Spinal G-Protein-Gated K+ Channels Formed by GIRK1 and GIRK2 Subunits Modulate Thermal Nociception and Contribute to Morphine Analgesia

doi:10.1523/JNEUROSCI.5251-03.2004

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The Journal of Neuroscience, March 17, 2004, 24(11):2806-2812; doi:10.1523/JNEUROSCI.5251-03.2004

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Behavioral/Systems/Cognitive
Spinal G-Protein-Gated K⁺ Channels Formed by GIRK1 and GIRK2 Subunits Modulate Thermal Nociception and Contribute to Morphine Analgesia
Cheryl L. Marker,¹ Markus Stoffel,² and Kevin Wickman¹
¹Department of Pharmacology, University of Minnesota, Minneapolis, Minnesota 55455, and ²Laboratory of Metabolic Diseases, The Rockefeller University, New York, New York 10021

G-protein-gated potassium (K⁺) channels are found throughoutthe CNS in which they contribute to the inhibitory effects ofneurotransmitters and drugs of abuse. Recent studies have implicatedG-protein-gated K⁺ channels in thermal nociception and the analgesicaction of morphine and other agents. Because nociception issubject to complex spinal and supraspinal modulation, however,the relevant locations of G-protein-gated K⁺ channels are unknown.In this study, we sought to clarify the expression pattern andsubunit composition of G-protein-gated K⁺ channels in the spinalcord and to assess directly their contribution to thermal nociceptionand morphine analgesia. We detected GIRK1 (G-protein-gated inwardlyrectifying K⁺ channel subunit 1) and GIRK2 subunits, but notGIRK3, in the superficial layers of the dorsal horn. Lack ofeither GIRK1 or GIRK2 was correlated with significantly lowerexpression of the other, suggesting that a functional and physicalinteraction occurs between these two subunits. Consistent withthese findings, GIRK1 knock-out and GIRK2 knock-out mice exhibitedhyperalgesia in the tail-flick test of thermal nociception.Furthermore, GIRK1 knock-out and GIRK2 knock-out mice displayeddecreased analgesic responses after the spinal administrationof higher morphine doses, whereas responses to lower morphinedoses were preserved. Qualitatively similar data were obtainedwith wild-type mice after administration of the G-protein-gatedK⁺ channel blocker tertiapin. We conclude that spinal G-protein-gatedK⁺ channels consisting primarily of GIRK1/GIRK2 complexes modulatethermal nociception and mediate a significant component of theanalgesia evoked by intrathecal administration of high morphinedoses.

Key words: knock-out; opioid; tail-flick; Kir3; potassium; pain

Received Nov 26, 2003; revised January 26, 2004; accepted January 27, 2004.

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