research in both fundamental and applied microbiology. Our goal is to publish articles that stimulate discussion and debate, as well as add to our knowledge base and further the understanding of microbial interactions and microbial processes. MicrobiologyOpen gives prompt and equal consideration to articles reporting theoretical, experimental, applied, and descriptive work in all aspects of bacteriology, virology, mycology and protistology, including, but not limited to: - agriculture - antimicrobial resistance - astrobiology - biochemistry - biotechnology - cell and molecular biology - clinical microbiology - computational, systems, and synthetic microbiology - environmental science - evolutionary biology, ecology, and systematics - food science and technology - genetics and genomics - geobiology and earth science - host-microbe interactions - infectious diseases - natural products discovery - pharmaceutical and medicinal chemistry - physiology - plant pathology - veterinary microbiology We will consider submissions across unicellular and cell-cluster organisms: prokaryotes (bacteria, archaea) and eukaryotes (fungi, protists, microalgae, lichens), as well as viruses and prions infecting or interacting with microorganisms, plants and animals, including genetic, biochemical, biophysical, bioinformatic and structural analyses. The journal features Original Articles (including full Research articles, Method articles, and Short Communications), Commentaries, Reviews, and Editorials. Original papers must report well-conducted research with conclusions supported by the data presented in the article. We also support confirmatory research and aim to work with authors to meet reviewer expectations. MicrobiologyOpen publishes articles submitted directly to the journal and those referred from other Wiley journals.
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