Medhurst A D, Rennie G, Chapman C G, Meadows H, Duckworth M D, Kelsell R E, Gloger I I, Pangalos M N
Neuroscience Research, SmithKline Beecham Pharmaceuticals, New Frontiers Science Park, Essex CM19 5AW, Harlow, UK.
Brain Res Mol Brain Res. 2001 Jan 31;86(1-2):101-14. doi: 10.1016/s0169-328x(00)00263-1.
Potassium channels are amongst the most heterogeneous class of ion channels known and are responsible for mediating a diverse range of biological functions. The most recently described family of K+ channels, the 'two pore-domain family', contain four membrane spanning domains and two pore-forming domains, suggesting that two channel subunits associate to form a functional K+ pore. Several sub-families of the two pore domain potassium channel family have been described, including the weakly inward rectifying K+ channel (TWIK), the acid-sensitive K+ channel (TASK), the TWIK-related K+ channel (TREK) and the TWIK-related arachidonic acid stimulated K+ channel (TRAAK). However, comparison of the mRNA expression of these channels has been difficult due to the differences in methods used and the species studied. In the present study, we used a single technique, TaqMan semi-quantitative reverse transcription polymerase chain reaction (RT-PCR), to investigate the mRNA distribution of all currently known two pore potassium channels in human central nervous system (CNS) and peripheral tissues. TWIK-1 and the TWIK-1-like channel KCNK7 were predominantly expressed in the CNS, in contrast to TWIK-2 which was preferentially expressed in peripheral tissues such as pancreas, stomach, spleen and uterus. TASK-1 was expressed in the CNS and some peripheral tissues, whereas TASK-2 was exclusively expressed in the periphery except for mRNA expression observed in dorsal root ganglion and spinal cord. In addition, mRNA expression of the recently identified TASK-3, was almost completely exclusive to cerebellum with little or no mRNA detected in any other tissues. TREK-1 and TRAAK mRNA expression was predominantly CNS specific in contrast to the closely related TREK-2, which was expressed in both CNS and peripheral tissues. Studying the mRNA expression profiles of known two pore domain K+ channels will aid in the understanding of the biological roles of these channels. Furthermore, identification of common areas of expression may help identify which channels, if any, associate to form heteromeric K+ channel complexes.
钾通道是已知的最为多样化的离子通道类别之一,负责介导多种生物学功能。最近描述的钾离子通道家族,即“双孔结构域家族”,包含四个跨膜结构域和两个孔形成结构域,这表明两个通道亚基结合形成一个功能性钾离子孔。双孔结构域钾通道家族已被描述了几个亚家族,包括弱内向整流钾通道(TWIK)、酸敏感钾通道(TASK)、TWIK相关钾通道(TREK)和TWIK相关花生四烯酸刺激钾通道(TRAAK)。然而,由于所使用的方法和所研究的物种不同,比较这些通道的mRNA表达一直很困难。在本研究中,我们使用单一技术,即TaqMan半定量逆转录聚合酶链反应(RT-PCR),来研究所有目前已知的双孔钾通道在人中枢神经系统(CNS)和外周组织中的mRNA分布。TWIK-1和TWIK-1样通道KCNK7主要在中枢神经系统中表达,与之相反,TWIK-2优先在胰腺、胃、脾脏和子宫等外周组织中表达。TASK-1在中枢神经系统和一些外周组织中表达,而TASK-2除了在背根神经节和脊髓中观察到mRNA表达外,仅在外周表达。此外,最近鉴定出的TASK-3的mRNA表达几乎完全局限于小脑,在任何其他组织中几乎检测不到或未检测到mRNA。与密切相关的TREK-2在中枢神经系统和外周组织中均有表达不同,TREK-1和TRAAK的mRNA表达主要是中枢神经系统特异性的。研究已知双孔结构域钾离子通道的mRNA表达谱将有助于理解这些通道的生物学作用。此外,确定共同的表达区域可能有助于确定哪些通道(如果有的话)结合形成异源钾离子通道复合物。
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