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一种源自抗菌肽 cathelicidin-2 的肽能有效破坏表皮葡萄球菌生物膜。

A cathelicidin-2-derived peptide effectively impairs Staphylococcus epidermidis biofilms.

机构信息

TNO Defense, Security and Safety, Rijswijk, The Netherlands.

出版信息

Int J Antimicrob Agents. 2011 May;37(5):476-9. doi: 10.1016/j.ijantimicag.2010.12.020. Epub 2011 Mar 3.

Abstract

Staphylococcus epidermidis is a major cause of nosocomial infections owing to its ability to form biofilms on the surface of medical devices. Biofilms are surface-adhered bacterial communities. In mature biofilms these communities are encased in an extracellular matrix composed of bacterial polysaccharides, proteins and DNA. The antibiotic resistance of bacteria present in biofilms can be up to 1000-fold higher compared with the planktonic phenotype. Host defence peptides (HDPs) are considered to be excellent candidates for the development of novel antibiotics. Recently, we demonstrated that a short variant of the HDP chicken cathelicidin-2, peptide F(2,5,12)W, has potent antibacterial and lipopolysaccharide-neutralising activities. This study reports on the antibiofilm activity of peptide F(2,5,12)W against two strains of S. epidermidis, including a multiresistant strain. Peptide F(2,5,12)W potently inhibited the formation of bacterial biofilms in vitro at a low concentration of 2.5 μM, which is below the concentration required to kill or inhibit growth (minimal inhibitory concentration=10 μM). Moreover, peptide F(2,5,12)W also impaired existing S. epidermidis biofilms. A 4-h challenge of pre-grown biofilms with 40 μM F(2,5,12)W reduced the metabolic activity of the wild-type strain biofilm completely and reduced that of the multiresistant strain biofilm by >50%. It is concluded that F(2,5,12)W prevents biofilm formation and impairs mature S. epidermidis biofilms.

摘要

表皮葡萄球菌因其能够在医疗器械表面形成生物膜而成为医院感染的主要原因。生物膜是附着在表面的细菌群落。在成熟的生物膜中,这些群落被包裹在由细菌多糖、蛋白质和 DNA 组成的细胞外基质中。生物膜中存在的细菌的抗生素耐药性比浮游表型高 1000 倍。宿主防御肽(HDPs)被认为是开发新型抗生素的理想候选物。最近,我们证明了 HDP 鸡 cathelicidin-2 的一种短变体,肽 F(2,5,12)W,具有强大的抗菌和脂多糖中和活性。本研究报告了肽 F(2,5,12)W 对两种表皮葡萄球菌菌株(包括多耐药菌株)的抗生物膜活性。肽 F(2,5,12)W 在低浓度 2.5 μM 时即可有效抑制细菌生物膜的形成,低于杀死或抑制生长所需的浓度(最小抑菌浓度=10 μM)。此外,肽 F(2,5,12)W 还损害了现有的表皮葡萄球菌生物膜。用 40 μM F(2,5,12)W 对预生长的生物膜进行 4 小时的挑战,完全抑制了野生型菌株生物膜的代谢活性,并使多耐药菌株生物膜的代谢活性降低了>50%。结论是 F(2,5,12)W 可防止生物膜形成并损害成熟的表皮葡萄球菌生物膜。

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