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Gram-positive three-component antimicrobial peptide-sensing system

机译:革兰氏阳性三组分抗菌肽传感系统

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To survive during colonization or infection of the human body, microorganisms must circumvent mechanisms of innate host defense. Antimicrobial peptides represent a key component of innate host defense, especially in phagocytes and on epithelial surfaces. However, it is not known how the clinically important group of Gram-positive bacteria sense antimicrobial peptides to coordinate a directed defensive response. By determining the genome-wide gene regulatory response to human β-defensin 3 in the nosocomial pathogen Staphylococcus epidermidis, we discovered an antimicrobial peptide sensor system that controls major specific resistance mechanisms of Gram-positive bacteria and is unrelated to the Gram-negative PhoP/PhoQ system. It contains a classical two-component signal transducer and an unusual third protein, all of which are indispensable for signal transduction and antimicrobial peptide resistance. Furthermore, our data indicate that a very short, extracellular loop with a high density of negative charges in the sensor protein is responsible for antimicrobial peptide binding and the observed specificity for cationic antimicrobial peptides. Our study shows that Gram-positive bacteria have developed an efficient and unique way of controlling resistance mechanisms to antimicrobial peptides, which may provide a promising target for antimicrobial drug development.
机译:为了在人类定植或感染过程中生存,微生物必须规避先天宿主防御的机制。抗菌肽代表先天宿主防御的关键组成部分,尤其是在吞噬细胞和上皮表面。但是,尚不知道临床上重要的革兰氏阳性细菌群如何感知抗菌肽以协调定向防御反应。通过确定医院病原体表皮葡萄球菌对人β-防御素3的全基因组基因调控应答,我们发现了一种抗菌肽传感器系统,该系统可控制革兰氏阳性细菌的主要特异性耐药机制,并且与革兰氏阴性PhoP / PhoQ系统。它包含一个经典的两组分信号转导子和一个不同寻常的第三种蛋白质,所有这些对于信号转导和抗菌肽抵抗都是必不可少的。此外,我们的数据表明,传感器蛋白中负电荷密度高的非常短的细胞外环负责抗菌肽的结合以及所观察到的阳离子抗菌肽的特异性。我们的研究表明,革兰氏阳性细菌已开发出一种有效且独特的方法来控制对抗菌肽的耐药机制,这可能为抗菌药物开发提供有希望的目标。

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