链霉菌的发育与病毒感染的有效控制有关。

microLife Pub Date : 2023-01-01 DOI:10.1093/femsml/uqad002
Tom Luthe, Larissa Kever, Sebastian Hänsch, Aël Hardy, Natalia Tschowri, Stefanie Weidtkamp-Peters, Julia Frunzke
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引用次数: 4

摘要

斑块的形成代表了噬菌体感染的标志,可视化了结构化环境中细菌草坪的清除。在这项研究中,我们研究了链霉菌在复杂的发育生命周期中细胞发育对噬菌体感染的影响。菌斑动力学分析显示,在一段时间的菌斑大小增大后,短暂的抗噬菌体链霉菌菌丝体在裂解区显著再生。对委内瑞拉链霉菌在细胞发育的不同阶段有缺陷的突变株的分析表明,这种再生依赖于感染界面上空气菌丝和孢子形成的开始。局限于营养生长的突变体(ΔbldN)没有明显的斑块面积收缩。荧光显微镜进一步证实斑块周围出现明显的细胞/孢子区,对碘化丙啶染色的细胞通透性降低。成熟菌丝体对噬菌体感染的易感性明显降低,这在细胞发育缺陷的菌株中不太明显。转录组分析显示,在噬菌体感染的早期阶段抑制细胞发育可能促进了噬菌体的有效繁殖。我们进一步观察到氯霉素生物合成基因簇的诱导,强调噬菌体感染是链霉菌隐代谢的触发因素。总之,我们的研究强调细胞发育和短暂噬菌体耐药性的出现是链霉菌抗病毒免疫的重要一层。
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Streptomyces development is involved in the efficient containment of viral infections.

The formation of plaques represents the hallmark of phage infection visualizing the clearance of the bacterial lawn in structured environments. In this study, we have addressed the impact of cellular development on phage infection in Streptomyces undergoing a complex developmental life cycle. Analysis of plaque dynamics revealed, after a period of plaque size enlargement, a significant regrowth of transiently phage-resistant Streptomyces mycelium into the lysis zone. Analysis of Streptomyces venezuelae mutant strains defective at different stages of cellular development indicated that this regrowth was dependent on the onset of the formation of aerial hyphae and spores at the infection interface. Mutants restricted to vegetative growth (ΔbldN) featured no significant constriction of plaque area. Fluorescence microscopy further confirmed the emergence of a distinct zone of cells/spores with reduced cell permeability towards propidium iodide staining at the plaque periphery. Mature mycelium was further shown to be significantly less susceptible to phage infection, which is less pronounced in strains defective in cellular development. Transcriptome analysis revealed the repression of cellular development at the early stages of phage infection probably facilitating efficient phage propagation. We further observed an induction of the chloramphenicol biosynthetic gene cluster highlighting phage infection as a trigger of cryptic metabolism in Streptomyces. Altogether, our study emphasizes cellular development and the emergence of transient phage resistance as an important layer of Streptomyces antiviral immunity.

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