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The influence of rough lipopolysaccharide structure on molecular interactions with mammalian antimicrobial peptides

机译:粗糙的脂多糖结构对与哺乳动物抗菌肽分子相互作用的影响

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The influence of Escherichia coli rough lipopolysaccharide chemotype on the membrane activity of the mammalian antimicrobial peptides (AMPS) human cathelicidin (LL37) and bovine lactoferricin (LFb) was studied on bilayers using solid state H-2 NMR (ssNMR) and on monolayers using the subphase injection technique, Brewster angle microscopy (BAM) and neutron reflectivity (NR). The two AMPs were selected because of their differing biological activities. Chain-deuterated dipalmitoylphosphatidylcholine (d(62)-DPPC) was added to the LPS samples, to highlight alterations in the system properties caused by the presence of the different LPS chemotypes and upon AMP challenge. Both LPS chemotypes showed a temperature dependent influence on the packing of the DPPC molecules, with a fluidizing effect exerted below the DPPC phase transition temperature (T-m), and an ordering effect observed above the T-m. The magnitude of these effects was influenced by LPS structure; the shorter Rc LPS promoted more ordered lipid packing compared to the longer Ra LPS. These differential ordering effects in turn influenced the penetrative activity of the two peptides, as the perturbation induced by both AMPs to Ra LPS-containing models was greater than that observed in those containing Rc LPS. The NR data suggests that in addition to penetrating into the monolayers, both LL37 and LFb formed a non-interacting layer below the LPS/DPPC monolayer. The overall activity of LL37, which showed a deeper penetration into the model membranes, was more marked than that of LFb, which appeared to localise at the interfacial region, thus providing evidence for the molecular origins of their different biological activities. (C) 2015 Elsevier B.V. All rights reserved.
机译:用固态H-2 NMR(ssNMR)在双层上研究了大肠杆菌粗糙脂多糖化学型对哺乳动物抗菌肽(AMPS)人cathelicidin(LL37)和牛乳铁蛋白(LFb)膜活性的影响以及对单层使用H2 NMR的影响次相注入技术,布鲁斯特角显微镜(BAM)和中子反射率(NR)。选择两种AMP是因为它们的生物活性不同。将链氘化的二铝甲酰基磷脂酰胆碱(d(62)-DPPC)添加到LPS样品中,以突出显示由于存在不同的LPS化学型和AMP挑战而引起的系统性能变化。两种LPS化学型均表现出对DPPC分子堆积的温度依赖性影响,在DPPC相变温度(T-m)以下施加流化作用,而在T-m上方观察到有序作用。这些影响的程度受LPS结构的影响;与较长的Ra LPS相比,较短的Rc LPS促进了更多有序的脂质堆积。这些不同的有序效应反过来影响了这两种肽的穿透活性,因为两种AMP对含Ra LPS的模型引起的扰动都大于含Rc LPS的模型。 NR数据表明,LL37和LFb除了渗透到单层外,还在LPS / DPPC单层下形成了一个非相互作用层。 LL37的整体活性显示出更深的渗透到模型膜中的能力,而LFb的活性总体上似乎位于界面区域,因此为它们不同生物学活性的分子起源提供了证据。 (C)2015 Elsevier B.V.保留所有权利。

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