Literature DB >> 16794780

Biophysical and pharmacological characteristics of native two-pore domain TASK channels in rat adrenal glomerulosa cells.

David P Lotshaw1.   

Abstract

Multiple genes of the TASK subfamily of two-pore domain K(+) channels are reported to be expressed in rat glomerulosa cells. To determine which TASK isoforms contribute to native leak channels controlling resting membrane potential, patch-clamp studies were performed to identify biophysical and pharmacological characteristics of macroscopic and unitary K(+) currents diagnostic of recombinant TASK channel isoforms. Results indicate K(+) conductance (gK(+)) is mediated almost exclusively by a weakly voltage-dependent (leak) K(+) channel closely resembling TASK-3. Leak channels exhibited a unitary conductance approximating that expected for TASK-3 under the recording conditions employed, brief mean open times and a voltage-dependent open probability. Extracellular H(+) induced voltage-independent inhibition of gK(+), exhibiting an IC(50) of 56 nM: (pH 7.25) and a Hill coefficient of 0.75. Protons inhibited leak channel open probability (P(o)) by promoting a long-lived closed state (tau > 500 ms). Extracellular Zn(2+) mimicked the effects of H(+); inhibition of gK(+) exhibited an IC(50) of 41 microM: with a Hill coefficient of 1.26, inhibiting channel gating by promoting a long-lived closed state. Ruthenium red (5 microM: ) inhibited gK(+) by 75.6% at 0 mV. Extracellular Mg(2+) induced voltage-dependent block of gK(+), inhibiting unitary current amplitude without affecting mean open time. Bupivacaine induced voltage-dependent block of gK(+), exhibiting IC(50) values of 116 microM: at -100 mV and 28 microM: at 40 mV with Hill coefficients of 1 at both potentials. Halothane induced a voltage-independent stimulation of gK(+) primarily by decreasing the leak channel closed-state dwell time.

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Year:  2006        PMID: 16794780     DOI: 10.1007/s00232-005-7012-x

Source DB:  PubMed          Journal:  J Membr Biol        ISSN: 0022-2631            Impact factor:   1.843


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5.  Molecular basis of the voltage-dependent gating of TREK-1, a mechano-sensitive K(+) channel.

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6.  Estimating the number of channels in patch recordings.

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Review 4.  The family of K2P channels: salient structural and functional properties.

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Journal:  J Physiol       Date:  2015-01-22       Impact factor: 5.182

5.  Adrenal Tissue-Specific Deletion of TASK Channels Causes Aldosterone-Driven Angiotensin II-Independent Hypertension.

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Review 10.  Ion Channel Function and Electrical Excitability in the Zona Glomerulosa: A Network Perspective on Aldosterone Regulation.

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