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异源寡聚化的生理作用:聚焦于双孔钾通道。

Physiological roles of heteromerization: focus on the two-pore domain potassium channels.

机构信息

Université côte d'Azur, IPMC CNRS UMR7275, Laboratory of Excellence ICST, 660 route des Lucioles 06650 Valbonne, France.

Inserm, 101 rue de Tolbiac, 75013, Paris, France.

出版信息

J Physiol. 2021 Feb;599(4):1041-1055. doi: 10.1113/JP279870. Epub 2021 Jan 4.

Abstract

Potassium channels form the largest family of ion channels with more than 80 members involved in cell excitability and signalling. Most of them exist as homomeric channels, whereas specific conditions are required to obtain heteromeric channels. It is well established that heteromerization of voltage-gated and inward rectifier potassium channels affects their function, increasing the diversity of the native potassium currents. For potassium channels with two pore domains (K ), homomerization has long been considered the rule, their polymodal regulation by a wide diversity of physical and chemical stimuli being responsible for the adaptation of the leak potassium currents to cellular needs. This view has recently evolved with the accumulation of evidence of heteromerization between different K subunits. Several functional intragroup and intergroup heteromers have recently been identified, which contribute to the functional heterogeneity of this family. K heteromerization is involved in the modulation of channel expression and trafficking, promoting functional and signalling diversity. As illustrated in the Abstract Figure, heteromerization of TREK1 and TRAAK provides the cell with more possibilities of regulation. It is becoming increasingly evident that K heteromers contribute to important physiological functions including neuronal and cardiac excitability. Since heteromerization also affects the pharmacology of K channels, this understanding helps to establish K heteromers as new therapeutic targets for physiopathological conditions.

摘要

钾离子通道是最大的离子通道家族之一,其中超过 80 个成员参与细胞兴奋和信号传递。它们中的大多数作为同型通道存在,而获得异型通道则需要特定的条件。众所周知,电压门控和内向整流钾通道的异源二聚化会影响它们的功能,增加了天然钾电流的多样性。对于具有两个孔结构域的钾通道(K ),同型二聚化长期以来被认为是规则,其对广泛的物理和化学刺激的多模态调节是导致泄漏钾电流适应细胞需求的原因。随着越来越多的证据表明不同 K 亚基之间存在异源二聚化,这种观点最近发生了变化。最近已经鉴定出几个功能上的同组和组间异质体,这有助于该家族的功能异质性。K 异源二聚化参与通道表达和运输的调节,促进功能和信号的多样性。如摘要图所示,TREK1 和 TRAAK 的异源二聚化为细胞提供了更多的调节可能性。越来越明显的是,K 异质体有助于包括神经元和心脏兴奋在内的重要生理功能。由于异源二聚化也会影响钾通道的药理学,因此这种理解有助于将 K 异质体确立为生理病理条件的新治疗靶点。

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