Pseudomonas aeruginosa (P.A.) is a human pathogen belonging to the top priorities for the discovery of new therapeutic solutions. Its propensity to generate biofilms strongly complicates the treatments required to cure P.A. infections. Herein, we describe the synthesis of a series of novel rotaxanes composed of a central galactosylated pillar5arene, a tetrafucosylated dendron, and a tetraguanidinium subunit. Besides the high affinity of the final glycorotaxanes for the two P.A. lectins LecA and LecB, potent inhibition levels of biofilm growth were evidenced, showing that their three subunits work synergistically. An antibiofilm assay using a double Delta lecA Delta lecB mutant compared to the wild type demonstrated that the antibiofilm activity of the best glycorotaxane is lectin-mediated. Such antibiofilm potency had rarely been reached in the literature. Importantly, none of the final rotaxanes was bactericidal, showing that their antibiofilm activity does not depend on bacteria killing, which is a rare feature for antibiofilm agents.
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机译:铜绿假单胞菌(Pseudomonas aeruginosa,简称PA)是一种人类病原体,是发现新治疗解决方案的首要任务。它产生生物膜的倾向使治愈 PA 感染所需的治疗变得非常复杂。在此,我们描述了由中央半乳糖基化柱[5]芳烃、四岩藻糖基化树突和四胍亚基组成的一系列新型轮烷的合成。除了最终糖杉烷对两种 PA 凝集素 LecA 和 LecB 的高亲和力外,还证明了对生物膜生长的有效抑制水平,表明它们的三个亚基协同作用。与野生型相比,使用双 Delta lecA Delta lecB 突变体的抗生物膜测定表明,最佳甘蓝杉烷的抗生物膜活性是凝集素介导的。这种抗生物膜效力在文献中很少达到。重要的是,最终的轮烷类化合物均不具有杀菌作用,这表明它们的抗生物膜活性不依赖于细菌杀灭,这是抗生物膜剂的罕见特征。
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