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      TWIK-1 and TREK-1 Are Potassium Channels Contributing Significantly to Astrocyte Passive Conductance in Rat Hippocampal Slices

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          Abstract

          Expression of a linear current–voltage ( I–V) relationship (passive) K + membrane conductance is a hallmark of mature hippocampal astrocytes. However, the molecular identifications of the K + channels underlying this passive conductance remain unknown. We provide the following evidence supporting significant contribution of the two-pore domain K + channel (K 2P) isoforms, TWIK-1 and TREK-1, to this conductance. First, both passive astrocytes and the cloned rat TWIK-1 and TREK-1 channels expressed in CHO cells conduct significant amounts of Cs + currents, but vary in their relative P Cs/ P K permeability, 0.43, 0.10, and 0.05, respectively. Second, quinine, which potently inhibited TWIK-1 (IC 50 = 85 μ m) and TREK-1 (IC 50 = 41 μ m) currents, also inhibited astrocytic passive conductance by 58% at a concentration of 200 μ m. Third, a moderate sensitivity of passive conductance to low extracellular pH (6.0) supports a combined expression of acid-insensitive TREK-1, and to a lesser extent, acid-sensitive TWIK-1. Fourth, the astrocyte passive conductance showed low sensitivity to extracellular Ba 2+, and extracellular Ba 2+ blocked TWIK-1 channels at an IC 50 of 960 μ m and had no effect on TREK-1 channels. Finally, an immunocytochemical study showed colocalization of TWIK-1 and TREK-1 proteins with the astrocytic markers GLAST and GFAP in rat hippocampal stratum radiatum. In contrast, another K 2P isoform TASK-1 was mainly colocalized with the neuronal marker NeuN in hippocampal pyramidal neurons and was expressed at a much lower level in astrocytes. These results support TWIK-1 and TREK-1 as being the major components of the long-sought K + channels underlying the passive conductance of mature hippocampal astrocytes.

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          Author and article information

          Journal
          J Neurosci
          J. Neurosci
          jneuro
          jneurosci
          J. Neurosci
          The Journal of Neuroscience
          Society for Neuroscience
          0270-6474
          1529-2401
          1 July 2009
          : 29
          : 26
          : 8551-8564
          Affiliations
          [1] 1Ordway Research Institute, Albany, New York 12208,
          [2] 2Department of Biological Sciences, University at Albany, State University of New York, Albany, New York 12222, and
          [3] 3Department of Neurology, Tongji Hospital, Tongji Medical College, Huazhong University of Science and Technology, Wuhan 430030, People's Republic of China
          Author notes
          Correspondence should be addressed to either of the following: Dr. Min Zhou, Ordway Research Institute, 150 New Scotland Avenue, Albany, NY 12208, mzhou@ 123456ordwayresearch.org ; or Dr. Haijun Chen, Department of Biological Sciences, University at Albany, State University of New York, Albany, NY 12222, hc323616@ 123456albany.edu
          Article
          PMC6665656 PMC6665656 6665656 3502673
          10.1523/JNEUROSCI.5784-08.2009
          6665656
          19571146
          d4cdf60b-38bd-4d1a-a80f-8e33f0a77a9d
          Copyright © 2009 Society for Neuroscience 0270-6474/09/298551-14$15.00/0
          History
          : 3 December 2008
          : 4 May 2009
          : 3 June 2009
          Categories
          Articles
          Cellular/Molecular

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