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Lipid Fluid–Gel Phase Transition Induced Alamethicin Orientational Change Probed by Sum Frequency Generation Vibrational Spectroscopy

机译:总和频率产生振动光谱探测脂质-凝胶相变诱导的阿米西星取向变化

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摘要

Alamethicin has been extensively studied as an antimicrobial peptide (AMP) and is widely used as a simple model for ion channel proteins. It has been shown that the antimicrobial activity of AMPs is related to their cell membrane orientation, which may be influenced by the phase of the lipid molecules in the cell membrane. The “healthy” cell membranes contain fluid phase lipids, while gel phase lipids can be found in injured or aged cells or in some phase separated membrane regions. Thus, investigations on how the phase of the lipids influences the membrane orientation of AMPs are important to understand more details regarding the AMP’s action on cell membranes. In this study, we determined the orientational changes of alamethicin molecules associated with planar substrate supported single lipid bilayers (serving as model cell membranes) with different phases (fluid or gel) as a function of peptide concentration using sum frequency generation (SFG) vibrational spectroscopy. The phase changes of the lipid bilayers were realized by varying the sample temperature. Our SFG results indicated that alamethicin lies down on the surface of fluid and gel phase 1,2-dimyristoyl(d54)-sn-glycero-3-phosphocholine (d-DMPC) lipid bilayers when the lipid bilayers are in contact with a peptide solution with a low concentration of 0.84 μM. However, at a medium peptide concentration of 10.80 μM, alamethicin inserts into the fluid phase lipid bilayer. Its orientation switches from a transmembrane to an in-plane (or lying down) orientation when the phase of the lipid bilayer changes from a fluid state to a gel state. At a high peptide concentration of 21.60 μM, alamethicin adopts a transmembrane orientation while associated with both fluid and gel phase lipid bilayers. We also studied the structural changes of the fluid and gel phase lipid bilayers upon their interactions with alamethicin molecules at different peptide concentrations.
机译:丙甲霉素已被广泛研究为抗菌肽(AMP),并已广泛用作离子通道蛋白的简单模型。已经显示出AMP的抗微生物活性与其细胞膜取向有关,这可能受细胞膜中脂质分子的相的影响。 “健康”的细胞膜含有液相脂质,而凝胶相脂质则存在于受损或老化的细胞或某些相分离的膜区域中。因此,对脂质相如何影响AMPs膜取向的研究对于了解有关AMP对细胞膜作用的更多细节非常重要。在这项研究中,我们使用总频率产生(SFG)振动光谱法确定了与具有不同相(流体或凝胶)的平面底物支撑的单个脂质双层(用作模型细胞膜)相关的alamethicin分子的取向变化与肽浓度的关系。通过改变样品温度实现脂质双层的相变。我们的SFG结果表明,当脂质双层与肽溶液接触时,alamethicin落在流体和凝胶相的表面上1,2-二肉豆蔻酰基(d54)-sn-甘油-3-磷酸胆碱(d-DMPC)脂质双层浓度低至0.84μM。但是,在中等肽浓度为10.80μM的情况下,乐果霉素会插入液相脂质双层中。当脂质双层的相从流体状态变为凝胶状态时,其取向从跨膜取向转变为面内(或躺下)取向。在21.60μM的高肽浓度下,乐果霉素采用跨膜取向,同时与液相和凝胶相脂质双层结合。我们还研究了在不同肽浓度下,液相和凝胶相脂质双层与缩水甘油分子相互作用的结构变化。

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