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首页> 外文期刊>European Biophysics Journal >Cyclic antimicrobial R-, W-rich peptides: The role of peptide structure and E. coli outer and inner membranes in activity and the mode of action
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Cyclic antimicrobial R-, W-rich peptides: The role of peptide structure and E. coli outer and inner membranes in activity and the mode of action

机译:富含R,W的环状抗菌肽:肽结构以及大肠杆菌内外膜在活性和作用方式中的作用

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This study compares the effect of cyclic R-, W-rich peptides with variations in amino acid sequences and sizes from 5 to 12 residues upon Gram negative and Gram positive bacteria as well as outer membrane-deficient and LPS mutant Escherichia coli (E. coli) strains to analyze the structural determinants of peptide activity. Cyclo-RRRWFW (c-WFW) was the most active and E. coli-selective sequence and bactericidal at the minimal inhibitory concentration (MIC). Removal of the outer membrane distinctly reduced peptide activity and the complete smooth LPS was required for maximal activity. c-WFW efficiently permeabilised the outer membrane of E. coli and promoted outer membrane substrate transport. Isothermal titration calorimetric studies with lipid A-, rough-LPS (r-LPS)- and smooth-LPS (s-LPS)-doped POPC liposomes demonstrated the decisive role of O-antigen and outer core polysaccharides for peptide binding and partitioning. Peptide activity against the inner E. coli membrane (IM) was very low. Even at a peptide to lipid ratio of 8/1, c-WFW was not able to permeabilise a phosphatidylglycerol/phosphatidylethanolamine (POPG/POPE) bilayer. Low influx of propidium iodide (PI) into bacteria confirmed a low permeabilising ability of c-WFW against PE-rich membranes at the MIC. Whilst the peptide effect upon eukaryotic cells correlated with the amphipathicity and permeabilisation of neutral phosphatidylcholine bilayers, suggesting a membrane disturbing mode of action, membrane permeabilisation does not seem to be the dominating antimicrobial mechanism of c-WFW. Peptide interactions with the LPS sugar moieties certainly modulate the transport across the outer membrane and are the basis of the E. coli selectivity of this type of peptides.
机译:这项研究比较了富含R和W的环状肽对革兰氏阴性和革兰氏阳性细菌以及外膜缺陷型和LPS突变型大肠杆菌(E. coli)的影响,其氨基酸序列和大小在5至12个残基之间变化。 )菌株以分析肽活性的结构决定因素。 Cyclo-RRRWFW(c-WFW)是最活跃的大肠杆菌序列,在最小抑制浓度(MIC)下具有杀菌作用。去除外膜明显降低了肽的活性,最大的活性需要完整的平滑LPS。 c-WFW有效地渗透了大肠杆菌的外膜并促进了外膜基质的运输。用脂质A,粗糙LPS(r-LPS)和光滑LPS(s-L​​PS)掺杂的POPC脂质体的等温滴定量热研究证明了O抗原和外多糖对肽结合和分配的决定性作用。针对大肠杆菌内膜(IM)的肽活性非常低。即使在肽与脂质的比率为8/1的情况下,c-WFW也无法透化磷脂酰甘油/磷脂酰乙醇胺(POPG / POPE)双层。碘化丙啶(PI)的低流入细菌证实了c-WFW对MIC处富含PE的膜的渗透能力低。尽管肽对真核细胞的作用与中性磷脂酰胆碱双层的两亲性和透化作用相关,表明膜的干扰作用方式,但膜透化作用似乎并不是c-WFW的主要抗菌机制。肽与LPS糖部分的相互作用无疑会调节跨外膜的运输,并且是此类肽在大肠杆菌中选择性的基础。

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