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含膜噬菌体Bam35感染苏云金芽孢杆菌的进入机制。

The entry mechanism of membrane-containing phage Bam35 infecting Bacillus thuringiensis.

作者信息

Gaidelyte Ausra, Cvirkaite-Krupovic Virginija, Daugelavicius Rimantas, Bamford Jaana K H, Bamford Dennis H

机构信息

Department of Biological and Environmental Sciences and Institute of Biotechnology, Biocenter 2, P.O. Box 56 (Viikinkaari 5), 00014 University of Helsinki, Finland.

出版信息

J Bacteriol. 2006 Aug;188(16):5925-34. doi: 10.1128/JB.00107-06.

Abstract

The temperate double-stranded DNA bacteriophage Bam35 infects gram-positive Bacillus thuringiensis cells. Bam35 has an icosahedral protein coat surrounding the viral membrane that encloses the linear 15-kbp DNA genome. The protein coat of Bam35 uses the same assembly principle as that of PRD1, a lytic bacteriophage infecting gram-negative hosts. In this study, we dissected the process of Bam35 entry into discrete steps: receptor binding, peptidoglycan penetration, and interaction with the plasma membrane (PM). Bam35 very rapidly adsorbs to the cell surface, and N-acetyl-muramic acid is essential for Bam35 binding. Zymogram analysis demonstrated that peptidoglycan-hydrolyzing activity is associated with the Bam35 virion. We showed that the penetration of Bam35 through the PM is a divalent-cation-dependent process, whereas adsorption and peptidoglycan digestion are not.

摘要

温和型双链DNA噬菌体Bam35感染革兰氏阳性苏云金芽孢杆菌细胞。Bam35有一个二十面体蛋白衣壳,围绕着包裹线性15千碱基对DNA基因组的病毒膜。Bam35的蛋白衣壳采用与PRD1相同的组装原理,PRD1是一种感染革兰氏阴性宿主的裂解性噬菌体。在本研究中,我们将Bam35进入细胞的过程分解为离散步骤:受体结合、肽聚糖穿透以及与质膜(PM)的相互作用。Bam35非常迅速地吸附到细胞表面,N-乙酰胞壁酸对Bam35的结合至关重要。酶谱分析表明,肽聚糖水解活性与Bam35病毒粒子相关。我们发现Bam35穿过质膜的过程是一个依赖二价阳离子的过程,而吸附和肽聚糖消化则不依赖二价阳离子。

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