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Crystal Structure of LysB4 an Endolysin from Bacillus cereus-Targeting Bacteriophage B4

机译:蜡状芽孢杆菌靶向噬菌体B4的内溶素LysB4的晶体结构

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摘要

Endolysins are bacteriophage-derived enzymes that hydrolyze the peptidoglycan of host bacteria. Endolysins are considered to be promising tools for the control of pathogenic bacteria. LysB4 is an endolysin produced by Bacillus cereus-infecting bacteriophage B4, and consists of an N-terminal enzymatic active domain (EAD) and a C-terminal cell wall binding domain (CBD). LysB4 was discovered for the first time as an Lalanoyl-D-glutamate endopeptidase with the ability to breakdown the peptidoglycan among B. cereus-infecting phages. To understand the activity of LysB4 at the molecular level, this study determined the X-ray crystal structure of the LysB4 EAD, using the full-length LysB4 endolysin. The LysB4 EAD has an active site that is typical of LAS-type enzymes, where Zn2+ is tetrahedrally coordinated by three amino acid residues and one water molecule. Mutational studies identified essential residues that are involved in lytic activity. Based on the structural and biochemical information about LysB4, we suggest a ligand-docking model and a putative endopeptidase mechanism for the LysB4 EAD. These suggestions add insight into the molecular mechanism of the endolysin LysB4 in B. cereus-infecting phages.
机译:内溶素是噬菌体衍生的酶,可水解宿主细菌的肽聚糖。内溶素被认为是控制病原细菌的有前途的工具。 LysB4是一种由蜡状芽孢杆菌感染的噬菌体B4产生的内溶素,由N端酶促活性域(EAD)和C端细胞壁结合域(CBD)组成。首次发现LysB4是Lalanoyl-D-谷氨酸内肽酶,具有分解蜡状芽胞杆菌感染噬菌体中肽聚糖的能力。为了了解LysB4在分子水平上的活性,本研究使用全长LysB4内溶素确定了LysB4 EAD的X射线晶体结构。 LysB4 EAD具有一个典型的LAS型酶活性位点,其中Zn 2 + 由三个氨基酸残基和一个水分子四面体配位。突变研究确定了涉及裂解活性的必需残基。基于有关LysB4的结构和生化信息,我们建议LysB4 EAD的配体对接模型和推定的内肽酶机制。这些建议增加了对蜡状芽孢杆菌感染噬菌体中溶血素lysB4分子机制的了解。

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