Chemin Jean, Patel Amanda Jane, Duprat Fabrice, Sachs Frederick, Lazdunski Michel, Honore Eric
Institut de Génomique Fonctionnelle, UPR 2580 CNRS, 141 rue de la Cardonille, 34094, Montpellier cedex 05, France.
Pflugers Arch. 2007 Oct;455(1):97-103. doi: 10.1007/s00424-007-0250-2. Epub 2007 Mar 24.
TREK-1 is an unconventional K(+) channel that is activated by both physical and chemical stimuli. In this study, we show that the inner leaflet membrane phospholipids, including PIP(2), exert a mixed stimulatory and inhibitory effect on TREK-1. Intra-cellular phospholipids inhibit basal channel activity and activation by membrane stretch, intra-cellular acidosis and arachidonic acid. However, binding of endogenous negative inner leaflet phospholipids with poly-lysine reduces inhibition and reveals channel stimulation by exogenous intra-cellular phospholipids. A similar effect is observed with PI, PE, PS and PA, unlike DG, demonstrating that the phosphate at position 3 is required although the global charge of the molecule is not critical. Inhibition depends on the distal C-terminal domain that conditions channel mechano-sensitivity, but is independent of the positively charged PIP(2) stimulatory site in the proximal C-terminal domain. This is, to our knowledge, the first report of an ion channel dually regulated by membrane phospholipids.
TREK - 1是一种非常规钾离子通道,可被物理和化学刺激激活。在本研究中,我们发现包括磷脂酰肌醇-4,5-二磷酸(PIP₂)在内的内膜小叶膜磷脂对TREK - 1具有混合的刺激和抑制作用。细胞内磷脂抑制基础通道活性以及由膜拉伸、细胞内酸中毒和花生四烯酸引起的激活。然而,内源性负电荷内膜小叶磷脂与聚赖氨酸的结合减少了抑制作用,并揭示了外源性细胞内磷脂对通道的刺激作用。与二酰甘油(DG)不同,磷脂酰肌醇(PI)、磷脂酰乙醇胺(PE)、磷脂酰丝氨酸(PS)和磷脂酸(PA)也观察到类似的效果,表明虽然分子的整体电荷并不关键,但3位的磷酸基团是必需的。抑制作用取决于调节通道机械敏感性的远端C末端结构域,但与近端C末端结构域中带正电荷的PIP₂刺激位点无关。据我们所知,这是关于离子通道受膜磷脂双重调节的首次报道。
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