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[胆固醇耗竭的K562细胞中钠通道的功能特性]

[Functional properties of sodium channels in cholesterol-depleted K562 cells].

作者信息

Sudarikova A V, Chubinskiĭ-Nadezhdin V I, Neguliaev Iu A, Morachevskaia E A

出版信息

Tsitologiia. 2009;51(8):676-83.

Abstract

The level of cellular cholesterol is known to determine functional compartmentalization of membrane lipids into ordered microdomains (rafts). Lipid rafts are assumed to play an essential role in the interactions between cell membrane and cortical cytoskeleton. As we have shown earlier, the activity of non-voltage-gated sodium channels in K562 human leukaemia cells is critically dependent on actin cytoskeleton organization. In the present paper, functional properties of sodium channels in K562 cells were examined after cholesterol-depleting treatment using methyl-beta-cyclodextrin (MbCD), selective acceptor of sterols. Single currents through sodium channels were recorded in cell-attached and inside-out mode experiments with the use of patch clamp technique. After incubation with MbCD (2.5 or 5.0 mM), an activation of sodium channels in response to cytochalasin B or D was observed in membrane fragments as well as in native cells. Characteristics of the channels in cholesterol-depleted K562 cells were similar to those in control; unitary conductance was 12 pS. Inside-out experiments with the use of globular actin have indicated that filament assembly on cytoplasmic membrane side causes an inactivation of sodium channels. These data imply that there is no association of sodium channels with cholesterol-rich membrane microdomains in K562 cells. Possible mechanisms underlying an interplay between plasma membrane and cortical cytoskeleton are discussed.

摘要

已知细胞胆固醇水平决定膜脂向有序微结构域(脂筏)的功能区室化。脂筏被认为在细胞膜与皮质细胞骨架之间的相互作用中起重要作用。正如我们之前所表明的,K562人白血病细胞中非电压门控钠通道的活性严重依赖于肌动蛋白细胞骨架的组织。在本文中,使用甲基-β-环糊精(MbCD,固醇的选择性受体)进行胆固醇耗竭处理后,检测了K562细胞中钠通道的功能特性。在细胞贴附式和内翻式模式实验中,使用膜片钳技术记录通过钠通道的单通道电流。用MbCD(2.5或5.0 mM)孵育后,在膜片段以及天然细胞中均观察到钠通道对细胞松弛素B或D的激活反应。胆固醇耗竭的K562细胞中通道的特性与对照相似;单通道电导为12 pS。使用球状肌动蛋白进行的内翻式实验表明,细胞质膜侧的细丝组装会导致钠通道失活。这些数据表明K562细胞中的钠通道与富含胆固醇的膜微结构域没有关联。本文还讨论了质膜与皮质细胞骨架之间相互作用的可能机制。

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