1-P-011
報酬行動を規定するKCNQチャネルの分子メカニズム
Molecular Mechanism of KCNQ Channels For Reward Behavior
〇坪井 大輔1、大塚 岳2、下村 拓史3、久保 義弘3、川口 泰雄2、貝淵 弘三1
Daisuke Tsuboi1, Takeshi Otsuka2, Takushi Shimomura3, Yoshihiro Kubo3, Yasuo Kawaguchi2, Kozo Kaibuchi1
1名古屋大・院医、2生理学研・大脳神経回路論研究部門、3生理学研・神経機能素子研究部門
1Dept. of Cell Pharmacology, Grad. Sch. of Midicine, Nagoya University, 2Division of Cerebral Circuitry, National Institute of Physiological sciences, 3Division of Biophysics and Neurobilogy, National Institute of Physiological Sciences
Dopamine plays a key role in the modulation of the circuit activity in striatum for reward behavior. We have reported that dopamine type 1 receptor (D1R) signaling in the striatum presumably regulates neuronal excitability and reward-related behaviors through PKA/Rap1/MAPK pathway. However, how D1Rs and its downstream signaling regulate neuronal excitability and behavior remain largely unknown. We focus on the post-modification of ion channels for neuronal excitability and reward behavior because protein phosphorylation of ion channels is vital for neuronal function. In this study, we identified a voltage-gated potassium channel, KCNQ2, as a phospho-candidate that is regulated by D1R signaling. Phosphorylation of KCNQ2 by MAPK cascade altered the open probability of KCNQ2/3 channels in Xenopus oocyte. The expression of phospho-defective mutants of KCNQ2 suppressed the functional modulation of KCNQ channel by MAPK. D1R agonist, SKF38393 caused a decrease in KCNQ-sensitive current in striatal slices, whereas D2R agonist, Quinpirole did not cause the effect. These results suggest that D1Rsignaling controls the channel activity of KCNQ via its phosphorylation for neuronal excitability and reward behavior.