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Charge-Driven Interaction of Antimicrobial Peptide NK-2 with Phospholipid Membranes

机译:抗菌肽NK-2与磷脂膜的电荷驱动相互作用

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NK-2, derived from a cationic core region of NK-lysin, displays antimicrobial activity toward negatively charged bacterial membranes. We have studied the interaction of NK-2 with various phospholipid membranes, using a variety of experimental techniques, such as, isothermal titration calorimetry (ITC), ζ potential, and dynamic light scattering. As bacteria mimicking membranes, we have chosen large unilamellar vesicles (LUVs) composed of negatively charged phospholipid and neutral phospholipids. ITC and ζ potential results show the stronger binding affinity of NK-2 to negatively charged membranes than to neutral membranes. Saturation of the isotherm, obtained from ITC, at a given lipid to NK-2 ratio, was found to be consistent with the charge compensation, determined from ζ potential. A surface partition model with electrostatic contribution was used to estimate the intrinsic binding constant and other thermodynamical parameters of binding kinetics of NK-2. The size distribution of negatively charged LUV in the presence of NK-2 was found to increase drastically, indicating the presence of large aggregates. Such a large aggregate has not been observed in neutral membranes, which supports the ITC and ζ potential results.
机译:源自NK-溶素的阳离子核心区域的NK-2对带负电荷的细菌膜显示抗菌活性。我们已经使用各种实验技术,例如等温滴定热量法(ITC),ζ电位和动态光散射研究了NK-2与各种磷脂膜的相互作用。作为模仿膜的细菌,我们选择了由带负电荷的磷脂和中性磷脂组成的大型单层囊泡(LUV)。 ITC和ζ电位结果表明,NK-2与带负电的膜的结合亲和力比与中性膜的结合亲和力强。发现在给定的脂质与NK-2比例下,从ITC获得的等温线的饱和度与电荷补偿一致,该电荷补偿由ζ电位确定。使用具有静电作用的表面分配模型来估计NK-2的固有结合常数和结合动力学的其他热力学参数。发现在NK-2存在下带负电荷的LUV的尺寸分布急剧增加,表明存在大的聚集体。在中性膜中未观察到如此大的聚集体,这支持了ITC和ζ电位的结果。

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