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Rapid and High-Throughput Evaluation of Diverse Configurations of Engineered Lysins Using the VersaTile Technique.

作者信息

Duyvejonck Lisa, Gerstmans Hans, Stock Michiel, Grimon Dennis, Lavigne Rob, Briers Yves

机构信息

Laboratory of Applied Biotechnology, Department of Biotechnology, Ghent University, Valentin Vaerwyckweg 1, 9000 Ghent, Belgium.

Laboratory of Gene Technology, Department of Biosystems, KU Leuven, Kasteelpark Arenberg 21, 3001 Leuven, Belgium.

出版信息

Antibiotics (Basel). 2021 Mar 11;10(3):293. doi: 10.3390/antibiotics10030293.

Abstract

Bacteriophage-encoded lysins are an emerging class of antibacterial enzymes based on peptidoglycan degradation. The modular composition of lysins is a hallmark feature enabling optimization of antibacterial and pharmacological properties by engineering of lysin candidates based on lysin and non-lysin modules. In this regard, the recent introduction of the VersaTile technique allows the rapid construction of large modular lysin libraries based on a premade repository of building blocks. In this study, we perform a high-throughput construction and screening of five combinatorial lysin libraries with different configurations, targeting . An elaborate analysis of the activity distribution of 940 variants and sequencing data of 74 top hits inhibiting the growth of could be associated with specific design rules. Specific outer membrane permeabilizing peptides (OMPs) and enzymatically active domains (EADs) are significantly overrepresented among the top hits, while cell wall binding domains (CBDs) are equally represented. Especially libraries with the configuration (OMP-linker-CBD-EAD) and the inverse configuration (CBD-EAD-linker-OMP) yield the most active variants, with discernible clusters of variants that emerge above the remaining variants. The approach implemented here provides a blueprint for discovery campaigns of engineered lysins starting from libraries with different configurations and compositions.

摘要

噬菌体编码的溶菌酶是一类基于肽聚糖降解的新兴抗菌酶。溶菌酶的模块化组成是一个标志性特征,通过基于溶菌酶和非溶菌酶模块对溶菌酶候选物进行工程改造,能够优化其抗菌和药理特性。在这方面,最近引入的VersaTile技术允许基于预制的构建模块库快速构建大型模块化溶菌酶文库。在本研究中,我们针对……对五个具有不同配置的组合溶菌酶文库进行了高通量构建和筛选。对940个变体的活性分布以及74个抑制……生长的顶级命中序列数据的详细分析可能与特定的设计规则相关。在顶级命中序列中,特定的外膜通透肽(OMP)和酶活性结构域(EAD)显著富集,而细胞壁结合结构域(CBD)的分布较为均匀。特别是具有(OMP-接头-CBD-EAD)配置和反向配置(CBD-EAD-接头-OMP)的文库产生了最具活性的变体,出现了明显高于其余变体的变体簇。这里实施的方法为从具有不同配置和组成的文库开始的工程溶菌酶发现活动提供了蓝图。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3532/7998686/fd36a43ff9cd/antibiotics-10-00293-g001.jpg

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