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Controlling biofilms of gram-positive pathogenic bacteria.

机译:控制革兰氏阳性病原菌的生物膜。

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摘要

Many bacteria can form aggregates on interfaces, called biofilms, where they are much more protected against toxic agents such as antibiotics or antibodies. Bacteria organized in biofilms are therefore very difficult to control and often even high dosages of antibiotics cannot clear infectious biofilms. To form biofilms bacteria have to start a complex genetic program to switch from planktonic to sessile lifestyle. This starts with the determination of their cell density, a process called quorum sensing, triggered by small, water soluble molecules, so called autoinducers. From Gram-positive bacteria several small peptides are known, many of them thiolactones. More recently another group of compounds was discovered probably formed from ribose-homocysteine and the first autoinducer-II identified is a furanosyl borate diester. While small peptides are found to trigger the intraspecies communication autoinducer-II is assumed to be used for communication at the interspecies level. Taking the lead structure from these peptides several derivatives have been developed which prevent biofilm formation in many Gram-positive bacteria, including Staphylococcus aureus. Some of these compounds are already in clinical studies. In this review the different approaches to control bacterial biofilms are discussed together with the difficulties arising from the species-specificity of the autoinducers.
机译:许多细菌会在称为生物膜的界面上形成聚集体,在这些聚集体上,它们会受到更多保护,免受诸如抗生素或抗体之类的有毒物质的侵害。因此,生物膜中组织的细菌非常难以控制,而且即使高剂量的抗生素也无法清除感染性生物膜。为了形成生物膜,细菌必须启动一个复杂的遗传程序,才能从浮游生活方式转变为无柄生活方式。首先从确定它们的细胞密度开始,这一过程称为群体感应,由小的水溶性分子触发,即所谓的自诱导剂。从革兰氏阳性细菌中已知几种小肽,其中许多是硫代内酯。最近,发现了另一组化合物,可能是由核糖同型半胱氨酸形成的,鉴定出的第一个自诱导剂-II是呋喃糖基硼酸酯二酯。虽然发现小肽会触发种间交流,但自动诱导因子-II被认为是用于种间水平的交流。以这些肽的前导结构为基础,已开发了几种衍生物,可防止许多革兰氏阳性细菌(包括金黄色葡萄球菌)中生物膜的形成。其中一些化合物已经在临床研究中。在这篇综述中,讨论了控制细菌生物膜的不同方法,以及自诱导物的物种特异性带来的困难。

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