Voltage-gated type 7 K+ (KV7 or KCNQ) channels regulate the contractility of various smooth muscles. With this study, we aimed to assess the role of KV7 channels in the regulation of human detrusor contractility, as well as the gene and protein expression of KV7 channels in this tissue. For these purposes, the isolated organ technique, RT-qPCR, and Western blot were used, respectively. XE-991, a selective KV7 channel blocker, concentration-dependently contracted the human detrusor; mean EC50 and Emax of XE-991-induced concentration-response curve were 14.1 μM and 28.8 % of the maximal bethanechol-induced contraction, respectively. Flupirtine and retigabine, selective KV7.2–7.5 channel activators, induced concentration-dependent relaxations of bethanechol-precontracted strips, with maximal relaxations of 51.6 and 51.8 % of the precontraction, respectively. XE-991 blocked the relaxations induced by flupirtine and retigabine. All five KCNQ genes were found to be expressed in the detrusor with KCNQ4 being the most expressed among them. Different bands, having sizes similar to some of reported KV7.1, 7.4, and 7.5 channel subunit isoforms, were detected in the detrusor by Western blot with the KV7.4 band being the most intense among them. In conclusion, KV7 channels contribute to set the basal tone of the human detrusor. In addition, KV7 channel activators significantly relax the detrusor. The KV7.4 channels are probably the most important KV7 channels expressed in the human detrusor. These data suggest that selective KV7.4 channel activators might represent new pharmacological tools for inducing therapeutic relaxation of the detrusor.

Bientinesi, R., Mancuso, C., Martire, M., Bassi, P., Sacco, E., Curro', D., KV7 channels in the human detrusor: channel modulator effects and gene and protein expression, <<NAUNYN-SCHMIEDEBERG'S ARCHIVES OF PHARMACOLOGY>>, 2017; 390 (2): 127-137. [doi:10.1007/s00210-016-1312-9] [http://hdl.handle.net/10807/91614]

KV7 channels in the human detrusor: channel modulator effects and gene and protein expression

Bientinesi, Riccardo
Primo
;
Mancuso, Cesare
Secondo
;
Martire, Maria;Bassi, Pierfrancesco;Sacco, Emilio
Penultimo
;
Curro', Diego
2017

Abstract

Voltage-gated type 7 K+ (KV7 or KCNQ) channels regulate the contractility of various smooth muscles. With this study, we aimed to assess the role of KV7 channels in the regulation of human detrusor contractility, as well as the gene and protein expression of KV7 channels in this tissue. For these purposes, the isolated organ technique, RT-qPCR, and Western blot were used, respectively. XE-991, a selective KV7 channel blocker, concentration-dependently contracted the human detrusor; mean EC50 and Emax of XE-991-induced concentration-response curve were 14.1 μM and 28.8 % of the maximal bethanechol-induced contraction, respectively. Flupirtine and retigabine, selective KV7.2–7.5 channel activators, induced concentration-dependent relaxations of bethanechol-precontracted strips, with maximal relaxations of 51.6 and 51.8 % of the precontraction, respectively. XE-991 blocked the relaxations induced by flupirtine and retigabine. All five KCNQ genes were found to be expressed in the detrusor with KCNQ4 being the most expressed among them. Different bands, having sizes similar to some of reported KV7.1, 7.4, and 7.5 channel subunit isoforms, were detected in the detrusor by Western blot with the KV7.4 band being the most intense among them. In conclusion, KV7 channels contribute to set the basal tone of the human detrusor. In addition, KV7 channel activators significantly relax the detrusor. The KV7.4 channels are probably the most important KV7 channels expressed in the human detrusor. These data suggest that selective KV7.4 channel activators might represent new pharmacological tools for inducing therapeutic relaxation of the detrusor.
2017
Inglese
Bientinesi, R., Mancuso, C., Martire, M., Bassi, P., Sacco, E., Curro', D., KV7 channels in the human detrusor: channel modulator effects and gene and protein expression, <<NAUNYN-SCHMIEDEBERG'S ARCHIVES OF PHARMACOLOGY>>, 2017; 390 (2): 127-137. [doi:10.1007/s00210-016-1312-9] [http://hdl.handle.net/10807/91614]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/10807/91614
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