Interactions between anesthetics and lipid rafts

Catia Bandeiras, B. Saramago, A. P. Serro
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引用次数: 1

Abstract

The exact mechanism by which anesthetics induce membrane-mediated modifications that lead to loss of sensation is still an open question. Since lipid rafts are membrane microdomains that have been associated with cell signaling pathways, as well as specific interaction with drugs, they may contribute to that mechanism. The interactions of a canonical liposomal lipid raft model, as well as of a model without cholesterol, with the anesthetics tetracaine (TTC), lidocaine (LDC) and propofol (PPF) were studied using quartz crystal microbalance with dissipation (QCM-D), differential scanning calorimetry (DSC) and phosphorus nuclear magnetic resonance (P-NMR). The three anesthetics induced effects such as membrane flu-idization, depression of phase transition temperatures, liposome swelling and/or viscosity changes of the adsorbed liposome layers on both models. Tetracaine interacts more with raftlike domains, lidocaine induces stronger modifications on POPC/SM liposomes and the results for propofol are not fully conclusive.
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麻醉药和脂筏之间的相互作用
麻醉药诱导膜介导的改变导致感觉丧失的确切机制仍然是一个悬而未决的问题。由于脂筏是与细胞信号通路以及与药物的特定相互作用有关的膜微域,它们可能有助于该机制。采用石英晶体耗散微天平(QCM-D)、差示扫描量热法(DSC)和磷核磁共振(P-NMR)研究了典型脂质体脂筏模型和无胆固醇模型与麻醉剂丁卡因(TTC)、利多卡因(LDC)和异丙酚(PPF)的相互作用。在两种模型上,三种麻醉剂引起膜流化、相变温度降低、脂质体肿胀和/或吸附脂质体层粘度变化等效应。丁卡因更多地与筏状结构域相互作用,利多卡因对POPC/SM脂质体的修饰更强,而异丙酚的结果还不完全确定。
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