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首页> 外文期刊>Frontiers in Microbiology >Antibacterial phage ORFans of Pseudomonas aeruginosa phage LUZ24 reveal a novel MvaT inhibiting protein
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Antibacterial phage ORFans of Pseudomonas aeruginosa phage LUZ24 reveal a novel MvaT inhibiting protein

机译:铜绿假单胞菌噬菌体LUZ24的抗菌噬菌体ORFans揭示了一种新型的MvaT抑制蛋白

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The functional elucidation of small unknown phage proteins (‘ORFans’) presents itself as one of the major challenges of bacteriophage molecular biology. In this work, we mined the Pseudomonas aeruginosa -infecting phage LUZ24 proteome for antibacterial and antibiofilm proteins against its host. Subsequently, their putative host target was identified. In one example, we observed an interaction between LUZ24 gp4 and the host transcriptional regulator MvaT. The polymerization of MvaT across AT-rich DNA strands permits gene silencing of foreign DNA, thereby limiting any potentially adverse effects of such DNA. Gel shift assays proved the inhibitory effect of LUZ24 gp4 on MvaT DNA binding activity. Therefore, we termed this gene product as Mip, the MvaT inhibiting protein. We hypothesize Mip prevents the AT-rich LUZ24 DNA from being physically blocked by MvaT oligomers right after its injection in the host cell, thereby allowing phage transcription and thus completion of the phage infection cycle.
机译:小未知噬菌体蛋白(“ ORFans”)的功能阐明将其自身视为噬菌体分子生物学的主要挑战之一。在这项工作中,我们提取了铜绿假单胞菌感染噬菌体LUZ24蛋白质组,以针对其宿主进行抗菌和抗生物膜蛋白处理。随后,确定了其推定的宿主靶标。在一个示例中,我们观察到LUZ24 gp4与宿主转录调节子MvaT之间的相互作用。 MvaT在富含AT的DNA链上的聚合允许外源DNA的基因沉默,从而限制了此类DNA的任何潜在不利影响。凝胶位移分析证明了LUZ24 gp4对MvaT DNA结合活性的抑制作用。因此,我们将该基因产物称为Mip,即MvaT抑制蛋白。我们假设Mip阻止了富含AT的LUZ24 DNA在注入宿主细胞后立即被MvaT寡聚体物理阻断,从而允许噬菌体转录并因此完成了噬菌体感染周期。

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