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Probing Insertion and Solubilization Effects of Lysolipids on Supported Lipid Bilayers Using Microcantilevers

机译:使用微悬臂梁探测溶脂对支持的脂质双层的插入和增溶作用

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The interaction of surfactants with lipid membranes can result in composition change, area expansion, solubilization, or the formation of protrusion features of the membranes. Amphipathic surfactant molecules are simplified analogues to membrane active drugs and peptides which are known for inserting into lipid bilayers; however, the effect of these amphipathic molecules on supported membranes is not well characterized. In this paper we explore the use of microcantilever sensors to quantify surfactants' effects on lipid membranes. We use microcantilevers which are coated with lipid membranes to probe the interactions between lysolipids and supported lipid bilayers (SLBs). In particular, we investigate the effects of four zwitterionic surfactants similar to phospholipids: lysolipids of different aliphatic chain lengths (lysophosphocholines, lysoPCs, 12:0, 14:0, 16:0, and 18:0) on 1-palmitoyl-2-oleoyl-sn-glycero-3-phosphocholine-supported lipid bilayers. By monitoring the deflection of the microcantilevers, real-time free energy changes in the SLBs upon the addition of lysolipids can be detected. Additionally, the bending direction reveals whether the lysoPCs incorporate into or solubilize the SLB. When the bulk lysoPC concentration is less than its critical micelle concentration (CMC), we observe a compressive bending of the microcantilever, indicating adsorption to the SLB. Additionally, the change in surface stress is found to be proportional to the amount of membrane-bound lysoPCs. For bulk concentrations greater than the CMC, lysoPCs 12:0 and 14:0, there is tensile bending, indicating that the lysoPCs begin to solubilize and destroy the SLBs. Interestingly, this is not observed for lysoPCs with longer chain lengths. This new method of using microcantilevers for detecting and quantifying the surfactant insertion and solubilization of SLBs offers additional insights into the interactions between small amphipathic molecules and lipid membranes.
机译:表面活性剂与脂质膜的相互作用可导致组成变化,面积膨胀,增溶或形成膜的突出特征。两亲性表面活性剂分子是膜活性药物和肽的简化类似物,已知可以插入脂质双层中。然而,这些两亲性分子对支持膜的作用尚未很好地表征。在本文中,我们探索了使用微悬臂梁传感器来量化表面活性剂对脂质膜的影响。我们使用涂有脂质膜的微悬臂梁来探测溶脂和支持的脂质双层(SLB)之间的相互作用。特别是,我们研究了四种与磷脂类似的两性离子表面活性剂:不同脂肪链长度的溶脂(溶血卵磷脂,溶血PC,12:0、14:0、16:0和18:0)对1-棕榈酰-2-的影响油酰基-sn-甘油-3-磷酸胆碱支持的脂质双层。通过监视微悬臂梁的挠度,可以检测到添加溶血脂后SLB中的实时自由能变化。另外,弯曲方向揭示了lysoPC是否掺入或溶解了SLB。当总体lysoPC浓度小于其临界胶束浓度(CMC)时,我们观察到微悬臂的压缩弯曲,表明吸附到SLB。此外,发现表面应力的变化与膜结合的lysoPC的数量成正比。对于大于CMC的lysoPC 12:0和14:0的体积浓度,存在拉伸弯曲,表明lysoPC开始溶解并破坏SLB。有趣的是,对于链长较长的lysoPC,未观察到此现象。这种使用微悬臂梁检测和定量表面活性剂的表面活性剂插入和增溶的新方法为小两亲分子与脂质膜之间的相互作用提供了更多见解。

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