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一种靶向革兰氏阴性菌的新型噬菌体溶菌酶的鉴定及体外特性研究

Identification and in vitro Characterization of a Novel Phage Endolysin that Targets Gram-Negative Bacteria.

作者信息

Bai Jaewoo, Lee Sangmi, Ryu Sangryeol

机构信息

Department of Food and Animal Biotechnology, Seoul National University, Seoul 08826, Korea.

Department of Agricultural Biotechnology, Seoul National University, Seoul 08826, Korea.

出版信息

Microorganisms. 2020 Mar 21;8(3):447. doi: 10.3390/microorganisms8030447.

Abstract

Most double-stranded (ds) DNA phages utilize holin proteins to secrete endolysin for host peptidoglycan lysis. In contrast, several holin-independent endolysins with secretion sequences or signal-arrest-release (SAR) sequences are secreted via the Sec pathway. In this study, we characterized a novel lysis protein (M4Lys) encoded by the dsDNA phage BSPM4, whose lysis function is not dependent on either holin or the Sec pathway in vitro. In silico analysis of M4Lys revealed that it contains a putative virion protein domain and an unusual C-terminal transmembrane domain (TMD). Turbidity reduction assays and liquid chromatography-mass spectrometry using purified peptidoglycan showed that the virion protein domain of M4Lys has peptidoglycan lysis activity. In vitro overproduction of M4Lys in revealed that M4Lys alone caused rapid cell lysis. Treatment of with a Sec inhibitor did not inhibit the lysis activity of M4Lys, indicating that the Sec pathway is not involved in M4Lys-mediated cell lysis. Truncation of the TMD eliminated the cell lysis phenomenon, while production of the TMD alone did not induce the cell lysis. All these findings demonstrate that M4Lys is a novel endolysin that has a unique mosaic structure distinct from other canonical endolysins and the TMD plays a critical role in M4Lys-mediated in vitro cell lysis.

摘要

大多数双链(ds)DNA噬菌体利用孔蛋白来分泌内溶素,以裂解宿主肽聚糖。相比之下,一些具有分泌序列或信号捕获释放(SAR)序列的不依赖孔蛋白的内溶素是通过Sec途径分泌的。在本研究中,我们对dsDNA噬菌体BSPM4编码的一种新型裂解蛋白(M4Lys)进行了表征,其裂解功能在体外不依赖于孔蛋白或Sec途径。对M4Lys的计算机分析表明,它包含一个假定的病毒体蛋白结构域和一个不寻常的C末端跨膜结构域(TMD)。使用纯化的肽聚糖进行的浊度降低试验和液相色谱-质谱分析表明,M4Lys的病毒体蛋白结构域具有肽聚糖裂解活性。在体外过量表达M4Lys表明,单独的M4Lys会导致细胞快速裂解。用Sec抑制剂处理并没有抑制M4Lys的裂解活性,这表明Sec途径不参与M4Lys介导的细胞裂解。TMD的截短消除了细胞裂解现象,而单独产生TMD并没有诱导细胞裂解。所有这些发现表明,M4Lys是一种新型内溶素,具有与其他典型内溶素不同的独特镶嵌结构,并且TMD在M4Lys介导的体外细胞裂解中起关键作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b3df/7143992/6fc51e3ec49c/microorganisms-08-00447-g001.jpg

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