Myometrial relaxation of mice via expression of two pore domain acid sensitive K(+) (TASK-2) channels

Myometrial relaxation of mouse via expression of two-pore domain acid sensitive (TASK) channels was studied. In our previous report, we suggested that two-pore domain acid-sensing K(+) channels (TASK-2) might be one of the candidates for the regulation of uterine circular smooth muscles in mice. In...

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Veröffentlicht in:The Korean journal of physiology & pharmacology 2016, 20(5), , pp.547-556
Hauptverfasser: Kyeong, Kyu-Sang, Hong, Seung Hwa, Kim, Young Chul, Cho, Woong, Myung, Sun Chul, Lee, Moo Yeol, You, Ra Young, Kim, Chan Hyung, Kwon, So Yeon, Suzuki, Hikaru, Park, Yeon Jin, Jeong, Eun-Hwan, Kim, Hak Soon, Kim, Heon, Lim, Seung Woon, Xu, Wen-Xie, Lee, Sang Jin, Ji, Il Woon
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Sprache:eng
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Zusammenfassung:Myometrial relaxation of mouse via expression of two-pore domain acid sensitive (TASK) channels was studied. In our previous report, we suggested that two-pore domain acid-sensing K(+) channels (TASK-2) might be one of the candidates for the regulation of uterine circular smooth muscles in mice. In this study, we tried to show the mechanisms of relaxation via TASK-2 channels in marine myometrium. Isometric contraction measurements and patch clamp technique were used to verify TASK conductance in murine myometrium. Western blot and immunehistochemical study under confocal microscopy were used to investigate molecular identity of TASK channel. In this study, we showed that TEA and 4-AP insensitive non-inactivating outward K(+) current (NIOK) may be responsible for the quiescence of murine pregnant longitudinal myometrium. The characteristics of NIOK coincided with two-pore domain acid-sensing K(+) channels (TASK-2). NIOK in the presence of K(+) channel blockers was inhibited further by TASK inhibitors such as quinidine, bupivacaine, lidocaine, and extracellular acidosis. Furthermore, oxytocin and estrogen inhibited NIOK in pregnant myometrium. When compared to non-pregnant myometrium, pregnant myometrium showed stronger inhibition of NIOK by quinidine and increased immunohistochemical expression of TASK-2. Finally, TASK-2 inhibitors induced strong myometrial contraction even in the presence of L-methionine, a known inhibitor of stretch-activated channels in the longitudinal myometrium of mouse. Activation of TASK-2 channels seems to play an essential role for relaxing uterus during pregnancy and it might be one of the alternatives for preventing preterm delivery.
ISSN:1226-4512
2093-3827
DOI:10.4196/kjpp.2016.20.5.547