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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >The impact of cell-penetrating peptides on membrane bilayer structure during binding and insertion
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The impact of cell-penetrating peptides on membrane bilayer structure during binding and insertion

机译:结合和插入过程中细胞穿透肽对膜双层结构的影响

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摘要

We have studied the effect of penetratin and a truncated analogue on the bilayer structure using dual polarisation interferometry, to simultaneously measure changes in mass per unit area and birefringence (an optical parameter representing bilayer order) with high sensitivity during the binding and dissociation from the membrane. Specifically, we studied penetratin (RQIKIWFQNRRMKWKK), along with a shortened and biotinylated version known as R8K-biotin (RRMKWKKK(Biotin)-NH2). Overall both peptides bound only weakly to the neutral DMPC and POPC bilayers, while much higher binding was observed for the anionic DMPC/DMPG and POPC/POPG. The binding of penetratin to gel-phase DMPC/DMPG was adequately represented by a two-state model, whereas on the fluid-phase POPC/POPG it exhibited a distinctly different binding pattern, best represented by a three-state kinetic model. However, R8K-biotin did not bind well to DMPC/DMPG and showed a more transitory and superficial binding to POPC/POPG. Comparing the modelling results for both peptides binding to POPC/POPG suggests an important role for a securely bound intermediate prior to penetratin insertion and trans location. Overall these results further elucidate the mechanism of penetratin, and provide another example of the significance of the ability of DPI to measure structural changes and the use of kinetic analysis to investigate the stages of peptide-membrane interactions. (C) 2016 Elsevier B.V. All rights reserved.
机译:我们使用双偏振干涉法研究了渗透素和截短的类似物对双层结构的影响,以便在结合和从膜上解离的过程中以高灵敏度同时测量单位面积质量和双折射(代表双层顺序的光学参数)的变化。 。具体来说,我们研究了渗透素(RQIKIWFQNRRMKWKK),以及缩短的生物素化版本,称为R8K-生物素(RRMKWKKK(Biotin)-NH2)。总体而言,两种肽均仅弱结合至中性DMPC和POPC双层,而阴离子DMPC / DMPG和POPC / POPG的结合力更高。渗透肽与凝胶相DMPC / DMPG的结合可以通过两种状态模型充分体现,而在液相POPC / POPG上则表现出明显不同的结合模式,最好用三态动力学模型来表示。然而,R8K-生物素不能很好地与DMPC / DMPG结合,并且显示出与POPC / POPG的更短暂和表面的结合。比较两种与POPC / POPG结合的肽的建模结果,表明在渗透肽插入和转运之前,牢固结合的中间体起着重要的作用。总体而言,这些结果进一步阐明了渗透肽的机理,并提供了DPI测量结构变化的能力以及使用动力学分析研究肽膜相互作用阶段的重要性的另一个例子。 (C)2016 Elsevier B.V.保留所有权利。

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