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四卡因对脂质膜动态重组的影响。

Effect of tetracaine on dynamic reorganization of lipid membranes.

机构信息

College of Chemistry and Chemical Engineering, Shanghai University of Engineering Science, Shanghai 201620, China.

College of Chemistry and Chemical Engineering, Shanghai University of Engineering Science, Shanghai 201620, China.

出版信息

Biochim Biophys Acta Biomembr. 2020 Sep 1;1862(9):183351. doi: 10.1016/j.bbamem.2020.183351. Epub 2020 May 13.

Abstract

To understand the intrinsic influence of a drug on lipid membranes is of critical importance in pharmacological science. Herein, we report fluorescence microscopy analysis of the interaction between the local anesthetic tetracaine (TTC) and planar supported lipid bilayers (SLBs), as model membranes. Our results show that TTC increases lipid chain mobility, destabilizes the SLBs and remarkably induces membrane disruption and solubilization. Upon TTC binding, a local curvature change in the bilayer was observed, which led to the subsequent formation of up to 20-μm-long flexible lipid tubules as well as the formation of micron-size holes. Quantitative analysis revealed that membrane solubilization process can be divided into two distinct different stages as a function of TTC concentration. In the first stage (<800 μM), the bilayer disruption profiles fit well to a Langmuir isotherm, while in the second stage (800 μM-25 mM), TTC solubilizes the membrane in a detergent-like manner. Notably, the onset of membrane solubilization occurred below the critical micelle concentration (cmc) of TTC, indicating a local accumulation of the drug in the membrane. Additionally, cholesterol increases the insertion of TTC into the membrane and thus promotes the solubilization effect of TTC on lipid bilayers. These findings may help to elucidate the possible mechanisms of TTC interaction with lipid membranes, the dose dependent toxicity attributed to local anesthetics, as well as provide valuable information for drug development and modification.

摘要

了解药物对脂质膜的内在影响在药理学中至关重要。在此,我们报告了荧光显微镜分析局部麻醉剂丁卡因(TTC)与平面支撑脂质双层(SLB)相互作用的结果,将其作为模型膜。我们的结果表明,TTC 增加了脂质链的流动性,使 SLB 不稳定,并显著诱导了膜的破坏和溶解。在 TTC 结合后,观察到双层中的局部曲率发生变化,导致随后形成长达 20-μm 的柔性脂质管以及微米大小的孔的形成。定量分析表明,膜溶解过程可以根据 TTC 浓度分为两个不同的阶段。在第一阶段(<800 μM),双层破坏曲线很好地符合 Langmuir 等温线,而在第二阶段(800 μM-25 mM),TTC 以去污剂的方式溶解膜。值得注意的是,膜溶解的起始发生在 TTC 的临界胶束浓度(cmc)以下,表明药物在膜中局部聚集。此外,胆固醇增加了 TTC 插入膜的程度,从而促进了 TTC 对脂质双层的溶解作用。这些发现可能有助于阐明 TTC 与脂质膜相互作用的可能机制、局部麻醉剂的剂量依赖性毒性,并为药物开发和修饰提供有价值的信息。

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