Two K(+)-selective channels in neonatal rat atrial cells activated by lipophilic compounds have been characterized in detail. The arachidonic acid-stimulated channel (IK.AA) had a slope conductance of 124 +/- 17 pS at +30 mV in symmetrical 140 mM potassium and a mean open time of approximately 1 ms, and was relatively voltage independent. IK.AA activity was reversibly increased by lowering pH to 6.0. Arachidonic acid was most effective in activating this channel, although a number of lipophilic compounds resulted in activation. Surprisingly, choline, a polar molecule, also activated the channel. A second K+ channel was activated by 10 microM phosphatidylcholine applied to the intracellular surface of inside-out atrial patches. This channel (IK.PC) had a slope conductance of 60 +/- 6 pS at +40 mV and a mean open time of approximately 0.6 ms, and was also relatively voltage independent. Fatty acids are probably monomeric in the membrane under the conditions of our recording; thus detergent effects are unlikely. Since a number of compounds including fatty acids and prostaglandins activated these two channels, an indirect, channel-specific mechanism may account for activation of these two cardiac K+ channels.
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1 November 1991
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November 01 1991
Two novel cardiac atrial K+ channels, IK.AA and IK.PC.
M A Wallert,
M A Wallert
Department of Pharmacology, Mayo Foundation, Rochester, Minnesota 55905.
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M J Ackerman,
M J Ackerman
Department of Pharmacology, Mayo Foundation, Rochester, Minnesota 55905.
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D Kim,
D Kim
Department of Pharmacology, Mayo Foundation, Rochester, Minnesota 55905.
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D E Clapham
D E Clapham
Department of Pharmacology, Mayo Foundation, Rochester, Minnesota 55905.
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M A Wallert,
M J Ackerman,
D Kim,
D E Clapham
Department of Pharmacology, Mayo Foundation, Rochester, Minnesota 55905.
Online ISSN: 1540-7748
Print ISSN: 0022-1295
J Gen Physiol (1991) 98 (5): 921–939.
Citation
M A Wallert, M J Ackerman, D Kim, D E Clapham; Two novel cardiac atrial K+ channels, IK.AA and IK.PC.. J Gen Physiol 1 November 1991; 98 (5): 921–939. doi: https://doi.org/10.1085/jgp.98.5.921
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