论文信息 - CNS Distribution of Members of the Two-Pore-Domain (KCNK) Potassium Channel Family

CNS Distribution of Members of the Two-Pore-Domain (KCNK) Potassium Channel Family

Two-pore-domain potassium (K+) channels are substrates for resting K+ currents in neurons. They are major targets for endogenous modulators, as well as for clinically important compounds such as volatile anesthetics. In the current study, we report on the CNS distribution in the rat and mouse of mRNA encoding seven two-pore-domain K+ channel family members: TASK-1 (KCNK3), TASK-2 (KCNK5), TASK-3 (KCNK9), TREK-1 (KCNK2), TREK-2 (KCNK10), TRAAK (KCNK4), and TWIK-1 (KCNK1). All of these genes were expressed in dorsal root ganglia, and for all of the genes except TASK-2, there was a differential distribution in the CNS. For TASK-1, highest mRNA accumulation was seen in the cerebellum and somatic motoneurons. TASK-3 was much more widely distributed, with robust expression in all brain regions, with particularly high expression in somatic motoneurons, cerebellar granule neurons, the locus ceruleus, and raphe nuclei and in various nuclei of the hypothalamus. TREK-1 was highest in the striatum and in parts of the cortex (layer IV) and hippocampus (CA2 pyramidal neurons). mRNA for TRAAK also was highest in the cortex, whereas expression of TREK-2 was primarily restricted to the cerebellar granule cell layer. There was widespread distribution of TWIK-1, with highest levels in the cerebellar granule cell layer, thalamic reticular nucleus, and piriform cortex. The differential expression of each of these genes likely contributes to characteristic excitability properties in distinct populations of neurons, as well as to diversity in their susceptibility to modulation.

[1] M. Lazdunski,et al. Polyunsaturated fatty acids are potent neuroprotectors , 2000, The EMBO journal.

[2] D. Bayliss,et al. The TASK-1 Two-Pore Domain K+ Channel Is a Molecular Substrate for Neuronal Effects of Inhalation Anesthetics , 2000, The Journal of Neuroscience.

[3] C. Kindler,et al. Localization of the tandem pore domain K+ channel KCNK5 (TASK-2) in the rat central nervous system. , 2000, Brain research. Molecular brain research.

[4] A. Gray,et al. Volatile Anesthetics Activate the Human Tandem Pore Domain Baseline K+ Channel KCNK5 , 2000, Anesthesiology.

[5] J T Williams,et al. Voltage- and ligand-activated inwardly rectifying currents in dorsal raphe neurons in vitro , 1988, The Journal of neuroscience : the official journal of the Society for Neuroscience.

[6] M. Lazdunski,et al. TASK, a human background K+ channel to sense external pH variations near physiological pH , 1997, The EMBO journal.

[7] J. Feldman,et al. Synaptic control of motoneuronal excitability. , 2000, Physiological reviews.

[8] B. Robertson,et al. A functional role for the two-pore domain potassium channel TASK-1 in cerebellar granule neurons. , 2000, Proceedings of the National Academy of Sciences of the United States of America.

[9] M. Lazdunski,et al. Inhalational anesthetics activate two-pore-domain background K+ channels , 1999, Nature Neuroscience.

[10] M. Lazdunski,et al. Genomic and functional characteristics of novel human pancreatic 2P domain K(+) channels. , 2001, Biochemical and biophysical research communications.

[11] Edmund M Talley,et al. TASK-1, a Two–Pore Domain K+ Channel, Is Modulated by Multiple Neurotransmitters in Motoneurons , 2000, Neuron.

[12] Donghee Kim,et al. TREK-2, a New Member of the Mechanosensitive Tandem-pore K+ Channel Family* , 2000, The Journal of Biological Chemistry.

[13] M. Lazdunski,et al. The structure, function and distribution of the mouse TWIK‐1 K+ channel , 1997, FEBS letters.

[14] M. Pangalos,et al. Distribution analysis of human two pore domain potassium channels in tissues of the central nervous system and periphery. , 2001, Brain research. Molecular brain research.

[15] M. Lazdunski,et al. TWIK‐1, a ubiquitous human weakly inward rectifying K+ channel with a novel structure. , 1996, The EMBO journal.

[16] L. Swanson. The Rat Brain in Stereotaxic Coordinates, George Paxinos, Charles Watson (Eds.). Academic Press, San Diego, CA (1982), vii + 153, $35.00, ISBN: 0 125 47620 5 , 1984 .

[17] K. Grzeschik,et al. THIK-1 and THIK-2, a Novel Subfamily of Tandem Pore Domain K+ Channels* 210 , 2001, The Journal of Biological Chemistry.

[18] A. Patel,et al. The neuroprotective agent riluzole activates the two P domain K(+) channels TREK-1 and TRAAK. , 2000, Molecular pharmacology.

[19] Donghee Kim,et al. TASK-5, a new member of the tandem-pore K(+) channel family. , 2001, Biochemical and biophysical research communications.

[20] A. Gray,et al. Localization of the tandem pore domain K+ channel TASK-1 in the rat central nervous system. , 2000, Brain research. Molecular brain research.

[21] G. Hervieu,et al. Distribution and expression of TREK-1, a two-pore-domain potassium channel, in the adult rat CNS , 2001, Neuroscience.

[22] M. Lazdunski,et al. Human TREK2, a 2P Domain Mechano-sensitive K+Channel with Multiple Regulations by Polyunsaturated Fatty Acids, Lysophospholipids, and Gs, Gi, and Gq Protein-coupled Receptors* , 2000, The Journal of Biological Chemistry.

[23] D. Kim,et al. Arachidonic acid activation of a new family of K+ channels in cultured rat neuronal cells. , 1995, The Journal of physiology.

[24] J. Gassenhuber,et al. Characterization of TASK‐4, a novel member of the pH‐sensitive, two‐pore domain potassium channel family , 2001, FEBS letters.

[25] Detlef Bockenhauer,et al. Potassium leak channels and the KCNK family of two-p-domain subunits , 2001, Nature Reviews Neuroscience.

[26] M. Lazdunski,et al. TREK‐1 is a heat‐activated background K+ channel , 2000, The EMBO journal.

[27] P. Murdock,et al. Cloning, localisation and functional expression of a novel human, cerebellum specific, two pore domain potassium channel. , 2000, Brain research. Molecular brain research.

[28] M. Lazdunski,et al. The endocannabinoid anandamide is a direct and selective blocker of the background K+ channel TASK‐1 , 2001, The EMBO journal.

[29] M. Lazdunski,et al. TWIK-2, an Inactivating 2P Domain K+ Channel* , 2000, The Journal of Biological Chemistry.

[30] M. Lazdunski,et al. Cloning, functional expression and brain localization of a novel unconventional outward rectifier K+ channel. , 1996, The EMBO journal.

[31] M. Lazdunski,et al. Immunolocalization of the arachidonic acid and mechanosensitive baseline TRAAK potassium channel in the nervous system , 1999, Neuroscience.

[32] G. Paxinos. The Rat nervous system , 1985 .

[33] E. Honoré,et al. Properties and modulation of mammalian 2P domain K+ channels , 2001, Trends in Neurosciences.

[34] Donghee Kim,et al. TASK-3, a New Member of the Tandem Pore K+ Channel Family* , 2000, The Journal of Biological Chemistry.

[35] A. Gray,et al. An Open Rectifier Potassium Channel with Two Pore Domains in Tandem Cloned from Rat Cerebellum , 1998, The Journal of Neuroscience.

[36] A. Patel,et al. Mechano- or Acid Stimulation, Two Interactive Modes of Activation of the TREK-1 Potassium Channel* , 1999, The Journal of Biological Chemistry.

[37] M. Lazdunski,et al. Cloning of a New Mouse Two-P Domain Channel Subunit and a Human Homologue with a Unique Pore Structure* , 1999, The Journal of Biological Chemistry.

[38] S. Waldegger,et al. A constitutively open potassium channel formed by KCNQ1 and KCNE3 , 2000, Nature.

[39] C. Colbert,et al. Arachidonic Acid Reciprocally Alters the Availability of Transient and Sustained Dendritic K+ Channels in Hippocampal CA1 Pyramidal Neurons , 1999, The Journal of Neuroscience.

[40] M. Lazdunski,et al. A neuronal two P domain K+ channel stimulated by arachidonic acid and polyunsaturated fatty acids , 1998, The EMBO journal.

[41] William Wisden,et al. Adaptive regulation of neuronal excitability by a voltage- independent potassium conductance , 2001, Nature.

[42] P. Murdock,et al. The neuroprotective agent sipatrigine (BW619C89) potently inhibits the human tandem pore-domain K+ channels TREK-1 and TRAAK , 2001, Brain Research.

[43] M. Lazdunski,et al. KCNE2 confers background current characteristics to the cardiac KCNQ1 potassium channel , 2000, The EMBO journal.

[44] W. Stühmer,et al. IRK(1–3) and GIRK(1–4) Inwardly Rectifying K+Channel mRNAs Are Differentially Expressed in the Adult Rat Brain , 1996, The Journal of Neuroscience.

[45] M. Lazdunski,et al. Axonal transport of TREK and TRAAK potassium channels in rat sciatic nerves , 2000, Neuroreport.

[46] M. Flonta,et al. Cold transduction by inhibition of a background potassium conductance in rat primary sensory neurones , 2001, Neuroscience Letters.

[47] A. Karschin,et al. TASK-3, a Novel Tandem Pore Domain Acid-sensitive K+Channel , 2000, The Journal of Biological Chemistry.

[48] D. McCormick. Neurotransmitter actions in the thalamus and cerebral cortex and their role in neuromodulation of thalamocortical activity , 1992, Progress in Neurobiology.

[49] M. Lazdunski,et al. Molecular and functional properties of two-pore-domain potassium channels. , 2000, American journal of physiology. Renal physiology.