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Exploiting the peptidoglycan-binding motif LysM for medical and industrial applications

机译:开发肽聚糖结合基序LysM用于医学和工业应用

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摘要

The lysin motif (LysM) was first identified by Garvey et al. in 1986 and, in subsequent studies, has been shown to bind noncovalently to peptidoglycan and chitin by interacting with N-acetylglucosamine moieties. The LysM sequence is present singly or repeatedly in a large number of proteins of prokaryotes and eukaryotes. Since the mid-1990s, domains containing one or more of these LysM sequences originating from different LysM-containing proteins have been examined for purely scientific reasons as well as for their possible use in various medical and industrial applications. These studies range from detecting localized binding of LysM-containing proteins onto bacteria to actual bacterial cell surface analysis. On a more applied level, the possibilities of employing the LysM domains for cell immobilization, for the display of peptides, proteins, or enzymes on (bacterial) surfaces as well as their utility in the development of novel vaccines have been scrutinized. To serve these purposes, the chimeric proteins containing one or more of the LysM sequences have been produced and isolated from various prokaryotic and eukaryotic expression hosts. This review gives a succinct overview of the characteristics of the LysM domain and of current developments in its application potential.
机译:溶素基序(LysM)首先由Garvey等人鉴定。在1986年和随后的研究中,已显示通过与N-乙酰氨基葡糖部分相互作用而与肽聚糖和几丁质非共价结合。 LysM序列单独或反复存在于大量的原核生物和真核生物蛋白质中。自1990年代中期以来,出于纯粹的科学原因以及它们在各种医学和工业应用中的可能用途,已经对包含一个或多个源自不同LysM蛋白质的LysM序列的域进行了研究。这些研究的范围从检测含LysM的蛋白质在细菌上的局部结合到实际的细菌细胞表面分析。在更广泛的应用水平上,已经研究了将LysM结构域用于细胞固定,在(细菌)表面上展示肽,蛋白质或酶的可能性以及它们在开发新型疫苗中的实用性。为了实现这些目的,已经生产了含有一个或多个LysM序列的嵌合蛋白,并从各种原核和真核表达宿主中分离了这些蛋白。这篇综述简要地概述了LysM结构域的特性及其应用潜力的最新发展。

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