首页> 外文期刊>Frontiers in Cellular and Infection Microbiology >Structure-Based Prototype Peptides Targeting the Pseudomonas aeruginosa Type VI Secretion System Effector as a Novel Antibacterial Strategy
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Structure-Based Prototype Peptides Targeting the Pseudomonas aeruginosa Type VI Secretion System Effector as a Novel Antibacterial Strategy

机译:靶向铜绿假单胞菌VI型分泌系统效应子的基于结构的原型肽作为一种新型的抗菌策略

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摘要

The type VI secretion system (T6SS) secretes numerous toxins for bacteria-bacteria competition. TplE is a newly identified trans-kingdom toxin secreted by the T6SS in Pseudomonas aeruginosa, while TplEi neutralizes the toxic effect of TplE to protect bacteria autointoxication. Blocking the interaction of TplE-TplEi could unleash the toxin, causing bacterial cell death. In this study, we applied a crystallographic approach to design a structural-based antimicrobial peptides targeting the interaction of TplE and TplEi. We found that a peptide (designed as “L” peptide based on its shape) derived from TplE can form a crystal complex with TplEi after subtilisin treatment and the crystal structure was solved at 2.2Å. The “L” peptide displays strong binding affinity to TplEi in vitro and can release the TplE toxin to induce bacteria death in vivo. Our findings indicate that as a toxin activator, the “L” peptide could be a possible drug lead for treating P. aeruginosa infection. Our findings provide the first example that the T6SS effector and immunity protein could be a potential drug target against bacteria infection.
机译:VI型分泌系统(T6SS)分泌大量毒素,促进细菌与细菌的竞争。 TplE是由铜绿假单胞菌中的T6SS分泌的一种新发现的跨王国毒素,而TplEi中和了TplE的毒性作用,以保护细菌自体中毒。阻断TplE-TplEi的相互作用可能释放毒素,导致细菌细胞死亡。在这项研究中,我们应用了一种晶体学方法来设计针对TplE和TplEi相互作用的基于结构的抗菌肽。我们发现,在枯草杆菌蛋白酶处理后,衍生自TplE的肽(根据其形状设计为“ L”肽)可以与TplEi形成晶体复合物,晶体结构在2.2Å时溶解。 “ L”肽在体外显示出对TplEi的强结合亲和力,并且可以释放TplE毒素以在体内诱导细菌死亡。我们的发现表明,作为毒素激活剂,“ L”肽可能是治疗铜绿假单胞菌感染的可能药物。我们的发现提供了第一个例子,即T6SS效应子和免疫蛋白可能是抵抗细菌感染的潜在药物靶标。

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