Structural and functional insights into the regulation of the lysis–lysogeny decision in viral communities

溶原循环 溶解循环 生物 溶解 群体感应 赖氨酸 细菌病毒 噬菌体 细胞生物学 微生物学 遗传学 病毒 毒力 大肠杆菌 免疫学 基因
作者
Chao Dou,Jie Xiong,Yijun Gu,Kun Yin,Jinjing Wang,Yuehong Hu,Dan Zhou,Xianghui Fu,Shiqian Qi,Xiaofeng Zhu,Shaohua Yao,Heng Xu,Chunlai Nie,Zongan Liang,Shengyong Yang,Yuquan Wei,Wei Cheng
出处
期刊:Nature microbiology [Nature Portfolio]
卷期号:3 (11): 1285-1294 被引量:64
标识
DOI:10.1038/s41564-018-0259-7
摘要

Communication is vital for all organisms including microorganisms, which is clearly demonstrated by the bacterial quorum-sensing system. However, the molecular mechanisms underlying communication among viruses (phages) via the quorum-sensing-like 'arbitrium' system remain unclear. Viral or host densities are known to be related to an increased prevalence of lysogeny; however, how the switch from the lytic to the lysogenic pathway occurs is unknown. Thus, we sought to reveal mechanisms of communication among viruses and determine the lysogenic dynamics involved. Structural and functional analyses of the phage-derived SAIRGA and GMPRGA peptides and their corresponding receptors, phAimR and spAimR, indicated that SAIRGA directs the lysis-lysogeny decision of phi3T by modulating conformational changes in phAimR, whereas GMPRGA regulates the lysis-lysogeny pathway by stabilizing spAimR in the dimeric state. Although temperate viruses are thought to share a similar lytic-lysogenic cycle switch model, our study suggests the existence of alternative strain-specific mechanisms that regulate the lysis-lysogeny decision. Collectively, these findings provide insights into the molecular mechanisms underlying communication among viruses, offering theoretical applications for the treatment of infectious viral diseases.
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