磷脂酸
钾通道
化学
脂质体
基因亚型
生物物理学
生物化学
离子通道
钾通道
离解常数
立体化学
膜
生物
磷脂
受体
基因
作者
Samantha Schrecke,Yun Zhu,Jacob W. McCabe,Mariah Bartz,Charles Packianathan,Minglei Zhao,Ming Zhou,David H. Russell,Arthur Laganowsky
标识
DOI:10.1038/s41589-020-00659-5
摘要
TRAAK is an ion channel from the two-pore domain potassium (K2P) channel family with roles in maintaining the resting membrane potential and fast action potential conduction. Regulated by a wide range of physical and chemical stimuli, the affinity and selectivity of K2P4.1 toward lipids remains poorly understood. Here we show the two isoforms of K2P4.1 have distinct binding preferences for lipids dependent on acyl chain length and position on the glycerol backbone. The channel can also discriminate the fatty acid linkage at the SN1 position. Of the 33 lipids interrogated using native mass spectrometry, phosphatidic acid had the lowest equilibrium dissociation constants for both isoforms of K2P4.1. Liposome potassium flux assays with K2P4.1 reconstituted in defined lipid environments show that those containing phosphatidic acid activate the channel in a dose-dependent fashion. Our results begin to define the molecular requirements for the specific binding of lipids to K2P4.1.
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