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Targeting Bacterial Cardiolipin Enriched Microdomains: An Antimicrobial Strategy Used by Amphiphilic Aminoglycoside Antibiotics

机译:针对细菌心磷脂富集的微域:两亲氨基糖苷类抗生素使用的抗菌策略。

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摘要

Some bacterial proteins involved in cell division and oxidative phosphorylation are tightly bound to cardiolipin. Cardiolipin is a non-bilayer anionic phospholipid found in bacterial inner membrane. It forms lipid microdomains located at the cell poles and division plane. Mechanisms by which microdomains are affected by membrane-acting antibiotics and the impact of these alterations on membrane properties and protein functions remain unclear. In this study, we demonstrated cardiolipin relocation and clustering as a result of exposure to a cardiolipin-acting amphiphilic aminoglycoside antibiotic, the 3′,6-dinonyl neamine. Changes in the biophysical properties of the bacterial membrane of P. aeruginosa, including decreased fluidity and increased permeability, were observed. Cardiolipin-interacting proteins and functions regulated by cardiolipin were impacted by the amphiphilic aminoglycoside as we demonstrated an inhibition of respiratory chain and changes in bacterial shape. The latter effect was characterized by the loss of bacterial rod shape through a decrease in length and increase in curvature. It resulted from the effect on MreB, a cardiolipin dependent cytoskeleton protein as well as a direct effect of 3′,6-dinonyl neamine on cardiolipin. These results shed light on how targeting cardiolipin microdomains may be of great interest for developing new antibacterial therapies.
机译:一些参与细胞分裂和氧化磷酸化的细菌蛋白与心磷脂紧密结合。心磷脂是在细菌内膜中发现的非双层阴离子磷脂。它形成位于细胞极和分裂平面的脂质微区。膜作用抗生素影响微区的机制以及这些改变对膜特性和蛋白质功能的影响尚不清楚。在这项研究中,由于暴露于具有心磷脂作用的两亲性氨基糖苷抗生素3',6-dinonyl Neamine,我们证明了心磷脂的重新定位和聚集。观察到铜绿假单胞菌细菌膜的生物物理特性发生了变化,包括流动性降低和通透性增加。两亲性氨基糖苷影响与心磷脂相互作用的蛋白质和受心磷脂调节的功能,因为我们证明了对呼吸链的抑制和细菌形状的改变。后一种效应的特征是通过长度的减小和曲率的增加而使细菌棒状形状丧失。这是由于它对MreB(一种依赖于心磷脂的细胞骨架蛋白)产生的作用以及3',6-二壬基神经酰胺对心磷脂的直接作用所致。这些结果揭示了靶向心磷脂微结构域对于开发新的抗菌疗法可能具有极大的兴趣。

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